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## Protocol Section ### Identification Module NCT ID: NCT06424132 Brief Title: Thermogenic Silencer Regulatory Factors in Humans Official Title: Identification of Thermogenic Silencing Regulatory Factors as Biomarkers of Metabolic Health in Humans #### Organization Study ID Info ID: PCO1051 #### Organization Class: OTHER Full Name: Rockefeller University ### Status Module #### Completion Date Date: 2027-05 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-05 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-10 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Cornell University #### Lead Sponsor Class: OTHER Name: Rockefeller University #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: A promising approach to correct the metabolic dysfunction associated with obesity is to activate brown fat non-shivering thermogenesis (NST). A critical limitation with NST as a therapeutic option, however, is that this beneficial process is silenced under human physiological temperature conditions and the mechanisms of how this occurs is unknown. This study will be the first to identify human NST silencing factors that may be targeted for the treatment of obesity and metabolic disorders. Detailed Description: Obesity and associated metabolic diseases such as type 2 diabetes continue to be one of the leading causes of death worldwide, demanding additional research into novel treatments beyond our current options. One promising experimental approach to overcome the metabolic dysfunctions associated with obesity, such as insulin resistance and glucose imbalance, is to activate brown fat non-shivering thermogenesis (NST). Activated human brown adipose tissue (BAT) increases energy expenditure at a molecular level and is associated with both improved insulin tolerance and glucose homeostasis. A critical limitation with human brown fat as a therapeutic option, however, is that its beneficial metabolic potential is restricted in a silenced state under physiological temperature conditions for most of human life. The regulatory factors that govern this silencing process are completely unknown. While many groups continue to seek novel mechanisms to activate brown fat, this study presents a unique approach, aiming to decipher the mechanisms that govern human brown fat silencing. The study hypothesizes that if the regulatory factors that silence brown fat NST can be defined, then these factors can be targeted for ablation to eliminate the "off switch", thereby keeping brown fat in a constitutively active state. Identification of human NST silencing factors will be critical to unlocking the metabolic benefits of human brown fat and would represent promising treatment opportunities for type 2 diabetes and other obesity-related disorders. Understanding these relationships will allow for precision treatment opportunities for type 2 diabetes in the future. The overall goal of this study is to unlock the metabolic benefits of human brown fat by defining the regulatory mechanisms that keep BAT in a silenced state. The study will generate the first human secretome (list of secreted proteins in blood) and transcriptome (list of gene transcripts in adipose tissue) compendium from human plasma and subcutaneous adipose tissue respectively which will be composed of target proteins, metabolites, and genes that are differentially expressed in response to NST silencing conditions. Top candidates from the profiling will then be functionally validated in human adipocytes for their role in NST silencing. The study will be an important resource for the field and will identify novel candidates that may harbor regulatory potential to govern the NST silencing process in humans. These factors can then be targeted to promote the constitutive activation of NST in order to overcome the metabolic dysfunction associated with obesity and metabolic disease. Given the invasive nature of direct human brown fat sampling, the study will instead interrogate circulating factors in human plasma as a proxy for metabolic health. In addition, the study will also obtain subcutaneous adipose tissue for RNA profiling to identify genes that are upregulated under NST-silenced conditions compared to cold exposure. ### Conditions Module Conditions: - Obesity - Metabolic Disease - Cold Exposure ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: CROSSOVER Intervention Model Description: Participants in from the three different study groups (lean, obese, and obese with type 2 diabetes) will receive the same intervention: cold environmental exposure followed by a rewarming period ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 120 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Body Mass Index (BMI) is \> 30, Hemoglobin A1c (HgA1c) \<5.7% Intervention Names: - Other: Cold Vest Exposure Period - Other: Rewarming Exposure Period - Other: Fasting Label: Obese group Type: EXPERIMENTAL #### Arm Group 2 Description: Body Mass Index (BMI) is \> 30, Hemoglobin A1c (HgA1c) is \>6.5% Intervention Names: - Other: Cold Vest Exposure Period - Other: Rewarming Exposure Period - Other: Fasting Label: Obese group with Type II diabetes Type: EXPERIMENTAL #### Arm Group 3 Description: Body Mass Index (BMI) is between 18.5 and 24.9. Hemoglobin A1c (HgA1c) \<5.7% Intervention Names: - Other: Cold Vest Exposure Period - Other: Rewarming Exposure Period - Other: Fasting Label: Lean group Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Lean group - Obese group - Obese group with Type II diabetes Description: A cold vest will be placed on the participant which consists of a water-perfused wearable vest, size S-M or M-L with adjustable straps attached to a small 'cooler' reservoir to circulate cold water between the vest and the cooler (Polar Products, Stow, OH- Product link: www.polarproducts.com/polarshop/pc/CoolOR-13-Quart-System-with-Arctic-Chiller-p24757.htm) This product is safe and recommended by experimental guidelines for human BAT studies. Participants will be cold exposed for a period of 3 hours resting in a reclined position engaged in reading and/or digital entertainment of their choice. Name: Cold Vest Exposure Period Type: OTHER #### Intervention 2 Arm Group Labels: - Lean group - Obese group - Obese group with Type II diabetes Description: Following cold exposure, the cold vests will be removed, and participants will be offered a warm blanket to ease the transition from cold back to warm temperatures. Participants will then be moved to an adjacent warm room maintained at 30 degrees celsius and asked to return to the resting position of their choice. Participants will then engage in reading and/or digital entertainment for a 3-hour warm exposure period. Name: Rewarming Exposure Period Type: OTHER #### Intervention 3 Arm Group Labels: - Lean group - Obese group - Obese group with Type II diabetes Description: Participants will be requested to refrain from food and caloric drinks for 12 hours (starting at 8pm) prior to the study visit. Blood will then be drawn the following morning (between 8 and 9am) 30mins later following a breakfast meal (9:30am- 10am). Participants will be housed in a room with ambient temperature at 25 degrees celsius between the two blood draws. Name: Fasting Type: OTHER ### Outcomes Module #### Primary Outcomes Description: RNA sequencing to measure and identify a list of gene transcripts that are differentially expressed before and after re-warming. A true change is defined as 1.5 fold increase or decrease in gene expression. Measure: Identification of adipose tissue transcriptome Time Frame: Before and after 3-hour rewarming period. Description: Proteins will be captured from blood and analyzed via mass spectrometry which generates a list of proteins for each sample. The investigators will compare the mean fold change (true change is greater than 1.5 fold) in protein abundance at the specified study time points. Measure: Identification of cold and warm-regulated proteome. Time Frame: Before and after 3 hour cold exposure period and before and after 3 hour rewarming period. Description: Metabolites will be captured from blood and analyzed via mass spectrometry which generates a list of metabolites for each sample. The investigators will compare the mean fold change (true change is greater than 1.5 fold) in metabolite abundance at the specified study time points. Measure: Identification of cold and warm-regulated metabolome. Time Frame: Time frame will be before and after 3 hour cold exposure period as well as before and after 3 hour rewarming period. #### Secondary Outcomes Description: Diet History Questionnaire III (DHQ III) calculates Healthy Eating Index (HEI- integer with no units). Measure: Nutritional assessments of individuals correlated to expression patterns of human silencer regulatory factors. Time Frame: Baseline Description: BMI is calculated by weight and height measured by anthropometric assessments, using the formula weight in kilograms divided by height in meters squared (kilograms/meter\^2). Measure: Body Mass Index (BMI) correlated to expression patterns of human silencer regulatory factors. Time Frame: Baseline Description: Bod Pod uses Air Displacement Plethysmography (ADP) to determine body composition, the ratio of fat mass to lean mass. The investigators will measure fat mass composition in units of percentage (%). Measure: Fat mass body composition (%) measured by Bod Pod correlated to expression patterns of human silencer regulatory factors. Time Frame: Baseline Description: Bod Pod uses Air Displacement Plethysmography (ADP) to determine body composition, the ratio of fat mass to lean mass. The investigators will measure lean mass composition in units of percentage (%). Measure: Lean Mass body composition (%) measured by Bod Pod correlated to expression patterns of human silencer regulatory factors. Time Frame: Baseline ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Age between 18 years old and 35 2. Lean group: BMI is between 18.5 and 24.9. HgA1c \<5.7% 3. Obese group: BMI is \>30, HgA1c \<5.7% 4. Obese group with Type II diabetes: BMI is \>30, HgA1c is \>6.5% If on oral medication for diabetes management, HgA1c may be \< 6.5% The following medications are also acceptable: statins, aspirin, angiotensin-converting enzyme inhibitors (ACEi), and angiotensin receptor blockers (ARB). Exclusion Criteria: 1. Diabetes type I (self-report) 2. Diagnosis of thyroid disease (including goiter, hyperthyroidism, hypothyroidism, thyroiditis)(self-report) 3. Diagnosis with cancer including skin cancer (self-report) 4. Diagnosis or evidence of Raynaud's Syndrome or systemic sclerosis (self-report) 5. A recent diagnosis of Coronavirus Disease 2019 (COVID-19) (last 2 weeks) or hospitalized at the time of diagnosis with COVID-19 6. Any vaccine administration within two weeks preceding the study procedure 7. Currently pregnant 8. Currently taking any prescribed medication other than oral contraceptives. Treatments for weight loss or any other supplements that may alter weight or metabolism are not acceptable. Vitamins are acceptable. 9. Has consumed nicotine (smoking, inhaling, ingesting) within the last 6 months 10. Has used illicit drugs within the last 6 months (marijuana users are eligible unless consumed in the last 30 days). 11. Any medical, psychological, or social condition that, in opinion of principle investigators, would jeopardize the health or well-being of the participant during the study procedure or the integrity of the data 12. Diabetes Type II that is managed by insulin. 13. Steroid use in the last 30 days to the exclusions Healthy Volunteers: True Maximum Age: 35 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Joeva Barrow, Ph.D., R.D. Phone: 607-255-9429 Role: CONTACT Contact 2: Email: [email protected] Name: Paul Cohen, Ph.D., M.D. Phone: 212-327-7918 Role: CONTACT #### Overall Officials Official 1: Affiliation: The Rockefeller University and Cornell University Name: Joeva Barrow, Ph.D., R.D. Role: PRINCIPAL_INVESTIGATOR Official 2: Affiliation: The Rockefeller University Name: Paul Cohen, Ph.D., M.D. Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Document Section ### Large Document Module #### Large Docs - Date: 2024-04-15 - Filename: Prot_SAP_000.pdf - Has ICF: False - Has Protocol: True - Has SAP: True - Label: Study Protocol and Statistical Analysis Plan - Size: 2110725 - Type Abbrev: Prot_SAP - Upload Date: 2024-04-26T13:28 - Date: 2024-04-15 - Filename: ICF_001.pdf - Has ICF: True - Has Protocol: False - Has SAP: False - Label: Informed Consent Form - Size: 913958 - Type Abbrev: ICF - Upload Date: 2024-04-26T13:23 ## Derived Section ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC01 - Name: Infections - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases ### Condition Browse Module - Browse Leaves - ID: M12701 - Name: Obesity - Relevance: LOW - As Found: Unknown - ID: M11639 - Name: Metabolic Diseases - Relevance: HIGH - As Found: Metabolic Diseases - ID: M14978 - Name: Respiratory Tract Infections - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000008659 - Term: Metabolic Diseases ### Intervention Browse Module - Browse Branches - Abbrev: Infl - Name: Anti-Inflammatory Agents - Abbrev: ARhu - Name: Antirheumatic Agents - Abbrev: Analg - Name: Analgesics - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M207501 - Name: Chrysarobin - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424119 Acronym: CREDIBLE Brief Title: Multi-Center Study of Clinical and Inflammatory Outcomes in Intensive Cardiac Rehabilitation and Traditional Cardiac Rehabilitation Programs Official Title: Multi-Center Randomized Study of Clinical and Inflammatory Outcomes in Intensive Cardiac Rehabilitation and Traditional Cardiac Rehabilitation Programs (CREDIBLE Study) #### Organization Study ID Info ID: CREDIBLE #### Organization Class: OTHER Full Name: Pritikin ICR ### Status Module #### Completion Date Date: 2027-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2026-06-30 Type: ESTIMATED #### Start Date Date: 2024-04-26 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-12 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Ballad Health Class: OTHER Name: Mission Health System, Asheville, NC Class: UNKNOWN Name: Trinity Health Class: OTHER Name: Connecting Health Innovation #### Lead Sponsor Class: OTHER Name: Pritikin ICR #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The goal of this prospective study is to evaluate whether the Intensive Cardiac Rehabilitation (ICR) program provides incremental benefits over the Traditional Cardiac Rehabilitation (TCR) program, defined by readmission costs. The study aims to confirm: * That ICR is associated with better outcomes than TCR, defined as lower readmission costs, lower incidence of major adverse cardiovascular events (MACE), and improvement in biomarkers, epigenetic markers, and inflammatory markers. * The addition of food to the ICR program will further improve these outcomes. ICR-eligible participants * Will be randomized into one of three groups: (1) ICR 72 session program with home-delivered C2life® supplied food, (2) ICR 72 session without C2life® supplied food, or (3) TCR 36 session program without C2life supplied food * Biometric measurements and laboratory measurements will be performed at entry into the rehab intervention, discharge from rehab intervention, and at 6 months after discharge. * Epigenetic measurements will be performed at admission and discharge from the rehab intervention ### Conditions Module Conditions: - Cardiovascular Diseases Keywords: - Intensive Cardiac Rehabilitation - Traditional Cardiac Rehabilitation ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: ICR-eligible patients are randomized into one of three groups of 150 patients: (1) ICR 72 session program with C2life® supplied food, (2) ICR 72 session without C2life® supplied food, or (3) TCR 36 session program without C2life supplied food (ICR-food, ICR-no food, and TCR-no food). ##### Masking Info Masking: SINGLE Who Masked: - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 450 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Intensive Cardiac Rehab (ICR) 72-session program without C2life® supplied food Intervention Names: - Behavioral: Intensive Cardiac Rehabilitation Label: ICR-No Food Type: EXPERIMENTAL #### Arm Group 2 Description: Intensive Cardiac Rehab (ICR_ 72-session program with C2life® supplied food Intervention Names: - Behavioral: Intensive Cardiac Rehabilitation - Other: C2life® Food Label: ICR-Food Type: EXPERIMENTAL #### Arm Group 3 Description: Traditional Cardiac Rehab (TCR) 36-session program without C2life® supplied food Intervention Names: - Behavioral: Traditional Cardiac Rehabilitation Label: TCR-No Food Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - TCR-No Food Description: Patient must have a qualifying cardiovascular event and eligible for ICR. Once patient is randomized to TCR arm, they will attend 36 sessions of the program at one of three locations. Name: Traditional Cardiac Rehabilitation Other Names: - TCR Type: BEHAVIORAL #### Intervention 2 Arm Group Labels: - ICR-Food - ICR-No Food Description: Patient must have a qualifying cardiovascular event and eligible for ICR. Once patient is randomized to ICR arm, they will attend 72 sessions of the program at one of three locations. Name: Intensive Cardiac Rehabilitation Other Names: - ICR Type: BEHAVIORAL #### Intervention 3 Arm Group Labels: - ICR-Food Description: Patient must have a qualifying cardiovascular event and eligible for ICR. Once patient is randomized to ICR arm with food, they will receive the food at the beginning of the second week of their respective program. Food will be delivered by mail weekly for a total of 11 weeks to the patient's home address. Name: C2life® Food Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Readmission rate data will include: 1. Actual number of all cause readmissions 2. Days in hospital for each readmission 3. Cost of readmission. Stratification between all cause and cardiovascular readmissions will be performed as an additional sub-analysis. Measure: Readmission Rate Data Time Frame: Followup may extend up to 5 years for a post-hoc EMR analysis. #### Secondary Outcomes Description: MACE is defined as all-cause death, non-fatal MI, hospitalization for unstable angina, PCI, CABG, peripheral artery revascularization, Ischemic stroke, CHF hospitalization, heart valve surgery, and heart transplant. Measure: MACE Time Frame: At 1 and 2 years. Description: Number of readmissions within 2 years. Measure: Composite Total Readmission Rates Time Frame: At 1 and 2 years Description: Composite length of stay in days for the total readmission events and each MACE category within 2 years. Measure: Readmission Days Time Frame: At 1 and 2 years Description: Scores will be calculated for the C2life® diet as a whole and for each participant at the prespecified measurement times. Measure: Dietary Inflammation Index (DII) Time Frame: At admission, discharge from program (about 12 weeks), and 6 month post-discharge Description: Labs will include lipids, comprehensive metabolic profile, HbA1c, Hs-CRP, IL-6, TNF-alpha, IFN-gamma, and ceramides. Measure: Labs Time Frame: At admission, discharge (about 12 weeks), and 6 months post-discharge Description: Buccal swab samples will be taken to obtain this data. We propose to use a set of epigenetic biomarkers to measure biological age, metabolic health, inflammation, and overall fitness. Measure: Epigenetic Biomarkers Performed by Prosper eDNA® Time Frame: Buccal swab at admission and discharge (about 12 weeks) ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * All patients eligible for an Intensive Cardiac Rehabilitation (ICR) Program at each of the three study sites outline below, stratified by one of the following qualifying cardiovascular events, including myocardial infarction (STEMI and NSTEMI), angioplasty and stents, coronary artery bypass, surgical or percutaneous valve repair or replacement, and stable congestive heart failure with reduced ejection fraction of 35% or less. Exclusion Criteria: * Anticipated life expectancy of under 2 years * Any co-morbidity that would limit participation in the study. Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Ypsilanti Contacts: *Contact 1:* - Email: [email protected] - Name: Frank Smith, MD - Phone: 734-712-8000 - Role: CONTACT *Contact 2:* - Name: Autumn Howe, RN - Phone: (734)712-8387 - Role: CONTACT *Contact 3:* - Name: Frank A. Smith, MD - Role: PRINCIPAL_INVESTIGATOR Country: United States Facility: Trinity Health Ann Arbor State: Michigan Status: RECRUITING Zip: 48197 Location 2: City: Asheville Contacts: *Contact 1:* - Email: [email protected] - Name: Brian Asbill, MD - Phone: 828-274-6000 - Role: CONTACT *Contact 2:* - Name: Brian Asbill, MD - Role: PRINCIPAL_INVESTIGATOR Country: United States Facility: Mission Health State: North Carolina Status: RECRUITING Zip: 28803 Location 3: City: Kingsport Contacts: *Contact 1:* - Email: [email protected] - Name: David Beckner, MD - Phone: 423-230-5640 - Role: CONTACT *Contact 2:* - Name: David Beckner, MD - Role: PRINCIPAL_INVESTIGATOR Country: United States Facility: Ballad CVA Heart Institute State: Tennessee Status: NOT_YET_RECRUITING Zip: 37660 #### Overall Officials Official 1: Affiliation: Mission Health Name: Brian Asbill, MD Role: PRINCIPAL_INVESTIGATOR Official 2: Affiliation: Ballad Health Name: David Beckner, MD Role: PRINCIPAL_INVESTIGATOR Official 3: Affiliation: Trinity Health Name: Frank A. Smith, MD Role: PRINCIPAL_INVESTIGATOR Official 4: Affiliation: Connecting Health Innovations, LLC (CHI) Name: James R. Hebert, ScD, MSPH Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ### References Module #### References Citation: Writing Group Members; Mozaffarian D, Benjamin EJ, Go AS, Arnett DK, Blaha MJ, Cushman M, Das SR, de Ferranti S, Despres JP, Fullerton HJ, Howard VJ, Huffman MD, Isasi CR, Jimenez MC, Judd SE, Kissela BM, Lichtman JH, Lisabeth LD, Liu S, Mackey RH, Magid DJ, McGuire DK, Mohler ER 3rd, Moy CS, Muntner P, Mussolino ME, Nasir K, Neumar RW, Nichol G, Palaniappan L, Pandey DK, Reeves MJ, Rodriguez CJ, Rosamond W, Sorlie PD, Stein J, Towfighi A, Turan TN, Virani SS, Woo D, Yeh RW, Turner MB; American Heart Association Statistics Committee; Stroke Statistics Subcommittee. Heart Disease and Stroke Statistics-2016 Update: A Report From the American Heart Association. 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Cardiac rehabilitation and secondary prevention of coronary heart disease: an American Heart Association scientific statement from the Council on Clinical Cardiology (Subcommittee on Exercise, Cardiac Rehabilitation, and Prevention) and the Council on Nutrition, Physical Activity, and Metabolism (Subcommittee on Physical Activity), in collaboration with the American association of Cardiovascular and Pulmonary Rehabilitation. Circulation. 2005 Jan 25;111(3):369-76. doi: 10.1161/01.CIR.0000151788.08740.5C. Erratum In: Circulation. 2005 Apr 5;111(13):1717. PMID: 15668354 Citation: McMahon SR, Ades PA, Thompson PD. The role of cardiac rehabilitation in patients with heart disease. Trends Cardiovasc Med. 2017 Aug;27(6):420-425. doi: 10.1016/j.tcm.2017.02.005. Epub 2017 Feb 15. PMID: 28318815 Citation: Kotseva K, Wood D, De Bacquer D; EUROASPIRE investigators. Determinants of participation and risk factor control according to attendance in cardiac rehabilitation programmes in coronary patients in Europe: EUROASPIRE IV survey. Eur J Prev Cardiol. 2018 Aug;25(12):1242-1251. doi: 10.1177/2047487318781359. Epub 2018 Jun 6. PMID: 29873511 Citation: Anderson L, Oldridge N, Thompson DR, Zwisler AD, Rees K, Martin N, Taylor RS. Exercise-Based Cardiac Rehabilitation for Coronary Heart Disease: Cochrane Systematic Review and Meta-Analysis. J Am Coll Cardiol. 2016 Jan 5;67(1):1-12. doi: 10.1016/j.jacc.2015.10.044. PMID: 26764059 Citation: Balady GJ, Williams MA, Ades PA, Bittner V, Comoss P, Foody JM, Franklin B, Sanderson B, Southard D; American Heart Association Exercise, Cardiac Rehabilitation, and Prevention Committee, the Council on Clinical Cardiology; American Heart Association Council on Cardiovascular Nursing; American Heart Association Council on Epidemiology and Prevention; American Heart Association Council on Nutrition, Physical Activity, and Metabolism; American Association of Cardiovascular and Pulmonary Rehabilitation. Core components of cardiac rehabilitation/secondary prevention programs: 2007 update: a scientific statement from the American Heart Association Exercise, Cardiac Rehabilitation, and Prevention Committee, the Council on Clinical Cardiology; the Councils on Cardiovascular Nursing, Epidemiology and Prevention, and Nutrition, Physical Activity, and Metabolism; and the American Association of Cardiovascular and Pulmonary Rehabilitation. Circulation. 2007 May 22;115(20):2675-82. doi: 10.1161/CIRCULATIONAHA.106.180945. Epub 2007 May 18. PMID: 17513578 Citation: R. James Barnard, Ph.D. The Pritikin Program: Understanding its value in Preventing and Controlling common diseases Citation: Gomez-Delgado F, Katsiki N, Lopez-Miranda J, Perez-Martinez P. Dietary habits, lipoprotein metabolism and cardiovascular disease: From individual foods to dietary patterns. Crit Rev Food Sci Nutr. 2021;61(10):1651-1669. doi: 10.1080/10408398.2020.1764487. Epub 2020 Jun 9. PMID: 32515660 Citation: Wong MMH, Louie JCY. A priori dietary patterns and cardiovascular disease incidence in adult population-based studies: a review of recent evidence. Crit Rev Food Sci Nutr. 2022;62(22):6153-6168. doi: 10.1080/10408398.2021.1897517. Epub 2021 Mar 10. PMID: 33715546 Citation: Zhong VW, Ning H, Van Horn L, Carnethon MR, Wilkins JT, Lloyd-Jones DM, Allen NB. Diet Quality and Long-Term Absolute Risks for Incident Cardiovascular Disease and Mortality. Am J Med. 2021 Apr;134(4):490-498.e24. doi: 10.1016/j.amjmed.2020.08.012. Epub 2020 Sep 14. PMID: 32941845 Citation: Kiecolt-Glaser JK. Stress, food, and inflammation: psychoneuroimmunology and nutrition at the cutting edge. Psychosom Med. 2010 May;72(4):365-9. doi: 10.1097/PSY.0b013e3181dbf489. Epub 2010 Apr 21. PMID: 20410248 Citation: Shivappa N, Godos J, Hebert JR, Wirth MD, Piuri G, Speciani AF, Grosso G. Dietary Inflammatory Index and Cardiovascular Risk and Mortality-A Meta-Analysis. Nutrients. 2018 Feb 12;10(2):200. doi: 10.3390/nu10020200. PMID: 29439509 Citation: Mazidi M, Shivappa N, Wirth MD, Hebert JR, Mikhailidis DP, Kengne AP, Banach M. Dietary inflammatory index and cardiometabolic risk in US adults. Atherosclerosis. 2018 Sep;276:23-27. doi: 10.1016/j.atherosclerosis.2018.02.020. Epub 2018 Feb 15. PMID: 30015256 Citation: Marx W, Veronese N, Kelly JT, Smith L, Hockey M, Collins S, Trakman GL, Hoare E, Teasdale SB, Wade A, Lane M, Aslam H, Davis JA, O'Neil A, Shivappa N, Hebert JR, Blekkenhorst LC, Berk M, Segasby T, Jacka F. The Dietary Inflammatory Index and Human Health: An Umbrella Review of Meta-Analyses of Observational Studies. Adv Nutr. 2021 Oct 1;12(5):1681-1690. doi: 10.1093/advances/nmab037. PMID: 33873204 Citation: Asadi Z, Yaghooti-Khorasani M, Ghazizadeh H, Sadabadi F, Mosa-Farkhany E, Darroudi S, Shabani N, Kamel-Khodabandeh A, Bahrami A, Khorrami-Mohebbseraj MS, Heidari-Bakavoli S, Heidari-Bakavoli A, Esmaily H, Moohebati M, Oladi MR, Shivappa N, Hebert JR, Ferns GA, Ghayour-Mobarhan M. Association between dietary inflammatory index and risk of cardiovascular disease in the Mashhad stroke and heart atherosclerotic disorder study population. IUBMB Life. 2020 Apr;72(4):706-715. doi: 10.1002/iub.2172. Epub 2019 Oct 16. PMID: 31617677 Citation: Todendi PF, Salla R, Shivappa N, Hebert JR, Ritter J, Cureau FV, Schaan BD. Association between dietary inflammatory index and cardiometabolic risk factors among Brazilian adolescents: results from a national cross-sectional study. Br J Nutr. 2022 Aug 28;128(4):744-752. doi: 10.1017/S0007114521003767. Epub 2021 Sep 21. Erratum In: Br J Nutr. 2022 Aug 28;128(4):784. PMID: 34544504 Citation: Zelen M. A new design for randomized clinical trials. N Engl J Med. 1979 May 31;300(22):1242-5. doi: 10.1056/NEJM197905313002203. PMID: 431682 Citation: Zelen M. Alternatives to classic randomized trials. Surg Clin North Am. 1981 Dec;61(6):1425-32. doi: 10.1016/s0039-6109(16)42596-x. PMID: 7313934 Citation: Zelen M. Randomized consent designs for clinical trials: an update. Stat Med. 1990 Jun;9(6):645-56. doi: 10.1002/sim.4780090611. PMID: 2218168 Citation: Torgerson DJ, Roland M. What is Zelen's design? BMJ. 1998 Feb 21;316(7131):606. doi: 10.1136/bmj.316.7131.606. No abstract available. PMID: 9518917 Citation: Peterson LR, Xanthakis V, Duncan MS, Gross S, Friedrich N, Volzke H, Felix SB, Jiang H, Sidhu R, Nauck M, Jiang X, Ory DS, Dorr M, Vasan RS, Schaffer JE. Ceramide Remodeling and Risk of Cardiovascular Events and Mortality. J Am Heart Assoc. 2018 May 3;7(10):e007931. doi: 10.1161/JAHA.117.007931. PMID: 29728014 ## Derived Section ### Condition Browse Module - Meshes - ID: D000002318 - Term: Cardiovascular Diseases ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424106 Brief Title: Effect of Glucagon on Fasting Insulin Secretion and Glucose Metabolism in Subjects Without Type 2 Diabetes Official Title: Effect of Glucagon on Fasting Insulin Secretion and Glucose Metabolism in Subjects Without Type 2 Diabetes #### Organization Study ID Info ID: 24-002639 #### Organization Class: OTHER Full Name: Mayo Clinic ### Status Module #### Completion Date Date: 2027-07-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-07-01 Type: ESTIMATED #### Start Date Date: 2024-07-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-13 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Mayo Clinic #### Responsible Party Investigator Affiliation: Mayo Clinic Investigator Full Name: Adrian Vella Investigator Title: Professor of Medicine Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Fasting hyperglycemia contributes disproportionately to nonenzymatic glycosylation and the microvascular complications of type 2 diabetes. However, little is known about the regulation of glucose concentrations in the fasting state relative to what is known about the postprandial state. The proposed experiment is part of a series of experiments designed to establish how glucagon and insulin interact with their receptors to control fasting glucose in health and in prediabetes. Detailed Description: The interaction between α-cell and β-cell function to regulate fasting glucose is incompletely understood. This is an important gap in our knowledge as fasting glucose contributes disproportionately to HbA1c and the microvascular complications of type 2 diabetes (T2DM). The regulation of fasting glucose in health and disease is relatively understudied. Insulin and glucagon should regulate glucose reciprocally through direct interaction; insulin restrains α-cell secretion while glucagon directly stimulates β-cell secretion. In addition, there are indirect interactions via changes in glucose. Glucagon increases endogenous glucose production (EGP) increasing glucose (and insulin secretion). Conversely, insulin stimulates glucose disappearance (Rd) and suppresses EGP, lowering glucose (and stimulating glucagon). However, this does not appear to occur uniformly in prediabetes. For example, in impaired fasting glucose (IFG), glucagon secretion rate (GSR) is inappropriate for the prevailing glucose. This is not accompanied by reciprocal changes in insulin secretion rate (ISR). Variability in the hepatic response to glucagon and to insulin further compound the dysregulation of fasting glucose. The net effect of these variables is unknown. This experiment is intended to test the hypothesis that impaired glucagon-induced insulin secretion contributes to fasting hyperglycemia in IFG. ### Conditions Module Conditions: - PreDiabetes Keywords: - Insulin secretion - glucagon secretion - endogenous glucose production - glucose disappearance ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: SEQUENTIAL Intervention Model Description: All participants will complete two experiments conducted in random order. On one day they will receive a graded glucagon infusion while on the other they will receive a glucose infusion that replicates the glucose concentrations observed in the first study day ##### Masking Info Masking: NONE Primary Purpose: BASIC_SCIENCE #### Enrollment Info Count: 60 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: A glucagon infusion (0.2 ng/kg/min) will start at 0900 (0 min), increasing to 0.4 (1000), 0.6 (1100) and 0.8 ng/kg/min (1200) at 60-minute intervals - ending at 1300 (240 min). Intervention Names: - Other: Glucagon Label: Glucagon Infusion Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: At 0900 (0 min) a glucose infusion will commence, and the infusion rate varied to replicate (± 5mg/dL) that individual's glucose concentrations observed during the Glucagon Infusion Day. The experiment will end at 1300 (240 min) when infusions are stopped. Intervention Names: - Other: Glucose Label: Glucose Infusion Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Glucagon Infusion Description: a variable rate glucagon infusion Name: Glucagon Type: OTHER #### Intervention 2 Arm Group Labels: - Glucose Infusion Description: a variable rate glucose infusion Name: Glucose Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The beta-cell responsivity observed during glucagon infusion will be compared to that observed during glucose infusion Measure: Change in beta-cell responsivity induced by glucagon Time Frame: Beta-cell responsivity will be calculated as the gradient of the relationship between glucose concentrations and insulin secretion rate during the study day over the 4 hours (0 to 240 minutes) of the study #### Secondary Outcomes Description: The endogenous glucose production observed during glucagon infusion will be compared to that observed during glucose infusion Measure: change in endogenous glucose production induced by glucagon Time Frame: The rate of endogenous glucose production at the end of the study (240 minutes) will be expressed as a percentage of that at the beginning of the study (0 minutes). The % change for each study day will then be compared Description: The glucose disappearance observed during glucagon infusion will be compared to that observed during glucose infusion Measure: change in glucose disappearance induced by glucagon Time Frame: The rate of glucose disappearance at the end of the study (240 minutes) will be expressed as a percentage of that at the beginning of the study (0 minutes). The % change for each study day will then be compared ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Individuals with normal or impaired fasting glucose and normal or impaired glucose tolerance Exclusion Criteria: * HbA1c less than 6.5% * Use of any glucose-lowering agents including metformin or sulfonylureas. * For female subjects: positive pregnancy test at the time of enrollment or study * History of prior upper abdominal surgery such as adjustable gastric banding, pyloroplasty and vagotomy. * Active systemic illness or malignancy. * Symptomatic macrovascular or microvascular disease. Healthy Volunteers: True Maximum Age: 65 Years Minimum Age: 25 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Kim Osmundson, CCRP Phone: 507-255-0907 Role: CONTACT Contact 2: Email: [email protected] Name: Jeanette Laugen Phone: 507-255-8110 Role: CONTACT #### Locations Location 1: City: Rochester Country: United States Facility: Mayo Clinic in Rochester State: Minnesota Zip: 55905 #### Overall Officials Official 1: Affiliation: Mayo Clinic Name: Adrian Vella, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: The data being shared is human data from clinical trials and therefore a higher level of protection is required. Access to this data will be controlled by a managed access process whereby access is provided only after approval. Data will be controlled access with the General Research Use Data Use Limitation, as allowed by the informed consent and the institutional certification. Description: In addition to the patient-level data, the metadata, data dictionary, statistical analysis plan, and final protocol will be shared. The sharing of the data dictionary, statistical analysis plan and final protocol with amendments will enable researchers to understand how the data was collected and to correctly interpret the data for future secondary analysis. We plan to share datasets resulting from the proposed studies in Vivli, a non-profit institution that supports the Vivli repository. Info Types: - STUDY_PROTOCOL - SAP - ICF - CSR - ANALYTIC_CODE IPD Sharing: YES Time Frame: The data shared will be archived and available on the platform for request by researchers for a minimum of 10 years after contribution. Data will be made accessible no later than the time of our associated publication or the end of the grant period (whichever comes first). On an ongoing basis, Vivli evaluates its data holdings regarding maintaining access and reserves the right to discontinue the distribution of a data collections when deemed appropriate. When materials are deaccessioned, the data are no longer publicly accessible at Vivli, they may still be preserved in Vivli's storage vault. Because digital files are assigned a persistent digital object identifier (DOI), the study description is still available to view, but is not searchable through Vivli. ## Derived Section ### Condition Browse Module - Ancestors - ID: D000003920 - Term: Diabetes Mellitus - ID: D000044882 - Term: Glucose Metabolism Disorders - ID: D000008659 - Term: Metabolic Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M14117 - Name: Prediabetic State - Relevance: HIGH - As Found: Prediabetes - ID: M20295 - Name: Glucose Intolerance - Relevance: LOW - As Found: Unknown - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M7119 - Name: Diabetes Mellitus, Type 2 - Relevance: LOW - As Found: Unknown - ID: M11639 - Name: Metabolic Diseases - Relevance: LOW - As Found: Unknown - ID: M25403 - Name: Glucose Metabolism Disorders - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000011236 - Term: Prediabetic State ### Intervention Browse Module - Ancestors - ID: D000005765 - Term: Gastrointestinal Agents - ID: D000006728 - Term: Hormones - ID: D000006730 - Term: Hormones, Hormone Substitutes, and Hormone Antagonists - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: Hypo - Name: Hypoglycemic Agents - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Gast - Name: Gastrointestinal Agents ### Intervention Browse Module - Browse Leaves - ID: M10365 - Name: Insulin - Relevance: LOW - As Found: Unknown - ID: M173166 - Name: Insulin, Globin Zinc - Relevance: LOW - As Found: Unknown - ID: M9043 - Name: Glucagon - Relevance: HIGH - As Found: Disability - ID: M26997 - Name: Glucagon-Like Peptide 1 - Relevance: LOW - As Found: Unknown - ID: M8881 - Name: Gastrointestinal Agents - Relevance: LOW - As Found: Unknown - ID: M9789 - Name: Hormones - Relevance: LOW - As Found: Unknown - ID: M9788 - Name: Hormone Antagonists - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000005934 - Term: Glucagon ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424093 Brief Title: Effect of Virtual Reality Technology for Managment of Acute Pain in Outpatient Hysteroscopy Official Title: Effect of Virtual Reality Technology for Managment of Acute Pain in Outpatient Hysteroscopy: A Randomised Controlled Trial #### Organization Study ID Info ID: Virtual Reality Technology #### Organization Class: INDUSTRY Full Name: Egymedicalpedia ### Status Module #### Completion Date Date: 2024-11-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-11-01 Type: ESTIMATED #### Start Date Date: 2024-05-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-11 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Egymedicalpedia #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: Performing out patient diagnostic and operative gynecological procedures is becoming more popular having the benefits of reducing risks of general anaesthetia, decreasing healthcare burden and increasing satisfaction for both patient and provider. Virtual reality (VR), a new technology, has been studied as a distraction technique for non-pharmacological method of pain relief. It is a computer-generated representation of an immersive videos viewed through a headset. Detailed Description: Performing out patient diagnostic and operative gynecological procedures is becoming more popular having the benefits of reducing risks of general anaesthetia, decreasing healthcare burden and increasing satisfaction for both patient and provider. Such procedures are usually well tolerated , However it can be associated with acute pain and anxiety. Options of Pain relief include sedation, local anaesthetic , analgesics and distraction techniques, however no consistent good quality evidence exists to support practice. Virtual reality (VR), a new technology, has been studied as a distraction technique for non-pharmacological method of pain relief. It is a computer-generated representation of an immersive videos viewed through a headset. The obstacles of cost, quality and accessibility of (VR) devices have significantly eliminated in recent years and offer promising application in the medical field. Virtual reality for managing pain has been studied in many fields including paediatrics, dentistry, burns treatment, chronic pain, labour, and episiotomy. Although a meta-analysis suggested that VR may have a role in reducing pain scores in acutely painful interventions , studies found it to be effective only in needles and burns physical therapy. The studies of VR on pain and anxiety, however, were limited by clinical and statistical heterogeneity. Nonpharmacological options of pain relief have not explored enough the role of VR in reducing pain and improving patient experience in outpatient hysteroscopy .To our knowledge, there is only one publication studying the role of virtual reality in the management of acute pain during office gynaecological procedures ### Conditions Module Conditions: - Acute Pain - Anxiety Keywords: - hysteroscopy - Acute Pain - Anxiety - Virtual Reality ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 50 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: About 25 women indicated for diagnostic hysteroscopy with using Virtual Reality Technology Intervention Names: - Procedure: Virtual Reality Technology Label: Group A: Cases Group Type: EXPERIMENTAL #### Arm Group 2 Description: About 25 women indicated for diagnostic hysteroscopy without using Virtual Reality Technology Intervention Names: - Procedure: Virtual Reality Technology Label: Group B: Control Group Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Group A: Cases Group - Group B: Control Group Description: To evaluate the role of virtual reality technology as distraction technique in the management of acute pain during outpatient hysteroscopy Name: Virtual Reality Technology Other Names: - Hysteroscopy Type: PROCEDURE ### Outcomes Module #### Primary Outcomes Description: The pain level of the cases is evaluated by means of the digital pain as the 11-point visual analog scale (VAS) whereas 0-Represents no pain, 10 - Worst imaginable pain), as well as the 11-point VAS-A (0-Represents no anxiety, 10 - Highest anxiety) Measure: Assessment of Pain Time Frame: 10 minutes from starting the procedure ### Eligibility Module Eligibility Criteria: Inclusion Criteria: - Patients scheduled for diagnostic hysteroscopy e.g. Infertility, AUB Exclusion Criteria: * Absolute contraindication to office hysteroscopy such as acute pelvic infection , active genital herpes , heavy bleeding or pregnancy. * Psychological ,hearing or visual disorders. * known anatomical condition that make performing office hysteroscopy is difficult such as cervical stenosis ,fibrosis or cervical amputation . * Previous history of failed office hysteroscopy * Patients scheduled for operative hysteroscopy. Maximum Age: 60 Years Minimum Age: 18 Years Sex: FEMALE Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Waleed Mohamed shawky, MSC Phone: +201093699004 Role: CONTACT Contact 2: Email: [email protected] Name: Tarek Sabry Mohamed, MSC Phone: +201096398888 Role: CONTACT #### Locations Location 1: City: Cairo Contacts: *Contact 1:* - Email: [email protected] - Name: Ahmed Eid Elsayed Zidan, MSc - Phone: +201067845518 - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Joseph Adel Ibrahim, MSc - Phone: +201285515950 - Role: CONTACT *Contact 3:* - Name: Rania Gamal Anwar, Lecturer - Role: PRINCIPAL_INVESTIGATOR *Contact 4:* - Name: Yassin Asaad Mostafa, MSc - Role: SUB_INVESTIGATOR Country: Egypt Facility: Ain Shams University Hospitals Status: RECRUITING #### Overall Officials Official 1: Affiliation: Head of Obstetrics and Gynecology department , Faculty of Medicine, Ain Shams University Name: Amr Elhussieny, Professor Role: STUDY_CHAIR Official 2: Affiliation: Department of obstetrics & gynecology, Faculty Of Medicine, Ain Shams University Name: Mortada El Sayed Ahmed, Professor Role: STUDY_DIRECTOR Official 3: Affiliation: Department of obstetrics & gynecology, Faculty Of Medicine, Ain Shams University Name: Radwa Rsaheedy Ali, M.D Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ## Derived Section ### Condition Browse Module - Ancestors - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M4324 - Name: Anxiety Disorders - Relevance: LOW - As Found: Unknown - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M29525 - Name: Acute Pain - Relevance: HIGH - As Found: Acute Pain - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000059787 - Term: Acute Pain ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424080 Brief Title: Oncological and Perioperative Outcomes of Laparoscopic Versus Robotic Partial Nephrectomy for Treatment of Renal Tumors. Official Title: Oncological and Perioperative Outcomes of Laparoscopic Versus Robotic Partial Nephrectomy for Treatment of Renal Tumors. #### Organization Study ID Info ID: 6-2024UROL #### Organization Class: OTHER Full Name: Menoufia University ### Status Module #### Completion Date Date: 2025-12-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-22 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-11-10 Type: ESTIMATED #### Start Date Date: 2024-05-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-13 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Menoufia University #### Responsible Party Investigator Affiliation: Menoufia University Investigator Full Name: Hossam Kandeel Investigator Title: Yassin Abdelghaffar st-from Gamal Abdel Nasar st- faculty of medicine Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: partial nephrectomy offers lower renal function impairment and equivalent oncological survival outcomes compared with radical nephrectomy in those with T1 tumors. As urology has embraced the gradual shift from open to minimally invasive surgery (MIS), PN is being completed more often by laparoscopic and robotic methods . The first laparoscopic transperitoneal partial nephrectomy was reported in 1993 by Winfield, with the retroperitoneal approach introduced 1 year later With advancing robotic technology and the development of the DaVinci system, urologists began to explore the realm of robotic-assisted urologic surgery. In 2004, Gettman et al. published a paper describing their experience with robotic-assisted laparoscopic partial nephrectomy. Moreover, robotic assisted partial nephrectomy (RAPN) and laparoscopic partial nephrectomy (LPN) seems to be significantly better than OPN in terms of perioperative complications, estimated blood loss and hospital stay. Conversely, transfusion rate, ischemia time, change in estimated glomerular filtration rate and early cancer outcomes are similar between the two approaches. International guidelines recommend the use of both approaches according to the surgeon and patient preferences. so, we are plaining to do the study comparing between RAPN and LPN regarding feasibility and ability of both techniques. Detailed Description: Renal cell carcinoma (RCC) represents a significant burden of malignancy. Over the past 2-3 decades, the incidence of kidney cancer has steadily increased all around the world ,.The EUA Guidelines suggested that surgery is the only curative treatment for localized renal cell carcinoma. Surgical treatment of RCC either radical or partial nephrectomy is related to the clinical stage of the disease and to the general condition of the patient. Modern medical imaging has further revolutionized the role of PN due to the increasing volume of incidentally diagnosed small renal masses. Indeed, partial nephrectomy offers lower renal function impairment and equivalent oncological survival outcomes compared with radical nephrectomy in those with T1 tumors. As urology has embraced the gradual shift from open to minimally invasive surgery (MIS), PN is being completed more often by laparoscopic and robotic methods . The first laparoscopic transperitoneal partial nephrectomy was reported in 1993 by Winfield, with the retroperitoneal approach introduced 1 year later With advancing robotic technology and the development of the DaVinci system, urologists began to explore the realm of robotic-assisted urologic surgery. In 2004, Gettman et al. published a paper describing their experience with robotic-assisted laparoscopic partial nephrectomy. Moreover, robotic assisted partial nephrectomy (RAPN) and laparoscopic partial nephrectomy (LPN) seems to be significantly better than OPN in terms of perioperative complications, estimated blood loss and hospital stay. Conversely, transfusion rate, ischemia time, change in estimated glomerular filtration rate and early cancer outcomes are similar between the two approaches. International guidelines recommend the use of both approaches according to the surgeon and patient preferences. so, we are plaining to do the study comparing between RAPN and LPN regarding feasibility and ability of both techniques. ### Conditions Module Conditions: - Renal Cell Carcinoma ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 20 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: cases of renal cell carcinoma , localized tumors , candidate for laparoscopic partial nephrectomy Intervention Names: - Procedure: laparoscopic partial nephrectomy Label: laparoscopic partial nephrectomy Type: OTHER #### Arm Group 2 Description: cases of renal cell carcinoma , localized tumors , candidate for robotic partial nephrectomy Intervention Names: - Procedure: robotic partial nephrectomy Label: robotic partial nephrectomy Type: OTHER ### Interventions #### Intervention 1 Arm Group Labels: - laparoscopic partial nephrectomy Description: cases amenable for partial nephrectomy Name: laparoscopic partial nephrectomy Type: PROCEDURE #### Intervention 2 Arm Group Labels: - robotic partial nephrectomy Description: cases amenable for partial nephrectomy Name: robotic partial nephrectomy Type: PROCEDURE ### Outcomes Module #### Primary Outcomes Description: to compare between laparoscopic and robotic partial nephrectomy regards ischemia time Measure: to compare between laparoscopic and robotic partial nephrectomy regards ischemia time Time Frame: 1 year #### Secondary Outcomes Description: compare between laparoscopic and robotic partial nephrectomy pathological safty margin Measure: compare between laparoscopic and robotic partial nephrectomy pathological safty margin Time Frame: 1 year ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * renal mass T1 according to TNM amenable for partial nephrectomy. Exclusion Criteria: * any unfit pt for partial nephrectomy * more than 7cm tumor * mass not amenable for partial nephrectomy * metastatic tumor or locally advanced Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: hossam elsayed kandeel, MSC Phone: 01097991198 Phone Ext: 002 Role: CONTACT #### Locations Location 1: City: Shibīn Al Kawm Contacts: *Contact 1:* - Email: [email protected] - Name: hossam elsayed kandeel, MSC - Phone: 01097991198 - Phone Ext: 002 - Role: CONTACT Country: Egypt Facility: Hossam Kandeel State: Menoufia - Status: RECRUITING Zip: 12345 #### Overall Officials Official 1: Affiliation: Director Name: hossam elsayed kandeel, MSC Role: STUDY_DIRECTOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000000230 - Term: Adenocarcinoma - ID: D000002277 - Term: Carcinoma - ID: D000009375 - Term: Neoplasms, Glandular and Epithelial - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000007680 - Term: Kidney Neoplasms - ID: D000014571 - Term: Urologic Neoplasms - ID: D000014565 - Term: Urogenital Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000052776 - Term: Female Urogenital Diseases - ID: D000005261 - Term: Female Urogenital Diseases and Pregnancy Complications - ID: D000091642 - Term: Urogenital Diseases - ID: D000007674 - Term: Kidney Diseases - ID: D000014570 - Term: Urologic Diseases - ID: D000052801 - Term: Male Urogenital Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: All - Name: All Conditions - Abbrev: BXS - Name: Urinary Tract, Sexual Organs, and Pregnancy Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M5534 - Name: Carcinoma - Relevance: LOW - As Found: Unknown - ID: M5548 - Name: Carcinoma, Renal Cell - Relevance: HIGH - As Found: Renal Cell Carcinoma - ID: M10703 - Name: Kidney Neoplasms - Relevance: LOW - As Found: Unknown - ID: M3585 - Name: Adenocarcinoma - Relevance: LOW - As Found: Unknown - ID: M12320 - Name: Neoplasms, Glandular and Epithelial - Relevance: LOW - As Found: Unknown - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M17320 - Name: Urologic Neoplasms - Relevance: LOW - As Found: Unknown - ID: M17315 - Name: Urogenital Neoplasms - Relevance: LOW - As Found: Unknown - ID: M2875 - Name: Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M27093 - Name: Female Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M14127 - Name: Pregnancy Complications - Relevance: LOW - As Found: Unknown - ID: M8399 - Name: Female Urogenital Diseases and Pregnancy Complications - Relevance: LOW - As Found: Unknown - ID: M10698 - Name: Kidney Diseases - Relevance: LOW - As Found: Unknown - ID: M17319 - Name: Urologic Diseases - Relevance: LOW - As Found: Unknown - ID: M27095 - Name: Male Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: T4906 - Name: Renal Cell Carcinoma - Relevance: HIGH - As Found: Renal Cell Carcinoma - ID: T1341 - Name: Clear Cell Renal Cell Carcinoma - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000002292 - Term: Carcinoma, Renal Cell ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424067 Brief Title: Study of Fingolimod Official Title: A Phase II Study of Fingolimod in Patients With Non-Small Cell and Small Cell Lung Cancer #### Organization Study ID Info ID: 103909 #### Organization Class: OTHER Full Name: Medical University of South Carolina ### Status Module #### Completion Date Date: 2027-05-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-05-31 Type: ESTIMATED #### Start Date Date: 2024-06-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-18 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Medical University of South Carolina #### Responsible Party Investigator Affiliation: Medical University of South Carolina Investigator Full Name: Mariam Alexander Investigator Title: Assistant Professor-Faculty Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Is US Export: True Oversight Has DMC: True ### Description Module Brief Summary: This is a single-institution, open-labeled study using fingolimod (FTY720/Gilenya) in patients with non-small cell lung cancer (NSCLC) and small cell lung cancer (SCLC) who have progressed on chemo-immunotherapy. The study design will be a 6 patient safety lead-in with 2 cohorts of patients for efficacy analysis where fingolimod 0.5 mg will be taken orally once daily. Detailed Description: Lung cancer is the second most common cancer and the leading cause of cancer death in the United States. There were approximately 237,000 new cases of lung cancer that were diagnosed in 2022 . The past decade has seen a revolution of new advances in the management of both non-small cell lung cancer (NSCLC) and small cell lung cancer (SCLC) with remarkable progress in screening, diagnosis, and treatment. The advances in systemic treatment have been driven primarily by the development of molecularly targeted therapeutics, immune-checkpoint inhibitors, and anti-angiogenic agents, all of which have transformed this field with significantly improved patient outcomes. Despite these advances, the prognosis for patients with advanced NSCLC and SCLC is poor, particularly after the failure of a platinum-based chemotherapy regimen and check point inhibitors with limited options available for patients. Therefore, new methods of targeting these malignancies are crucial. Fingolimod is a sphingosine analog that has demonstrated strong tumor suppressive activity in preclinical models of lung cancers and warrants further study. This proposed study is a single institution Phase II clinical trial to investigate the safety and efficacy of fingolimod in patients with NSCLC and SCLC. Fingolimod is a small molecule derived from myriocin that acts as a sphingosine analog. It is currently FDA-approved to treat patients with relapsing forms of multiple sclerosis (MS), including clinically isolated syndrome, relapsing-remitting disease, and active secondary progressive disease by binding to sphingosine-1-phosphate (S1P) receptors 1, 3, 4, and 5 causing T lymphocyte egression and retention in peripheral lymphoid organs leading to immunosuppression. However, it can act as an antagonist for the S1P receptor promoting tumor suppression in multiple cancer cell lines and mouse models inhibiting cell proliferation, and inducing cancer cell death. There are multiple studies demonstrating its activity in preclinical models of lung cancer. Fingolimod induces a type of programmed cell death called necroptosis in lung cancer cells. This is mediated by activation of the tumor suppressor protein phosphatase 2A (PP2A) through interaction with the PP2A inhibitor (I2PP2A). Specifically, work done using the adenocarcinoma cell line A549 and small cell carcinoma cell line H1341 showed that fingolimod-mediated stress induced the formation of ceramidosomes leading to plasma membrane blebbing, compromised membrane integrity, and necroptosis. This study will evaluate the safety, tolerability, and response rate in patients with NCSLC and SCLC who have progressed on front-line therapy including chemotherapy, immune checkpoint inhibitors, and targeted agents. It will contribute to the development of new methods for targeting these malignancies and provide insights into the potential use of fingolimod as a treatment option for these patients. ### Conditions Module Conditions: - Non Small Cell Lung Cancer - Small-cell Lung Cancer ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 38 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: n=22 NSCLC Any adult patients with lung cancer progressed on 2L+ systemic therapy n=any eligible patients from safety lead-in Intervention Names: - Drug: Fingolimod 0.5 milligram (mg) [Gilenya] Label: Efficacy in NSCLC Type: EXPERIMENTAL #### Arm Group 2 Description: n=16 SCLC Any adult patients with lung cancer progressed on 2L+ systemic therapy n=any eligible patients from safety lead-in Intervention Names: - Drug: Fingolimod 0.5 milligram (mg) [Gilenya] Label: Efficacy in SCLC Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Efficacy in NSCLC - Efficacy in SCLC Description: Oral fingolimod will be administered at a dose of 0.5 mg once a day. Name: Fingolimod 0.5 milligram (mg) [Gilenya] Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Number of Participants With Treatment-Related Adverse Events as Assessed by CTCAE v4.0. Measure: Safety of Fingolimod Time Frame: 6 months Description: To evaluate the objective response rate (ORR) (when measurable) according to RECIST 1.1 criteria Measure: Response Rate Time Frame: 6 months #### Secondary Outcomes Description: Progression-free survival (PFS) as measured from the date of the first study treatment to the date of the first objective documentation of radiographic disease progression or death due to any cause Measure: Progression-free Survival Time Frame: 6 months Description: Overall survival (OS) as measured from the date of first study treatment to the date of death due to any cause Measure: Overall Survival Time Frame: 6 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Voluntary, signed, and dated, Institutional Review Board (IRB) approved consent form in accordance with regulatory and institutional guidelines. * Stated willingness to comply with all study procedures and availability for the duration of the study. * Male or female * 18 years of age or older * Measurable/evaluable as defined by RECIST 1.1 at baseline of advanced/metastatic non-small cell lung cancer progressed on 2L+ systemic therapy with any molecular subtype and PD-L1 Tumor Proportion Score (TPS). * Measurable/evaluable as defined by RECIST 1.1 at baseline of extensive stage small cell lung cancer progressed on 2L+ systemic therapy. * Ability to take oral medication and be willing to adhere to the fingolimod regimen. * ECOG performance status 0-2 * Baseline lymphocyte count \>1000 cells/mL * For females of reproductive potential: use of highly effective contraception for at least 1 month before screening and agreement to use such a method during study participation and for an additional 2 months after the end of fingolimod administration. * For males of reproductive potential: use of condoms or other methods during and for an additional 2 months after the end of fingolimod treatment to ensure effective contraception with a partner. Exclusion Criteria: * Patients who have had a recent (within the last 6 months) occurrence of cardiac event including myocardial infarction, unstable angina, stroke, transient ischemic attack, decompensated heart failure requiring hospitalization, or New York Heart Association Class III or IV heart failure, and congenital long QT-syndrome * Patients who are receiving any medication(s) identified as having a Category D or higher interaction with the identified study agent who cannot be switched to another agent or discontinued before treatment if clinically appropriate. This medication review will be conducted by an oncology-trained Doctor of Pharmacy and discussed with the investigators before starting the treatment phase of this study. Careful evaluation for the following class of medications should be warranted due to their potential for severe side effects: * Concurrent therapy with QT-prolonging medications with a known risk of torsade de pointes * Concurrent therapy with drugs that slow heart rate or atrioventricular conduction * Concurrent therapy with antineoplastic, immunosuppressive, or immune-modulating therapies * Patients taking ketoconazole who have not completed their last dose at least 2 weeks before starting fingolimod. * Active untreated brain metastases. Patients are eligible if brain metastases are previously treated and are asymptomatic. Patients must be neurologically stable and must be on stable or tapering corticosteroids 2 weeks before Cycle 1 Day 1 * Patients who have a history or presence of Mobitz Type II 2nd-degree or 3rd-degree atrioventricular block or sick sinus syndrome, unless patients have a functioning pacemaker. * Patients who have a baseline QTc interval ≥ 500 msec * Patients who have cardiac arrhythmias requiring Class IA or Class III anti-arrhythmic drugs. * Class IA: disopyramide (Norpace), quinidine (Quinidex), procainamide (Procanbid) * Class III: dronedarone (Multaq), dofetilide (Tikosyn), sotalol (Betapace), ibutilide (Corvert), amiodarone (Nexterone) * Patients who have a hypersensitivity or allergic reaction (including rash, urticaria, and angioedema) to fingolimod or any of the excipients. * Patients who have an active, uncontrolled acute or chronic bacterial, viral, or fungal infection * Patients who have not completed all immunizations in accordance with current immunization guidelines before initiating fingolimod therapy * Unwillingness or inability to comply with procedures required in this protocol. * Patients who are currently participating in any other clinical trial of an investigational product * Female patients who are of child-bearing potential (WOCBP) who are pregnant, planning to become pregnant during the study, or lactating. A urine pregnancy test for WOCBP will be collected during the screening period. Females will be determined to be not of child-bearing potential with a history of hysterectomy, tubal ligation, or age 45 or older with postmenopausal status \> 12 months. Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Alan Brisendine Phone: 8437929007 Role: CONTACT Contact 2: Email: [email protected] Name: Jasmin Brooks Role: CONTACT ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012142 - Term: Respiratory Tract Neoplasms - ID: D000013899 - Term: Thoracic Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000008171 - Term: Lung Diseases - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000002283 - Term: Carcinoma, Bronchogenic - ID: D000001984 - Term: Bronchial Neoplasms ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M5546 - Name: Carcinoma, Non-Small-Cell Lung - Relevance: LOW - As Found: Unknown - ID: M11172 - Name: Lung Neoplasms - Relevance: HIGH - As Found: Lung Cancer - ID: M28323 - Name: Small Cell Lung Carcinoma - Relevance: HIGH - As Found: Small Cell Lung Cancer - ID: M5534 - Name: Carcinoma - Relevance: LOW - As Found: Unknown - ID: M14979 - Name: Respiratory Tract Neoplasms - Relevance: LOW - As Found: Unknown - ID: M16658 - Name: Thoracic Neoplasms - Relevance: LOW - As Found: Unknown - ID: M11168 - Name: Lung Diseases - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: M5540 - Name: Carcinoma, Bronchogenic - Relevance: LOW - As Found: Unknown - ID: M5260 - Name: Bronchial Neoplasms - Relevance: LOW - As Found: Unknown - ID: T5271 - Name: Small Cell Lung Cancer - Relevance: HIGH - As Found: Small Cell Lung Cancer ### Condition Browse Module - Meshes - ID: D000008175 - Term: Lung Neoplasms - ID: D000055752 - Term: Small Cell Lung Carcinoma ### Intervention Browse Module - Ancestors - ID: D000081243 - Term: Sphingosine 1 Phosphate Receptor Modulators - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000007166 - Term: Immunosuppressive Agents - ID: D000007155 - Term: Immunologic Factors - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M323 - Name: Fingolimod Hydrochloride - Relevance: HIGH - As Found: Staining - ID: M10212 - Name: Immunosuppressive Agents - Relevance: LOW - As Found: Unknown - ID: M10201 - Name: Immunologic Factors - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000068876 - Term: Fingolimod Hydrochloride ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424054 Acronym: eChemoCoach Brief Title: Mitigating Toxicity by Electronic Health Portal-mediated Interactive Monitoring of Patient-reported Side Effects Official Title: Mitigating Toxicity of (Neo)Adjuvant Chemotherapy by Applying Electronic Health Portal-mediated Interactive Monitoring of Patient-reported Side Effects: the Prospective Randomized eChemoCoach Trial #### Organization Study ID Info ID: 2023-01/15741 (KWF-grant) #### Organization Class: OTHER Full Name: Noordwest Ziekenhuisgroep ### Status Module #### Completion Date Date: 2029-12-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2029-06-01 Type: ESTIMATED #### Start Date Date: 2025-06-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-09 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Comprehensive Cancer Centre The Netherlands Class: OTHER Name: University of Twente Class: OTHER Name: Dutch Cancer Society Class: NETWORK Name: Borstkanker Onderzoek Groep #### Lead Sponsor Class: OTHER Name: Noordwest Ziekenhuisgroep #### Responsible Party Investigator Affiliation: Noordwest Ziekenhuisgroep Investigator Full Name: Mathijs Hendriks, MD Investigator Title: Principal investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Chemotherapy induces side effects varying in severity, impacting patients' quality of life and necessitating unplanned hospital care. Patient-reported outcomes (PROs) could aid in early detection and management of side effects. However, existing PRO monitoring lacks triage capabilities, leading to clinician involvement and suboptimal symptom management. The investigators propose eChemoCoach, an electronic questionnaire integrated into the electronic health portal, offering real-time symptom assessment and personalized advice based on CTCAE criteria. Our study aims to assess the impact of eChemoCoach on non-hematological CTCAE ≥ 3 graded side effects in early breast cancer patients undergoing chemotherapy. This is a randomized controlled trial involving 746 patients that will evaluate the eChemoCoach's efficacy compared to standard monitoring. Phase one will validate questionnaires and assess usability, while phase two focuses on the primary outcome. Te investigators anticipate reduced severe side effects, thereby enhancing patients' quality of life, reducing stress, and minimizing hospital visits. Detailed Description: Problem description: The aim of (neo)adjuvant chemotherapy is to increase survival. Therefore, treatment adherence is important. However, patients may experience treatment-related side-effects. In current practice, clinicians evaluate toxicity just a few days before the next chemotherapy is scheduled. Monitoring and timely anticipation of chemotherapy related side-effects may prevent escalation of toxicity, increase treatment adherence and reduce the decline in quality of life. Evaluating toxicity more frequently and on-demand could be a solution to reduce severe toxicity. Therefore, patients should receive a direct advice when experiencing side-effects. However, without interference of a health care professional, this is not possible in standard care. Solution / research direction: There is increasing evidence that incorporating patient reported outcomes (PROs) in clinical care enhances symptom monitoring in cancer patients. Therefore, it is desirable to develop and investigate an electronic smart-phrased side-effects questionnaire which: 1) delivers a real-time personalized advice to the patient, based on CTCAE grading, after the questionnaire is completed and 2) is accessible for patients using an electronic health portal (EHP) of the electronic health record (EHR) to integrate the PRO data into the EHR. Aim / hypothesis: To investigate the effect of adding weekly EHP-mediated monitoring of chemotherapy related side-effects based on CTCAE grading using smart-phrased electronic PRO side-effects questionnaires to standard of care monitoring of side-effects, on the occurrence of CTCAE \>= grade 3 toxicity. Plan of investigation: To conduct a pilot study to validate the smart-phrased ePRO side-effects questionnaire. Thereafter, a multicenter clinical randomized trial will start where patients with breast cancer qualifying for (neo)adjuvant chemo(immune)therapy will be randomized to real-time EHP-mediated monitoring of side-effects using a novel smart-phrased ePRO side-effects questionnaire in addition to standard of care monitoring, or to standard of care monitoring solely. Primary objective is the overall rate of CTC grade \>=3 non hematological toxicity between both arms. Secondary objectives include relative dose intensity, health-related quality of life, experienced distress, the number of unplanned health care usage and costs. Expected outcome: The investigators hypothesize that adding weekly EHP-mediated monitoring of side-effects using ePRO side-effects questionnaires will significantly lower the occurrence rate of CTCAE grade \>=3 non-hematological toxicities. ### Conditions Module Conditions: - Breast Cancer - eHealth - Symptom Monitoring - Self Management Keywords: - Breast Cancer - remote monitoring - emonitoring - eHealth - symptom management - symptom monitoring ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: A clinical randomized controlled trial will be performed in 746 breast cancer patients treated with (neo-)adjuvant chemotherapy. Patients will be randomized to the intervention group, using the eChemoCoach in addition to standard of care monitoring to manage side effects or are randomized to solely standard of care monitoring. ##### Masking Info Masking: NONE Masking Description: This is a open label study since blinding is not possible as healthcare professionals will receive the CTC gradation based on the reported side effects in the intervention group and are obligated to act on these reports. Primary Purpose: PREVENTION #### Enrollment Info Count: 746 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients assigned to the intervention arm fill in the eChemoCoach questionnaires. They will be asked to report their side effects at baseline (2 - 4 days before their first chemotherapy cycle) and weekly thereafter. Moreover, they can report their symptoms at any time in case of potential toxicity, with a maximum of once a day. Non-responders receive reminders. Both intervention and control groups receive standard monitoring and coaching, including pre-scheduled checks for side effects before chemotherapy. Patients in both groups are asked to complete questionnaires measuring the impact on HRQoL, anxiety, distress, and patient empowerment at baseline, 10 weeks, and 20 weeks post-chemotherapy initiation. Usability of the eChemoCoach will be assessed through an online survey for patients and healthcare professionals using the System Usability Scale Intervention Names: - Other: eChemoCoach Label: eChemoCoach Group Type: EXPERIMENTAL #### Arm Group 2 Description: Patients in the control group receive standard of care. Both intervention and control groups receive standard monitoring and coaching, including pre-scheduled checks for side effects before chemotherapy. Patients in both groups are asked to complete questionnaires measuring the impact on HRQoL, anxiety, distress, and patient empowerment at baseline, 10 weeks, and 20 weeks post-chemotherapy initiation. Label: Control group Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - eChemoCoach Group Description: the eChemoCoach is an electronic questionnaire which is accessible for patients via the secured electronic health portal (EHP) of the EHR, which is CE-certified. By utilizing the eChemoCoach, patients (for this project we focus on breast cancer patients) have the ability to complete a questionnaire on a daily basis, when experiencing side effects. The eChemoCoach has the potential to evaluate the severity of adverse effects based on the CTCAE criteria and triage them, mimicking the decision-making process of a HCP through computer adaptive testing (CAT). Upon completing the questionnaire, the eChemoCoach translates the responses for each specific side effect into corresponding CTCAE grades. The tool then promptly offers patients personalized advice, tailored to their individual condition. Name: eChemoCoach Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The occurrence of any non-hematological side effects grade ≥3 during neo-adjuvant or adjuvant treatment Measure: The occurrence of any non-hematological side effects grade ≥3 Time Frame: Up to 30 weeks after start chemotherapy #### Secondary Outcomes Description: Time to occurrence of both grade 2 and grade ≥3 toxicity will be analyzed with a Kaplan-Meier curves. Occurrence of grade 2 side effects during (neo)adjuvant will be presented as numbers with percentages for patients in both study groups. Measure: Toxicity patterns Time Frame: Up to 30 weeks after start chemotherapy Description: For analyzing the RDI, the RDI will be calculated for each chemotherapeutic agent and presented as mean with standard deviations (SD) (for a description of calculation of the RDI see the objective section paragraph 2.0). The RDI will be calculated per cycle. The RDI will be compared between the intervention and the control group. Measure: Relative dose intensity (RDI) Time Frame: Up to 30 weeks after start chemotherapy Description: Health-related quality of life measured by the Quality of Life Questionnaire (QLQ-C30s). Scale is ranging from 1 to 4. 1 = not at all, 4 = very much. Higher scores mean a worse QOL. Measure: HRQOL Time Frame: on baseline, 10 and 20 weeks after start of chemotherapy Description: Patient experienced anxiety measured using the Hospital Anxiety and Depression Scale. Scale is ranging from 0 to 3. 0 = often, 3 = never. Higher scores means a less worse Hads score. Measure: Patient experienced anxiety Time Frame: on baseline, 10 and 20 weeks after start of chemotherapy Description: Patient empowerment using Patient Activation Measure (PAM13) questionnaire. Ranging from 0 to 3. 0 = I do not agree, 3= I totally agree. A lower score is worse. Measure: Patient empowerment Time Frame: on baseline, 10 and 20 weeks after start of chemotherapy Description: Patient experienced stress using a distress thermometer. Ranging from 0 to 10 per problem. 0 = no problem, 10 = worst. A higher score means more stress. Measure: Patient experienced stress Time Frame: on baseline, 10 and 20 weeks after start of chemotherapy Description: The amount of unplanned hospital care will be presented as median (IQR) and will be analyzed by comparing the number of admissions, unplanned visits, days of hospital admissions between the intervention and control group using Poisson regression analysis. Measure: Unplanned Care Time Frame: Up to 30 weeks after start chemotherapy Description: Cognitive interviews will be analyzed with thematic content analysis. Agreement between professional triage estimations and eChemoCoach will be quantified using Cohen's Kappa coefficient. A semi qualitative assessment will be conducted, comparing the patient-reported adverse effects using eChemoCoach with medical professionals' CTCAE severity assessments. Interviews will be analyzed with thematic content analysis. Measure: Validation of eChemoCoach questionnaires Time Frame: During the first year of the study Description: The System Usability Scale will be used for global assessment of the eChemoCoach. usability. Usability will also be assessed by healthcare professionals from participating. sites. The SUS is a 10 item questionnaire with 5 response options. Ranging from strongly disagree to strongly agree. The average SUS score from all 500 studies is a 68. A SUS score above a 68 would be considered above average and anything below 68 is below average. Measure: Usability Time Frame: After inclusion of all intervention patients Description: To assess the concordance among eChemoCoach-reported grades, PRO-CTCAE, and CTCAEs graded by healthcare professionals (HCPs), we employ the eChemoCoach platform for patient experienced symptom data collection. Each questionnaire administered includes the eChemoCoach and the PRO-CTCAE questionnaire, facilitating immediate and direct comparison of both outcomes. HCPs will document symptom grading in patient files using standardized CTCAE forms. HCPs will grade the severity on pre-planned checks (standard of care) and when necessary in case of severe side effects. Measure: Agreement eChemoCoach-reported grades and those reported by PRO-CTCAE, HCPs, and the Dutch translation of CTCAE Time Frame: Up to 30 weeks after start chemotherapy ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * - Starting (neo)adjuvant treatment with chemotherapy for breast cancer according to one of the below mentioned treatment protocols: * Four cycles of doxorubicin 60mg/m2 and cyclophosphamide 600mg/m2 (AC) dose dense q 2 weeks, followed by twelve cycles of weekly paclitaxel 80mg/m2 (also in combination with carboplatin AUC6 q 3 weeks) * Nine cycles q 3 weeks of paclitaxel 80mg/m2 on day 1 and 8, carboplatin AUC 3 on day 1 and 8, trastuzumab 8mg/kg loading dose (followed by doses of 6mg/m2 at subsequent cycles) on day1 and pertuzumab loading dose of 840mg (followed by doses of 420mg at subsequent cycles) on day 1 * Age ≥ 18 years * WHO PS ≤1 * Capable of using the EHP or get help in case of low (e-)health literacy. This includes being capable of login using DigiD, a system used by the Dutch government to verify the identity of a person * Being able to read or get help from a relative in case of illiteracy Exclusion Criteria: * - Participation in a trial with an investigational product (because more frequent and structured symptom reporting is performed in these studies). * Patients who have been treated with chemotherapy in the past (since these patients are at higher risk for developing side effects of current chemotherapy). * Patients that already started with their chemotherapy cycle Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Manon Hanrath-Komen, PhD Phone: 0031 72 5482872 Role: CONTACT Contact 2: Email: [email protected] Name: Rubin Verduin, drs Phone: 0625289930 Role: CONTACT ### IPD Sharing Statement Module IPD Sharing: YES ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000001941 - Term: Breast Diseases - ID: D000012871 - Term: Skin Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC17 - Name: Skin and Connective Tissue Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M5220 - Name: Breast Neoplasms - Relevance: HIGH - As Found: Breast Cancer - ID: M5218 - Name: Breast Diseases - Relevance: LOW - As Found: Unknown - ID: M15674 - Name: Skin Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000001943 - Term: Breast Neoplasms ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424041 Acronym: FM-FMT-RCT Brief Title: Fecal Microbiome Transplantation From Healthy Donors to Individuals With Fibromyalgia Official Title: Fecal Microbiome Transplantation From Healthy Donors to Individuals With Fibromyalgia: A Prospective Randomized, Controlled Double-Blind Study #### Organization Study ID Info ID: 0521-23 #### Organization Class: OTHER Full Name: Rambam Health Care Campus #### Secondary ID Infos Domain: Weston Family Foundation ID: Weston Family Foundation Type: OTHER_GRANT Domain: Israel Science Foundation ID: Israel Science Foundation Type: OTHER_GRANT ### Status Module #### Completion Date Date: 2027-03 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: ENROLLING_BY_INVITATION #### Primary Completion Date Date: 2026-03 Type: ESTIMATED #### Start Date Date: 2024-03-11 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-09 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Rambam Health Care Campus #### Responsible Party Investigator Affiliation: Rambam Health Care Campus Investigator Full Name: Amir Minerbi MD Investigator Title: Deputy Director Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This study aims to investigate if a fecal microbiome transplantation (FMT) from healthy donors can reduce symptoms of fibromyalgia, a condition causing chronic pain that is difficult to treat and diagnose. Changes in the gut bacteria of women with fibromyalgia were previously reported, which might be linked to their symptoms. In mice studies, transferring gut bacteria from individuals with fibromyalgia was shown to increase sensitivity to pain, while treatment with antibiotics and transferring bacteria from healthy individuals reversed this effect. In a small open label trial in women, improvements in pain, fatigue, and sleep problems were observed after FMT. The investigators aim to perform a larger trial following a similar path. The study aims to conduct a double-blinded, randomized, placebo-controlled trial involving 80 women diagnosed with severe fibromyalgia. Half of the participants (40) will receive the active treatment, while the other half (40) will receive a sham treatment. The allocation to either group will be randomized. Throughout the study period, both the caregivers and the participants will remain unaware of their assigned groups until the study conclusion. Participants' symptoms will be documented and their blood and stool will be tested for changes in certain metabolites. If this treatment works, it could be a significant breakthrough in managing fibromyalgia and might provide new insights into its causes. Detailed Description: A double-blind, randomized placebo-controlled study to test the therapeutic potential of encapsulated oral fecal microbiota transplantation (FMT) from healthy donors to humans with fibromyalgia. Fibromyalgia, a chronic and debilitating syndrome characterized by widespread pain, fatigue, sleep disturbances, and cognitive dysfunction poses a significant clinical, social, and economic burden globally, with limited targeted treatment options available. Recent studies have shed light on the potential role of the gut microbiome in fibromyalgia pathogenesis, highlighting alterations in gut microbiome composition correlated with clinical indices of the syndrome. Building upon this knowledge, the study seeks to explore the therapeutic potential of FMT, a well-established treatment increasingly investigated across various medical conditions. Preclinical investigations in mice have shown that FMT from fibromyalgia patients induces symptoms of the syndrome, while FMT from healthy controls reverses them. Encouragingly, preliminary results from an open-label pilot clinical trial involving fibromyalgia patients receiving encapsulated oral FMT from healthy donors demonstrated significant improvements in pain intensity, symptomatic burden, and quality of life measures, with favorable safety profiles. Based on these promising findings, a prospective randomized, controlled double-blind study is proposed to further evaluate the efficacy and safety of encapsulated oral FMT from healthy individuals in fibromyalgia patients. Clinical outcomes, as well as stool and serum samples, will be extensively characterized to elucidate the mechanisms underlying the effects of FMT, including its modulation of gut microbiome composition and function. The hypotheses involve expecting clinically significant improvements in pain and other symptoms of fibromyalgia following FMT, alongside corresponding alterations in gut microbiome composition and metabolomics profiles. This study aims to contribute valuable insights into the potential role of FMT as a novel therapeutic approach for fibromyalgia, addressing an unmet need in the management of this challenging condition. ### Conditions Module Conditions: - Fibromyalgia Keywords: - Fibromyalgia - Fecal Microbiome Transplantation (FMT) - Microbiome - Chronic Pain ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: A Double-Blinded, Randomized Placebo-Controlled Trial ##### Masking Info Masking: QUADRUPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 100 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants in this arm will receive a total of 5 real FMT treatments administered weekly, followed by an additional 5 maintenance FMT treatments on a monthly basis. The first induction treatment will consist of 30 grams, with subsequent treatments comprising 15 grams each. Intervention Names: - Other: Fecal Microbiome Transplantation Label: Active Treatment - FMT Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: Participants in this arm will receive a total of 5 sham FMT treatments administered weekly, followed by an additional 5 maintenance sham FMT treatments on a monthly basis. The first induction treatment will consist of 30 grams, with subsequent treatments comprising 15 grams each. Intervention Names: - Other: Sham Fecal Microbiome Transplantation Label: Sham Treatment - FMT Type: SHAM_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Active Treatment - FMT Description: Healthy donor fecal microbiome transplantation, following depletion of the endogenous microbial communities using antibiotics and bowel cleansing Name: Fecal Microbiome Transplantation Type: OTHER #### Intervention 2 Arm Group Labels: - Sham Treatment - FMT Description: Capsules containing preservative solution only, following depletion of the endogenous microbial communities using antibiotics and bowel cleansing Name: Sham Fecal Microbiome Transplantation Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Pain intensity will be assessed using the Visual Analogue Scale (VAS), with a score of zero indicating no pain and a score of 10 representing the worst possible pain. Measure: Pain intensity at week five post-transplantation Time Frame: Week five post transplantation induction #### Secondary Outcomes Description: As measured using the Fibromyalgia Impact Questionnaire (range 0-100, higher scores indicate worse symptoms) Measure: overall symptomatic burden Time Frame: Week five post transplantation induction and then on months 1, 3, 6 after last FMT Description: As assessed by the Hospital Anxiety and Depression Scale questionnaire (range 0-21 for each of the domains, higher scores indicate worse symptoms) Measure: Anxiety and depression Time Frame: Week five post transplantation induction and then on months 1, 3, 6 after last FMT Description: As assessed by the Pittsburgh Sleep Quality Inventory (range 0-21, higher scores indicate worse sleep quality). Measure: Sleep quality Time Frame: Week five post transplantation induction and then on months 1, 3, 6 after last FMT Description: Pressure, heat and cold pain thresholds (Kg/cm\^2, degrees C respectively, lower thresholds indicate increased pain sensitivity) Measure: Quantitative Sensory Testing Time Frame: Week five post transplantation induction and then on months 1, 3, 6 after last FMT ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Adult women aged 18-75 years. 2. Diagnosis of fibromyalgia confirmed according to the 2016 diagnostic criteria by a pain physician who is a part of the study team. 3. An average reported pain of 6 or above during the preceding week. 4. Has remained symptomatic despite receiving standard care for fibromyalgia. Exclusion Criteria: 1. Any active inflammatory condition (rheumatic, gastrointestinal or other). 2. Malignant neoplasm in the preceding 5 years. 3. Immunosuppression due to medical condition or treatment. 4. Uncontrolled psychiatric pathology. 5. Any other clinically important condition at the discretion of the investigator. 6. Known allergy to the antibiotics or laxatives used in the preparation protocol, or severe food allergy. 7. Active infection or expected antibiotic treatment in the upcoming 3 months after inclusion. 8. Pregnancy or intention to conceive. Maximum Age: 75 Years Minimum Age: 18 Years Sex: FEMALE Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Haifa Country: Israel Facility: Rambam Health Care Campus State: North Zip: 3109601 #### Overall Officials Official 1: Affiliation: Rambam Health Care Campus Name: Amir Minerbi, MD-PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009135 - Term: Muscular Diseases - ID: D000009140 - Term: Musculoskeletal Diseases - ID: D000012216 - Term: Rheumatic Diseases - ID: D000009468 - Term: Neuromuscular Diseases - ID: D000009422 - Term: Nervous System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC05 - Name: Musculoskeletal Diseases - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC17 - Name: Skin and Connective Tissue Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M29442 - Name: Chronic Pain - Relevance: LOW - As Found: Unknown - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M8486 - Name: Fibromyalgia - Relevance: HIGH - As Found: Fibromyalgia - ID: M12161 - Name: Myofascial Pain Syndromes - Relevance: HIGH - As Found: Fibromyalgia - ID: M16355 - Name: Syndrome - Relevance: LOW - As Found: Unknown - ID: M12092 - Name: Muscular Diseases - Relevance: LOW - As Found: Unknown - ID: M12097 - Name: Musculoskeletal Diseases - Relevance: LOW - As Found: Unknown - ID: M15045 - Name: Rheumatic Diseases - Relevance: LOW - As Found: Unknown - ID: M6323 - Name: Collagen Diseases - Relevance: LOW - As Found: Unknown - ID: M12411 - Name: Neuromuscular Diseases - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000005356 - Term: Fibromyalgia - ID: D000009209 - Term: Myofascial Pain Syndromes ### Intervention Browse Module - Browse Branches - Abbrev: Infe - Name: Anti-Infective Agents - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: PhSol - Name: Pharmaceutical Solutions ### Intervention Browse Module - Browse Leaves - ID: M4222 - Name: Anti-Bacterial Agents - Relevance: LOW - As Found: Unknown - ID: M21860 - Name: Pharmaceutical Solutions - Relevance: LOW - As Found: Unknown - ID: M4224 - Name: Antibiotics, Antitubercular - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424028 Brief Title: Acute Right Ventricular Infarction Registry Official Title: Presentation, Management, Hospital-course, and Prognosis of Acute Right Ventricular Infarction: A Prospective Registry of Patients Presenting to the Largest Primary Percutaneous Coronary Intervention Centre of Pakistan #### Organization Study ID Info ID: IRB-62/2023 #### Organization Class: OTHER Full Name: National Institute of Cardiovascular Diseases, Pakistan ### Status Module #### Completion Date Date: 2024-08-19 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-07-19 Type: ESTIMATED #### Start Date Date: 2024-01-20 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-10 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: National Institute of Cardiovascular Diseases, Pakistan #### Responsible Party Investigator Affiliation: National Institute of Cardiovascular Diseases, Pakistan Investigator Full Name: Dr. Rajesh Kumar Investigator Title: Associate Professor Adult Cardiology Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This Study aims to provide an assessment of clinical presentation, management, hospital course, and prognosis of acute right ventricular infarction presenting with or without Inferior or infero-posterior wall Myocardial Infarction and the assessment of composite adverse clinical outcome after reperfusion in-hospital and post-discharge (in 30 Days Prognosis). Detailed Description: After fulfilling the eligibility criteria, informed consent will be obtained from all the patients regarding using data for research while maintaining anonymity.Data will be collected for various patient, system, and procedure related characteristics with the help of a predefined structured proforma consisted of demographic data, clinical presentation, history and co-morbid conditions, and angiographic and procedural characteristics. All the recruited patients will be kept under observiton during the hospital stay and a telephonic follow-up will be carried out after 30-days of discharge and occurrence of the MACE will be recorded. Univariate and multivariable binary logistic regression analysis will be performed to determine the clinical predictors of RVI. Odds ratio (OR) along with 95% confidence interval (CI) will be reported. The statistical significance criteria will be set as p-value\<0.05. For data verification, 10% of the data will be cross-checked with the source document (Patient file). ### Conditions Module Conditions: - Inferior Wall; Transmural Myocardial Infarction - Right Ventricular Dysfunction ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 1000 Type: ESTIMATED Patient Registry: True Study Type: OBSERVATIONAL Target Duration: 30 Days ### Arms Interventions Module ### Interventions #### Intervention 1 Description: Consecutive patients presented with isolated inferior, infero-posterior and inferolateral wall MI with or without acute right ventricular infarction. Name: Right Ventricular Infarct Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Atleast one adverse event, such as pump failure, cerebrovascular accident (CVA), stent thrombosis, major bleeding, contrast-induced nephropathy (CIN), ventricular arrhythmias, or mortality. Measure: Composite adverse clinical outcome Time Frame: Upto 30 days from admission ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Patients of Inferior, infero-lateral and infero-posterior wall MI with and without RV infarction undergoing PPCI. * Both male and female patients. * Patients of age ≥ 18 years. Exclusion Criteria: • Patients who will not give consent for participation. Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Patients presented at a tertiary care hospital with Inferior and posterior wall MI with and without RV infarction undergoing PPCI who are fulfilling the eligibility criteria will be enrolled. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Rajesh Kumar, MBBS, FCPS Phone: +923337306090 Role: CONTACT Contact 2: Email: [email protected] Name: Musa Karim, MSc Phone: 03323646169 Role: CONTACT #### Locations Location 1: City: Karachi Contacts: *Contact 1:* - Email: rajeshnarsoolal@@gmail.com - Name: Rajesh Kumar, MBBS, FCPS - Phone: +923337306090 - Role: CONTACT Country: Pakistan Facility: National Institute of Cardiovascular Diseases State: Sindh Status: RECRUITING Zip: 75510 #### Overall Officials Official 1: Affiliation: National Institute of Cardiovascular Diaseses Name: Rajesh Kumar, MBBS, FCPS Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Description: The Hospital Medical Record number will be used as the patient identifier. IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000007511 - Term: Ischemia - ID: D000010335 - Term: Pathologic Processes - ID: D000009336 - Term: Necrosis - ID: D000017202 - Term: Myocardial Ischemia - ID: D000006331 - Term: Heart Diseases - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000014652 - Term: Vascular Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M12155 - Name: Myocardial Infarction - Relevance: HIGH - As Found: Myocardial Infarction - ID: M10282 - Name: Infarction - Relevance: HIGH - As Found: Infarction - ID: M20824 - Name: Ventricular Dysfunction - Relevance: HIGH - As Found: Ventricular Dysfunction - ID: M20601 - Name: Ventricular Dysfunction, Right - Relevance: HIGH - As Found: Right Ventricular Dysfunction - ID: M10543 - Name: Ischemia - Relevance: LOW - As Found: Unknown - ID: M12284 - Name: Necrosis - Relevance: LOW - As Found: Unknown - ID: M6546 - Name: Coronary Artery Disease - Relevance: LOW - As Found: Unknown - ID: M19506 - Name: Myocardial Ischemia - Relevance: LOW - As Found: Unknown - ID: M9419 - Name: Heart Diseases - Relevance: LOW - As Found: Unknown - ID: M17400 - Name: Vascular Diseases - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000009203 - Term: Myocardial Infarction - ID: D000018754 - Term: Ventricular Dysfunction - ID: D000018497 - Term: Ventricular Dysfunction, Right - ID: D000007238 - Term: Infarction ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424015 Brief Title: Insulin and Insulin Pulses During Fasting Official Title: Effect of Insulin and Insulin Pulses on Fasting Glucagon Secretion and on Glucose Metabolism in Subjects Without Type 2 Diabetes #### Organization Study ID Info ID: 24-002631 #### Organization Class: OTHER Full Name: Mayo Clinic ### Status Module #### Completion Date Date: 2027-09-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-09-01 Type: ESTIMATED #### Start Date Date: 2024-09-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-13 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Mayo Clinic #### Responsible Party Investigator Affiliation: Mayo Clinic Investigator Full Name: Adrian Vella Investigator Title: Professor of Medicine Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Fasting hyperglycemia contributes disproportionately to nonenzymatic glycosylation and the microvascular complications of type 2 diabetes. However, little is known about the regulation of glucose concentrations in the fasting state relative to what is known about the postprandial state. The proposed experiment is part of a series of experiments designed to establish how glucagon and insulin interact with their receptors to control fasting glucose in health and in prediabetes. Detailed Description: Decreased insulin action increases glucagon concentrations. In rodents, insulin signaling restrains glucagon secretion. It is unclear if this is the case in all (subtypes of) prediabetes. Impaired hepatic insulin action exacerbates glucagon's effects on endogenous glucose production. Also, insulin resistance in the β-cell impairs negative feedback inhibition of insulin secretion. This leads to hyperinsulinemia in rodents and humans. How these variables interact is unknown. This experiment will determine how insulin variably regulates fasting glucagon (and insulin) secretion directly, or indirectly, in prediabetes. The inability of the proinsulin to insulin ratio to reliably predict β-cell integrity, endoplasmic reticulum stress and β-cell function has led to the identification of novel markers of β-cell health. In addition, the relationship of glucagon and insulin pulses will be quantified. Preliminary data shows that there is heterogeneity in these relationships even in normal fasting glucose. Th experiment will also determine how islet hormone / glucose crosstalk and pulse characteristics contribute to prediabetes. ### Conditions Module Conditions: - PreDiabetes Keywords: - insulin secretion - glucagon secretion - endogenous glucose production - glucose disappearance ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: CROSSOVER ##### Masking Info Masking: NONE Primary Purpose: BASIC_SCIENCE #### Enrollment Info Count: 60 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Between 0600 (-180 min) and 1300 (240 min) Intralipid (20%, 0.011ml/kg/min; Baxter, Healthcare, Deerfield, IL) and heparin (200 units prime, 0.2 unit/kg/min continuous) will be infused to induce acute insulin resistance. Intervention Names: - Other: Intralipid and heparin Label: Intralipid and heparin Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: Between 0600 (-180 min) and 1300 (240 min) saline will be infused Intervention Names: - Other: Saline Label: Saline Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Intralipid and heparin Description: Intralipid (20%, 0.011ml/kg/min; Baxter, Healthcare, Deerfield, IL) and heparin (200 units prime, 0.2 unit/kg/min continuous) will be infused to induce acute insulin resistance Name: Intralipid and heparin Type: OTHER #### Intervention 2 Arm Group Labels: - Saline Description: Saline will be infused Name: Saline Type: OTHER ### Outcomes Module #### Primary Outcomes Description: comparison of EGP in people with IFG vs NFG in response to insulin infusion Measure: Suppression of Endogenous glucose production (EGP) by insulin Time Frame: The rate of EGP at 240 minutes (end of study) expressed as a percentage of fasting EGP (at the start of the study i.e.: 0 minutes. Description: comparison of Insulin pulse orderliness measured by approximate entropy in people with IFG vs NFG Measure: Insulin pulse orderliness Time Frame: Approximate Entropy (ApEn) will be calculated from the insulin concentrations observed every 2 minutes between -45 and 0 minutes ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * people with normal or impaired fasting glucose and normal or impaired glucose tolerance Exclusion Criteria: 1. HbA1c \> 6.5% 2. BMI ≥ 35 Kg/M2 3. Use of any glucose-lowering agents including metformin or sulfonylureas. 4. For female subjects: positive pregnancy test at the time of enrollment or study 5. History of prior upper abdominal surgery such as adjustable gastric banding, pyloroplasty and vagotomy. 6. Active systemic illness or malignancy. 7. Symptomatic macrovascular or microvascular disease. 8. Hematocrit \< 35% Healthy Volunteers: True Maximum Age: 65 Years Minimum Age: 25 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Kim Osmundson, CCRP Phone: 507-255-0907 Role: CONTACT Contact 2: Email: [email protected] Name: Jeanette Laugen Phone: 507-255-8110 Role: CONTACT #### Locations Location 1: City: Rochester Country: United States Facility: Mayo Clinic in Rochester State: Minnesota Zip: 55905 #### Overall Officials Official 1: Affiliation: Mayo Clinic Name: Adrian Vella, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: The data being shared is human data from clinical trials and therefore a higher level of protection is required. Access to this data will be controlled by a managed access process whereby access is provided only after approval. Data will be controlled access with the General Research Use Data Use Limitation, as allowed by the informed consent and the institutional certification. Description: Data that will be preserved and shared include results of screening labs, immunoassay data and glucose turnover data. In addition, we will share the study protocol, statistical analysis plan, a data dictionary and anonymization guidance (methodology to anonymize data).In addition to the patient-level data, the metadata, data dictionary, statistical analysis plan, and final protocol will be shared. The sharing of the data dictionary, statistical analysis plan and final protocol with amendments will enable researchers to understand how the data was collected and to correctly interpret the data for future secondary analysis. The final patient level dataset will include demographics as well as screening data and primary and secondary outcomes.We plan to share datasets resulting from the proposed studies in Vivli, a non-profit institution that supports the Vivli repository. Info Types: - STUDY_PROTOCOL - SAP - ICF - CSR - ANALYTIC_CODE IPD Sharing: YES Time Frame: The data shared will be archived and available on the platform for request by researchers for a minimum of 10 years after contribution. Data will be made accessible no later than the time of our associated publication or the end of the grant period (whichever comes first). On an ongoing basis, Vivli evaluates its data holdings regarding maintaining access and reserves the right to discontinue the distribution of a data collections when deemed appropriate. When materials are deaccessioned, the data are no longer publicly accessible at Vivli, they may still be preserved in Vivli's storage vault. Because digital files are assigned a persistent digital object identifier (DOI), the study description is still available to view, but is not searchable through Vivli. ## Derived Section ### Condition Browse Module - Ancestors - ID: D000003920 - Term: Diabetes Mellitus - ID: D000044882 - Term: Glucose Metabolism Disorders - ID: D000008659 - Term: Metabolic Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M14117 - Name: Prediabetic State - Relevance: HIGH - As Found: Prediabetes - ID: M20295 - Name: Glucose Intolerance - Relevance: LOW - As Found: Unknown - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M7119 - Name: Diabetes Mellitus, Type 2 - Relevance: LOW - As Found: Unknown - ID: M11639 - Name: Metabolic Diseases - Relevance: LOW - As Found: Unknown - ID: M25403 - Name: Glucose Metabolism Disorders - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000011236 - Term: Prediabetic State ### Intervention Browse Module - Ancestors - ID: D000000925 - Term: Anticoagulants - ID: D000005343 - Term: Fibrinolytic Agents - ID: D000050299 - Term: Fibrin Modulating Agents - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000005217 - Term: Fat Emulsions, Intravenous - ID: D000057947 - Term: Parenteral Nutrition Solutions - ID: D000019999 - Term: Pharmaceutical Solutions ### Intervention Browse Module - Browse Branches - Abbrev: Hypo - Name: Hypoglycemic Agents - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Gast - Name: Gastrointestinal Agents - Abbrev: FiAg - Name: Fibrinolytic Agents - Abbrev: AnCoag - Name: Anticoagulants - Abbrev: PhSol - Name: Pharmaceutical Solutions - Abbrev: HB - Name: Herbal and Botanical ### Intervention Browse Module - Browse Leaves - ID: M10365 - Name: Insulin - Relevance: LOW - As Found: Unknown - ID: M173166 - Name: Insulin, Globin Zinc - Relevance: LOW - As Found: Unknown - ID: M9043 - Name: Glucagon - Relevance: LOW - As Found: Unknown - ID: M9579 - Name: Heparin - Relevance: HIGH - As Found: Obesity - ID: M46053 - Name: Calcium heparin - Relevance: LOW - As Found: Unknown - ID: M26997 - Name: Glucagon-Like Peptide 1 - Relevance: LOW - As Found: Unknown - ID: M223889 - Name: Soybean oil, phospholipid emulsion - Relevance: HIGH - As Found: 5000 - ID: M4244 - Name: Anticoagulants - Relevance: LOW - As Found: Unknown - ID: M8473 - Name: Fibrinolytic Agents - Relevance: LOW - As Found: Unknown - ID: M8360 - Name: Fat Emulsions, Intravenous - Relevance: LOW - As Found: Unknown - ID: M21860 - Name: Pharmaceutical Solutions - Relevance: LOW - As Found: Unknown - ID: M28934 - Name: Parenteral Nutrition Solutions - Relevance: LOW - As Found: Unknown - ID: T294 - Name: Soy Bean - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000006493 - Term: Heparin - ID: C000545823 - Term: Soybean oil, phospholipid emulsion ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06424002 Brief Title: The Impact RTS,S/AS01 Vaccine in School Aged Children RTS,S/AS01 Malaria Vaccine in School Aged Children Official Title: The Impact, Feasibility Acceptability and Cost Effectiveness of the RTS,S/AS01 Malaria Vaccine in School Aged Children #### Organization Study ID Info ID: P.09/22/3771 #### Organization Class: OTHER Full Name: Kamuzu University of Health Sciences ### Status Module #### Completion Date Date: 2024-12-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-12-20 Type: ESTIMATED #### Start Date Date: 2024-06-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2023-02-22 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER_GOV Name: Ministry of Health, Malawi Class: OTHER Name: Boston University Class: OTHER Name: Michigan State University #### Lead Sponsor Class: OTHER Name: Kamuzu University of Health Sciences #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: Across sub-Saharan Africa, school-age children bear an under-appreciated burden of malaria. An estimated 200 million school-age children are at risk of malaria and in many areas prevalence of infection exceeds 50%. The high infection rates in this group serves as a source of onward parasite transmission, undermining elimination and control efforts. Furthermore, malaria illness and malaria-induced anemia in this age group lead to school absenteeism, and impaired cognitive function and classroom attention, ultimately resulting in reduced academic achievement. Although universal malaria interventions, such as insecticide treated nets (ITNs) and access to prompt diagnosis and treatment are available to school-age children, this age group is the least likely to benefit from these interventions. Furthermore, efficacy of these approaches may be compromised by increasing anti-malarial drug and insecticide resistance. A malaria vaccine could help to avert the burden of malaria in this age group. The RTS,S/AS01 malaria vaccine has recently been recommended for vaccination of young children (\< 24 months) by the World health organization (WHO) after a Phase 3 trial and an implementation trial showed that the vaccine had moderate but significant efficacy to prevent clinical and severe malaria in young children. Previous randomized trials suggest that the vaccine is safe for older children. However, efficacy of the vaccine has never been assessed in school age children. Kamuzu University of Health Sciences in partnership with the Malawian Ministry of Health seeks to evaluate the efficacy of the newly introduced RTSS/AS01 malaria vaccine in school aged children. The study hypothesizes that vaccination will decrease the morbidity and transmission of malaria, as well as improve school absenteeism and educational outcomes. Detailed Description: This study will be an individual randomized open-label clinical trial to assess the impact, feasibility, acceptability and cost effectiveness of the RTS,S/AS01 vaccine in school-aged children in a malaria endemic environment. A total of 5400 children aged 6 to 15 years who are attending standards 1-8 in five schools in rural (Machinga) district of Malawi will be randomized to one of the four intervention arms: RTS,S/AS01 vaccine only (RTS,S-only), RTS,S/AS01 vaccine plus an effective antimalarial (artemether-lumefantrine) at the start of the study (RTS,S+AL), artemether-lumefantrine only (AL-only) and a control group that receives only Vitamin A at the start of the study (VIT-A). After obtaining consent from guardians and assent from children older than 13 years of age, participating children will be randomly allocated in a 1:1:1:1 ratio into the intervention arms. Randomization will be stratified by classroom and school. Additionally, two siblings of a subset of 1000 children receiving the vaccine will be enrolled to evaluate the indirect effect of vaccination. All children will be followed for up to 12 months after vaccination. Clinical malaria will be ascertained through passive case detection (PCD), and attendance and education outcomes will be ascertained through school records. PCD will conducted using the Learner Treatment Kit program platform, a school-based malaria diagnosis and treatment program that the Ministry of Health and Education are currently supporting across the selected schools. Through PCD, the safety of the interventions will also be monitored. In a subset of 1000 enrolled in the study (250 per intervention arm) and two of their siblings will also be followed in three pre-scheduled visits, the active case detection (ACD) cohort in which the investigators will evaluate outcomes including the direct effect of the vaccine on malaria subclinical infection and the indirect effect of the vaccine. Children will be selected for this cohort randomly, stratifying the samples by school and four age strata (6-7 years, 8-9 years, 10-12 years, 13-15 years). Participants will be invited to visit a health center at baseline, i.e., before the interventions are administered, one month, six months, and 12 months after the end of the primary regimen of RTS,S/AS01. At each of these visits, capillary blood (\~500 µl) will be collected through finger pricks for a dry blood spot, from which malaria quantitative polymerase chain reactions (qPCRs) will be performed to detect asexual parasites. In addition, one drop of blood will be used to measure hemoglobin concentrations. The remaining blood will be stored In 500 children enrolled in the ACD cohort and receiving vaccination, 6 mL of venous blood will be collected to evaluate immunological outcomes. These children will be randomly selected among those receiving RTS, S/AS01 (200 RTSS+AL and 200 RTSS-only) in four schools (50 X 2 intervention groups in each school), and the 4 age strata (\~ 12 per age strata in each school and intervention group). Feasibility, acceptability and cost data will be collected through interviews with all study stakeholders: learners, parents, teachers, community leaders, and district and national policy makers. ### Conditions Module Conditions: - Malaria,Falciparum ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 5400 Type: ESTIMATED Phases: - PHASE4 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Three doses of the vaccine will be administered, each with one month interval. RTS,S is a subunit vaccine that includes a portion of the circumsporozoite protein (CSP) co-expressed with Hepatitis B surface antigen. The adjuvant is AS01. Intervention Names: - Biological: Mosquirixs Label: RTS,S/AS01 Vaccine Type: EXPERIMENTAL #### Arm Group 2 Description: RTS,S/AS01 Vaccine will be provided with a therapeutic dose of artemether-lumefantrine (20 mg of artemether and 120 mg of lumefantrine). Artemether-lumefantrine will be given twice a day for 3 days based on the weight of the child as per treatment guidelines. Intervention Names: - Biological: Mosquirixs - Drug: artemether-lumefantrine Label: RTS,S/AS01 Vaccine plus artemether-lumefantrine Type: EXPERIMENTAL #### Arm Group 3 Description: A therapeutic dose of artemether-lumefantrine will be given twice a day for 3 days based on the weight of the child as per treatment guidelines. Intervention Names: - Drug: artemether-lumefantrine Label: Artemether-lumefantrine only Type: EXPERIMENTAL #### Arm Group 4 Description: This is the control group where Vitamin A will be given. Label: Vitamin A Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - RTS,S/AS01 Vaccine - RTS,S/AS01 Vaccine plus artemether-lumefantrine Description: RTS,S is a subunit vaccine that includes a portion of the circumsporozoite protein (CSP) co-expressed with Hepatitis B surface antigen. The adjuvant is AS01. Three doses of the vaccine will be administered, each with one month interval. Name: Mosquirixs Type: BIOLOGICAL #### Intervention 2 Arm Group Labels: - Artemether-lumefantrine only - RTS,S/AS01 Vaccine plus artemether-lumefantrine Description: A therapeutic dose of artemether-lumefantrine (20 mg of artemether and 120 mg of lumefantrine) will be given twice a day for 3 days based on the weight of the child as per treatment guidelines. Name: artemether-lumefantrine Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Based on symptoms of malaria plus a positive malaria rapid diagnostic test. A bood slide will also be collected for future assessment for malaria parasites Measure: Proportion of enrolled school children with clinical malaria incident events throughout the study period (PCD). Time Frame: During 18 months of follow up, when the child presents with symptoms of malaria within 48 hours at the leaner treatment kit (LTK) program which is run by teachers Description: This will be based on electronic classroom registers Measure: Proportion of enrolled school children that are daily absent from class throughout the study period (using electronic classroom registers) Time Frame: During 18 months of follow up, a daily register will be administered to record school attendance #### Secondary Outcomes Description: Pass rate based on classroom records Measure: Proportion of enrolled school children who pass their examinations at the end of the year and proceed to the next class (Pupil's passing fraction based on classroom records) Time Frame: During 18 months of follow up, classroom records will record children passing end of year examinations Description: Based on symptoms of malaria plus a positive malaria rapid diagnostic test. A bood slide will also be collected for future assessment for malaria parasites Measure: Proportion of enrolled school children with clinical malaria incident events throughout the study period (ACD) Time Frame: During 18 months of follow up, clinical malaria will be assessed during sick visits (PCD) and during active case detection Description: Based dried blood spot (DBS) samples from index child Measure: Proportion of enrolled school children with P. falciparum infections during the study period (ACD). Time Frame: During 18 months of follow up, malaria infection will be assessed during the ACD visits Description: As measured by hemocue machines Measure: Proportion of children with low levels of hemoglobin levels (hb<11g/dl) during the study period (ACD). Time Frame: At baseline, midline, endline and during ACD visits, hemoglobin levels will be measured during the 18 months follow up period Description: Based DBS samples from siblings of index child Measure: Proportion of siblings of enrolled children with P. falciparum infections at the beginning and end of the study period (indirect or "spill over" effect) (ACD) Time Frame: During 18 months of follow up, malaria infection will be assessed during the ACD visits Description: Magnitude of immunoglobulin G (IgG) against NANP. 2. Geometric mean of magnitude of antibodies against the two antigens, as well as avidity, and fractional catabolic rate (FcR) binding activity over time. Measure: Levels of antibodies against N-4-azido-2-nitrophenylpyridoxyl-5-phosphate (NANP) and CSP Time Frame: At endline and during ACD visits, levels of antibodies will be measured during 18 months of follow up ### Eligibility Module Eligibility Criteria: Inclusion criteria: * Pupils aged approximately 6 years to 15 years and enrolled in Standard 1 - 8 in the participating schools * Planning to remain in the study area for 1 year * Parental/guardian consent for child's participation and child assent if the child is 13 years of age or older Exclusion criteria: * Pregnancy, defined based on menstrual history. Pupils who had their last menstrual period more than 6 weeks before enrollment will be excluded. This threshold was chosen considering that menstrual cycles are irregular in this age group * Viral infections resulting in fever, chills, new loss of taste/smell and sore throat * Known allergy or history of adverse reaction to antimalarial treatment or vaccines * Chronic use of anti-malarial medication, azithromycin, or cotrimoxazole * Enrollment in any other study * Evidence of heart disease, HIV, or epilepsy * Severe disability Healthy Volunteers: True Maximum Age: 15 Years Minimum Age: 6 Years Sex: ALL Standard Ages: - CHILD ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Don P Mathanga, PhD Phone: +2651871911 Role: CONTACT #### Overall Officials Official 1: Affiliation: Kamuzu University of Health Sciences Name: Don P Mathanga, PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: Access will be based on requests and review of the request. As per NIH policy, data will be shared through approved links. Description: Under this proposal, Investigators will de-identify all the data intended for broader use, and all variables that could be used to deductively disclose the identity of individual subjects. Examples of data that will be removed include names, dates of birth, medical record numbers, telephone numbers, and locations of homes. All data will be sent to the approved Malawi government data repository center for safe keeping and will also be made available through NIH-supported portals for wide dissemination and access. Any data shared will be subject to Malawi government conditions of use governing access to the public release of data, including restrictions against attempting to identify study participants, destruction of data after analyses are completed, reporting responsibilities, restrictions on redistribution of data to third parties, and proper acknowledgement of data source. Info Types: - STUDY_PROTOCOL - SAP - ICF - CSR - ANALYTIC_CODE IPD Sharing: YES Time Frame: At the end of the study ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011528 - Term: Protozoan Infections - ID: D000010272 - Term: Parasitic Diseases - ID: D000007239 - Term: Infections - ID: D000096724 - Term: Mosquito-Borne Diseases - ID: D000079426 - Term: Vector Borne Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC01 - Name: Infections - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M11280 - Name: Malaria - Relevance: HIGH - As Found: Malaria - ID: M19133 - Name: Malaria, Falciparum - Relevance: HIGH - As Found: Malaria,Falciparum - ID: M10283 - Name: Infections - Relevance: LOW - As Found: Unknown - ID: M6368 - Name: Communicable Diseases - Relevance: LOW - As Found: Unknown - ID: M14388 - Name: Protozoan Infections - Relevance: LOW - As Found: Unknown - ID: M13185 - Name: Parasitic Diseases - Relevance: LOW - As Found: Unknown - ID: M3255 - Name: Mosquito-Borne Diseases - Relevance: LOW - As Found: Unknown - ID: M2054 - Name: Vector Borne Diseases - Relevance: LOW - As Found: Unknown - ID: T3571 - Name: Malaria - Relevance: HIGH - As Found: Malaria ### Condition Browse Module - Meshes - ID: D000008288 - Term: Malaria - ID: D000016778 - Term: Malaria, Falciparum ### Intervention Browse Module - Ancestors - ID: D000000962 - Term: Antimalarials - ID: D000000981 - Term: Antiprotozoal Agents - ID: D000000977 - Term: Antiparasitic Agents - ID: D000000890 - Term: Anti-Infective Agents ### Intervention Browse Module - Browse Branches - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Infe - Name: Anti-Infective Agents - Abbrev: Micro - Name: Micronutrients - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: Vi - Name: Vitamins ### Intervention Browse Module - Browse Leaves - ID: M17360 - Name: Vaccines - Relevance: LOW - As Found: Unknown - ID: M1936 - Name: Lumefantrine - Relevance: HIGH - As Found: Metabolic Syndrome - ID: M1827 - Name: Artemether - Relevance: HIGH - As Found: Moxifloxacin - ID: M1867 - Name: Artemether, Lumefantrine Drug Combination - Relevance: HIGH - As Found: Brochure - ID: M17558 - Name: Vitamins - Relevance: LOW - As Found: Unknown - ID: M17544 - Name: Vitamin A - Relevance: LOW - As Found: Unknown - ID: M302395 - Name: Retinol palmitate - Relevance: LOW - As Found: Unknown - ID: M4280 - Name: Antimalarials - Relevance: LOW - As Found: Unknown - ID: M4298 - Name: Antiprotozoal Agents - Relevance: LOW - As Found: Unknown - ID: M4294 - Name: Antiparasitic Agents - Relevance: LOW - As Found: Unknown - ID: M4214 - Name: Anti-Infective Agents - Relevance: LOW - As Found: Unknown - ID: T468 - Name: Vitamin A - Relevance: LOW - As Found: Unknown - ID: T462 - Name: Retinol - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000078102 - Term: Lumefantrine - ID: D000077549 - Term: Artemether - ID: D000077611 - Term: Artemether, Lumefantrine Drug Combination ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423989 Brief Title: Role of Immunoglobulin in Male Infertility Official Title: Role of Immunoglobulin in Male Infertility #### Organization Study ID Info ID: 102023 #### Organization Class: OTHER Full Name: Salma Kafeel Medical Centre ### Status Module #### Completion Date Date: 2024-12-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-06-01 Type: ESTIMATED #### Start Date Date: 2023-04-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-17 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Dr Salma kafeel Qureshi #### Responsible Party Investigator Affiliation: Salma Kafeel Medical Centre Investigator Full Name: Dr Salma kafeel Qureshi Investigator Title: Medical director head of Gynaecological and Reproductive unit Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: to investigate the role of IVIG in male infertility and to determine its benefits in term of semen parameters and assisted reproduction outcome ### Conditions Module Conditions: - Male Subfertility ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: OTHER #### Enrollment Info Count: 50 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Combination Product: IVIG Label: male fertility Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - male fertility Description: treatment of subfertility Name: IVIG Other Names: - pentaglobin Type: COMBINATION_PRODUCT ### Outcomes Module #### Primary Outcomes Description: Sperm concentration/ml Measure: Semen parameters percentage improvement Time Frame: 6 month Description: Percentage active motile sperm Measure: Sperm motility Time Frame: 6 month Description: Percentage of normal sperm Measure: Sperm morphology Time Frame: 6 month #### Secondary Outcomes Description: Percentage of fertilized Measure: Assisted Reproduction outcome measure Time Frame: 12 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * male patients Exclusion Criteria: * female Healthy Volunteers: True Sex: MALE Standard Ages: - CHILD - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: DR Riffat, PhD Phone: 00923225041390 Role: CONTACT Contact 2: Email: [email protected] Name: DR Riffat, PhD Phone: 00923225041390 Role: CONTACT #### Locations Location 1: City: Islamabad Contacts: *Contact 1:* - Name: dr riffat, PhD - Role: CONTACT Country: Pakistan Facility: SKMC State: Capital Status: RECRUITING Zip: 44000 ### IPD Sharing Statement Module Description: with in 6 month Info Types: - STUDY_PROTOCOL IPD Sharing: YES Time Frame: 6 month ## Derived Section ### Condition Browse Module - Ancestors - ID: D000091662 - Term: Genital Diseases - ID: D000091642 - Term: Urogenital Diseases - ID: D000005832 - Term: Genital Diseases, Male - ID: D000052801 - Term: Male Urogenital Diseases ### Condition Browse Module - Browse Branches - Abbrev: BXS - Name: Urinary Tract, Sexual Organs, and Pregnancy Conditions - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M10290 - Name: Infertility - Relevance: HIGH - As Found: Infertility - ID: M10292 - Name: Infertility, Male - Relevance: HIGH - As Found: Male Infertility - ID: M2876 - Name: Genital Diseases - Relevance: LOW - As Found: Unknown - ID: M2875 - Name: Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M8944 - Name: Genital Diseases, Male - Relevance: LOW - As Found: Unknown - ID: M27095 - Name: Male Urogenital Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000007246 - Term: Infertility - ID: D000007248 - Term: Infertility, Male ### Intervention Browse Module - Browse Branches - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M4225 - Name: Antibodies - Relevance: LOW - As Found: Unknown - ID: M10184 - Name: Immunoglobulins - Relevance: LOW - As Found: Unknown - ID: M19117 - Name: Immunoglobulins, Intravenous - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423976 Acronym: MMC Brief Title: Microbiome Molecular Charaterisation Official Title: Collection of Clinical Material From Patients With Prostate Cancer or Undergoing Investigation for Diagnostic or Follow up Purposes for Molecular Characterisation and Microbiome Analysis #### Organization Study ID Info ID: CCR5856 #### Organization Class: OTHER Full Name: Institute of Cancer Research, United Kingdom ### Status Module #### Completion Date Date: 2038-10 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-24 Type: ACTUAL Last Update Submit Date: 2024-05-23 Overall Status: RECRUITING #### Primary Completion Date Date: 2038-10 Type: ESTIMATED #### Start Date Date: 2023-10-23 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2023-10-25 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Institute of Cancer Research, United Kingdom #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Preclinical models of prostate cancer have proved to be poorly predictive of the behaviour of the disease in patients. This protocol describes the acquisition of prostate cancer tissue or cells from patients with treatment naïve/hormone-sensitive and castration-resistant prostate cancer or patients undergoing diagnostic or follow up investigations. The knowledge gained will improve the investigators' understanding of the steps leading to the development of castration resistance and identify new molecular targets for treatment. The human microbiome has been under investigation in a range of human diseases (i.e. metabolic disease/obesity, neurological disorders, cardiovascular disease, mental disorders, autoimmune disease, asthma and allergies) and cancer. The human microbiota can have direct (e.g. via direct genotoxicity, induction of chronic inflammation, etc.) and/or indirect (e.g. effects on tumour effects on tumour development or progression exerted through microbial communities that exist at a site distant to the tumour) effects on the disease. Emerging data supports the influence of the gut microbiota on the efficacy of anti-cancer treatments, including immunotherapy. To date, the impact of the gut microbiome on prostate cancer therapies is virtually unexplored. Based on the evidence to date, the investigators hypothesize that the gut flora may be altered by certain treatments for advanced prostate cancer, and that the composition of the microbiome in the gastrointestinal tract may be used to predict therapeutic efficacy or therapy-related toxicities; as well as prevent treatment toxicity and/or enhance treatment response. Furthermore, the purpose is to investigate the association between gut flora and treatment response and related toxicities/morbidities in advanced prostate cancer. Detailed Description: Prostate cancer is the second commonest malignancy in the UK and the second commonest cause of male mortality in the UK. Androgen deprivation therapy remains the mainstay of treatment, not only for advanced prostate cancer but also in the adjuvant and neo-adjuvant settings. Androgen deprivation therapy induces a remission in 80 to 90% of patients with advanced disease and results in a median progression-free survival of 12 to 33 months, at which time an androgen-independent phenotype usually emerges. This accounts for a median overall survival of 23 to 37 months from the initiation of androgen deprivation. Recent preclinical studies have shown that the intestinal microbiota is associated with response to treatments such as platinum chemotherapy (oxaliplatin) \[1\], cyclophosphamide \[2\] and both CTLA-4 blockade \[3\] and anti-PD-L1 \[4\] immunotherapies. Eradication of commensal intestinal flora by antibiotic treatment, or via deriving specific-pathogen-free (SPF) and/or germ-free animals, has been shown to alter the therapeutic efficacy of these agents in tumour models. Intriguingly, a recent study in a melanoma model showed that responses to anti-PD-L1 immunotherapy could be increased by feeding animals a strain of Bifidobacterium - a species commonly used in probiotic supplements - prior to initiating therapy. Collectively, these studies suggest that the composition of the intestinal microbiome is both essential for therapeutic efficacy and a target that could potentially be modulated to enhance treatment response. MMC is a prospective, observational, multi-centre study evaluating prostate cancer biology and associated microbiota. Patients must be willing to undergo a fresh tumour biopsy for molecular analyses. Following consent to MMC, fresh tumour tissue will be sent to designated research laboratories (see laboratory manual) for analyses to identify molecular aberrations and dysbiosis through targeted or broader molecular analyses (e.g. exome, transcriptome, whole genome), as well as (when indicated) orthogonal assays (e.g. immunohistochemistry, immunofluorescence, RNAish, digital droplet PCR). MMC will focus on tumour and microbiota characterisation (both CSPC and mCRPC) with recent studies indicating that this is a highly heterogeneous disease. The data acquired will be made available to patients, when indicated, and their clinical care team to help select what early clinical trial options merit consideration. Patients will not receive any treatment or IMP as part of this MMC protocol. Results of the molecular characterisation and microbiota studies will be made available to the treating investigator and the patient at a study specific visit (telephonic or face-to-face); patients will then be followed up every 6-months via medical notes review or telephone for survival and anti-cancer treatment data. ### Conditions Module Conditions: - Prostate Cancer ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 1000 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module ### Interventions #### Intervention 1 Description: Sequencing of tumour samples for microbiome analysis and molecular charcterisation. Name: Sequencing study Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Describing the microbiome composition in prostate cancer patients using metagenomic and metabolomic studies. Measure: Microbiome composition in prostate cancer patients Time Frame: through study completion, an average of 1 year #### Secondary Outcomes Description: Prevalence of prostate cancer aberrations including at DNA, RNA, protein or metabolite level. Measure: Prevalence of prostate cancer aberrations Time Frame: through study completion, an average of 1 year Description: Overall response rate defined as the proportion of patients with partial or complete response to a given treatment according to clinical \[Symptoms\], biochemical \[PSA\] or radiographic criteria (e.g., RECIST). * Prognostic clinical parameters - Hb \[Haemoglobin\], Albumin, LDH \& ALP * Time to castration resistance defined as time from study entry to diagnosis of castration resistant prostate cancer. * Time to treatment progression defined as time from start of therapy to progression (clinical \[Symptoms\], biochemical \[PSA\], or radiographic) on treatment. * Progression-free survival defined as the time from start of treatment to progression on treatment (clinical \[Symptoms\], biochemical \[PSA\] or radiographic) or death from any cause. * Overall survival defined as time from study entry to death from any cause. Measure: Patient clinical outcomes Time Frame: time to castration resistance, time to treatment progression and overall survival. ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Male \>=18 years. 2. Eastern Cooperative Oncology Group (ECOG) performance status (PS) 0 - 2. 3. Undergoing investigation for diagnosis, or with a proven diagnosis of prostate cancer and undergoing further investigation or clinical trial participation. 4. Patients with tumour deemed by the designated investigator as safely suitable for fresh biopsy AND who are medically fit (according to local practice) to undergo a biopsy or surgical procedure to acquire tumour tissue. 5. Willing and able to comply with the requirements of the sample collection including fresh tumour biopsy. 6. The subject is capable of understanding and complying with the protocol requirements and has given written informed consent. 7. A record of PSA levels within last 3 months. Exclusion Criteria: 1. The presence of any haematological disorders, including coagulation disorders, which would be a contraindication if patient were to undergo a biopsy. 2. Any psychiatric illness/social situations that would limit compliance with study requirements. 3. Presence of any concurrent condition or situation, which, in the investigator's opinion, may put the patient at significant risk, may confound the study results, or may interfere significantly with the patient's participation in the study. Minimum Age: 18 Years Sampling Method: PROBABILITY_SAMPLE Sex: MALE Standard Ages: - ADULT - OLDER_ADULT Study Population: The sample size is not based on formal statistical power analyses but rather on pragmatic and feasibility considerations. Our experience with our previous MC study lets us assume that we will be able to recruit 200 patients per year (from 1-2 participating centres) over a recruitment period of five years. Thus, the total expected sample size will be 1000 patients. The expected study endpoint analysis will commence following the 5-year recruitment period but no longer than the overall 15-year end of study timeline. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Omobola Fadahunsi Phone: 0203 437 3500 Role: CONTACT Contact 2: Email: [email protected] Name: Sasha Gayle Phone: 0208 722 4672 Role: CONTACT #### Locations Location 1: City: Sutton Contacts: *Contact 1:* - Email: [email protected] - Name: Johann De-Bono - Phone: 02086426011 - Role: CONTACT *Contact 2:* - Name: Prof. Johann De-Bono - Role: PRINCIPAL_INVESTIGATOR Country: United Kingdom Facility: Institute of Cancer Research/Royal Marsden NHS FT State: Surrey Status: RECRUITING Zip: SM2 5PT #### Overall Officials Official 1: Affiliation: The Royal Marsden NHS FT\The Institute of Cancer Research Name: Johann De-Bono Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000005834 - Term: Genital Neoplasms, Male - ID: D000014565 - Term: Urogenital Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000005832 - Term: Genital Diseases, Male - ID: D000091662 - Term: Genital Diseases - ID: D000091642 - Term: Urogenital Diseases - ID: D000011469 - Term: Prostatic Diseases - ID: D000052801 - Term: Male Urogenital Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BXS - Name: Urinary Tract, Sexual Organs, and Pregnancy Conditions - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M14335 - Name: Prostatic Neoplasms - Relevance: HIGH - As Found: Prostate Cancer - ID: M8946 - Name: Genital Neoplasms, Male - Relevance: LOW - As Found: Unknown - ID: M17315 - Name: Urogenital Neoplasms - Relevance: LOW - As Found: Unknown - ID: M2876 - Name: Genital Diseases - Relevance: LOW - As Found: Unknown - ID: M8944 - Name: Genital Diseases, Male - Relevance: LOW - As Found: Unknown - ID: M2875 - Name: Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M14333 - Name: Prostatic Diseases - Relevance: LOW - As Found: Unknown - ID: M27095 - Name: Male Urogenital Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000011471 - Term: Prostatic Neoplasms ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423963 Brief Title: Remote Exercise and Nutritional Prehabilitation for Pancreatic Cancer Official Title: Remote Exercise and Nutritional Prehabilitation for Pancreatic Cancer #### Organization Study ID Info ID: MCC-23088 #### Organization Class: OTHER Full Name: H. Lee Moffitt Cancer Center and Research Institute ### Status Module #### Completion Date Date: 2026-02 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-02 Type: ESTIMATED #### Start Date Date: 2024-02-08 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-22 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: H. Lee Moffitt Cancer Center and Research Institute #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The purpose of the study is to examine the feasibility and acceptability of an exercise and nutrition "prehabilitation" program for patients preparing for pancreatic cancer resection (removal). ### Conditions Module Conditions: - Pancreatic Cancer ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: SUPPORTIVE_CARE #### Enrollment Info Count: 26 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Behavioral: Physical Activity - Behavioral: Nutrition Counseling Label: Physical activity, nutrition counseling and monitoring group (PA/N) Type: EXPERIMENTAL #### Arm Group 2 Intervention Names: - Behavioral: Physical Activity - Behavioral: Nutrition Counseling - Behavioral: Resistance Training Label: Physical activity, tele-resistance training, nutrition counseling and monitoring group (RT/N) Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Physical activity, nutrition counseling and monitoring group (PA/N) - Physical activity, tele-resistance training, nutrition counseling and monitoring group (RT/N) Description: Each participant will receive a Fitbit device with instruction and encouragement to self-monitor physical activity using step counts. Name: Physical Activity Type: BEHAVIORAL #### Intervention 2 Arm Group Labels: - Physical activity, nutrition counseling and monitoring group (PA/N) - Physical activity, tele-resistance training, nutrition counseling and monitoring group (RT/N) Description: Participants will receive nutritional counseling with a registered dietician. Name: Nutrition Counseling Type: BEHAVIORAL #### Intervention 3 Arm Group Labels: - Physical activity, tele-resistance training, nutrition counseling and monitoring group (RT/N) Description: Participants will engage in progressive, full-body resistance training based on American College of Sports Medicine (ACSM) guidelines. Name: Resistance Training Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: The number of participants who complete T1 and T0 measures. Measure: Feasibility and acceptability of PA/N and RT/N programs Time Frame: Up to 16 weeks #### Secondary Outcomes Description: The number of participants who demonstrate improvements in exploratory outcome measures. Measure: Examine exploratory outcomes and clinical characteristics Time Frame: Up to 16 weeks Description: Chi-Square testing will be used to determine if there's a significant difference in outcomes between the treatment group and a usual care comparison group. Measure: Compare clinical and treatment outcomes Time Frame: Up to 16 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age 18 years or older * Biopsy-proven pancreatic ductal adenocarcinoma (PDAC), borderline resectable at diagnosis * Eastern Cooperative Oncology Group (ECOG) performance status 0-2 * Undergoing neoadjuvant chemotherapy with treatment plan including chemoradiation therapy and surgical resection * Ability to read and speak English Exclusion Criteria: * Regular engagement in RT (2x/week targeting all major muscle groups) * Screen failure for exercise safety based on PAR-Q * Underlying unstable cardiac or pulmonary disease or symptomatic cardiac disease * Recent fracture or acute musculoskeletal injury that precludes ability to participate in RT * Numeric pain rating scale greater than or equal to a 7 out of 10 * Myopathic or rheumatologic disease that impacts physical function Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Morgan Bean Phone: 813-745-1786 Role: CONTACT #### Locations Location 1: City: Tampa Contacts: *Contact 1:* - Email: [email protected] - Name: Morgan Bean - Phone: 813-745-1786 - Role: CONTACT *Contact 2:* - Name: Nathan Parker, PhD - Role: PRINCIPAL_INVESTIGATOR *Contact 3:* - Name: Pamela Hodul, MD - Role: PRINCIPAL_INVESTIGATOR *Contact 4:* - Name: Sylvia Crowder, PhD - Role: SUB_INVESTIGATOR Country: United States Facility: Moffitt Cancer Center State: Florida Status: RECRUITING Zip: 33612 #### Overall Officials Official 1: Affiliation: Moffitt Cancer Center Name: Nathan Parker, PhD Role: PRINCIPAL_INVESTIGATOR Official 2: Affiliation: Moffitt Cancer Center Name: Pamela Hodul, MD Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000004701 - Term: Endocrine Gland Neoplasms - ID: D000004066 - Term: Digestive System Diseases - ID: D000010182 - Term: Pancreatic Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M13110 - Name: Pancreatic Neoplasms - Relevance: HIGH - As Found: Pancreatic Cancer - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7863 - Name: Endocrine Gland Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M13102 - Name: Pancreatic Diseases - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown - ID: T4387 - Name: Pancreatic Cancer - Relevance: HIGH - As Found: Pancreatic Cancer ### Condition Browse Module - Meshes - ID: D000010190 - Term: Pancreatic Neoplasms ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423950 Brief Title: Generating Novel Translational and Therapeutic Strategies Based on a Multicenter, Pediatric and AYA Evolutionary Tumor Board (pedsETB) Official Title: Feasibility of Generating Novel Translational and Therapeutic Strategies Based on a Multicenter, Pediatric and AYA Evolutionary Tumor Board (pedsETB) #### Organization Study ID Info ID: MCC-22170 #### Organization Class: OTHER Full Name: H. Lee Moffitt Cancer Center and Research Institute ### Status Module #### Completion Date Date: 2027-04 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2027-04 Type: ESTIMATED #### Start Date Date: 2024-04-30 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-09 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: National Pediatric Cancer Foundation #### Lead Sponsor Class: OTHER Name: H. Lee Moffitt Cancer Center and Research Institute #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: To evaluate the ability of a multidisciplinary and multisite group, the Pediatric Evolutionary Tumor Board (pedsETB), to develop additional therapeutic strategies in patients without curative options or with suboptimal outcomes. ### Conditions Module Conditions: - Pediatric Cancer ### Design Module #### Bio Spec Description: Peripheral blood collected at study enrollment and subsequently at designated time points: Screening/Baseline/Enrollment, first post pedsETB Visit, and every 12 weeks (+/- 6 weeks) or upon changes in disease status, therapeutic intervention, and/or events of special interest at the discretion of the treating physician. Retention: SAMPLES_WITH_DNA #### Design Info Observational Model: CASE_ONLY Time Perspective: PROSPECTIVE #### Enrollment Info Count: 35 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants clinical history, available therapeutic options, and outcome expectations will be presented to the Evolutionary Tumor Board (ETB) along with images and pathology. Strategies and models will be presented regarding additional evolutionary ideas that can be applied. These ideas will be characterized (e.g. first strike-second strike, adaptive, novel sequential therapy, novel combination, novel dosing schedule, etc.). Intervention Names: - Other: Peds Evolutionary Tumor Board (pedsETB) Label: Participants Reviewed by ETB ### Interventions #### Intervention 1 Arm Group Labels: - Participants Reviewed by ETB Description: The pedsETB consists of evolutionary biologists, mathematicians, research scientists, statisticians, data scientists, radiologists, pathologists, oncologists (surgical, radiation, medical, and pediatric), and clinical trial coordinators. The pedsETB membership is inclusive of members from the participating institutions. The pedsETB will generate hypotheses, mathematical models, and experiments from the discussion towards further integration of evolutionary ideas towards therapeutic strategies for participants. The pedsETB will collect data through a chart review regarding adherence and results of ETB recommendation. Name: Peds Evolutionary Tumor Board (pedsETB) Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The investigators will measure the ability of a multidisciplinary group, the pedsETB, to develop additional therapeutic strategies in patients without curative options. The investigators plan to enroll 35 patients on the study. The primary objective will be successfully met if the pedsETB can develop an evolutionary based therapeutic strategy that differs from the oncologist's opinion prior to presentation for at least 80%, or 28 of these patients. Measure: The feasibility of the pedsETB developing therapeutic strategies Time Frame: Baseline to up to 60 months from end of therapy ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Participant must be considered likely incurable given the standard of care. This is inclusive of patients newly diagnosed, relapsed or in remission but at high risk of recurrence, with suboptimal responses to previous therapy, or with many potentially beneficial, but unlikely curative options for care. The site investigator will make this determination based on their experience. * Participant must have an age-appropriate performance status: Karnofsky 50 or more for patients 16 years of age or older OR Lansky score of 50 or more for patients less than16 years of age. * Participant and/or parents or legal guardian and primary oncologist must be willing to consider the therapeutic strategies recommended by the pedsETB. * Participant must be willing to be followed over time and allow collection of clinical data including scans, available blood and lab samples, and optional pedsETB serial blood sampling. * All Participants and/or their parents or legal guardians must have the ability to understand and the willingness to sign a written informed consent or assent document. Exclusion Criteria: * Participants without known therapies to reliably induce a response are excluded from pedsETB and should seek clinical trials. Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT Study Population: Participants who are patients at participating pedsETB sites. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Jessica Crimella Phone: 813-745-6250 Role: CONTACT Contact 2: Name: Jonathan Metts, MD Role: CONTACT #### Locations Location 1: City: Tampa Contacts: *Contact 1:* - Email: [email protected] - Name: Jessica Crimella - Phone: 813-745-6250 - Role: CONTACT *Contact 2:* - Name: Jonathan Metts, MD - Role: PRINCIPAL_INVESTIGATOR *Contact 3:* - Name: Mark Robertson-Tessi, PhD - Role: PRINCIPAL_INVESTIGATOR *Contact 4:* - Name: Joel S Brown, PhD - Role: SUB_INVESTIGATOR *Contact 5:* - Name: Rikesh Makanji, MD - Role: SUB_INVESTIGATOR *Contact 6:* - Name: Andriy Marusyk, PhD - Role: SUB_INVESTIGATOR *Contact 7:* - Name: Alexander Anderson, PhD - Role: SUB_INVESTIGATOR Country: United States Facility: Moffitt Cancer Center State: Florida Status: RECRUITING Zip: 33612 #### Overall Officials Official 1: Affiliation: Moffitt Cancer Center Name: Jonathan Metts, MD Role: PRINCIPAL_INVESTIGATOR ### References Module #### See Also Links Label: Moffitt Cancer Center Clinical Trials Website URL: http://moffitt.org/clinical-trials-research/clinical-trials/ ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423937 Brief Title: Fruquintinib Plus Camrelizumab and HAIC in the Treatment of Non-MSI-H Advanced Colorectal Cancer Official Title: A Single-center, Open-label, Double-cohort Clinical Study of Fruquintinib Plus Camrelizumab Plus HAIC in the Treatment of Non-MSI-H Advanced Colorectal Cancer Patients With Liver Metastasis After the Failure of First-line Treatment #### Organization Study ID Info ID: HMPL-013-SH-CRC-106 #### Organization Class: OTHER Full Name: Fudan University ### Status Module #### Completion Date Date: 2027-07 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-07 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-11 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Fudan University #### Responsible Party Investigator Affiliation: Fudan University Investigator Full Name: Lu Wang, MD, PhD Investigator Title: Head of liver surgery department Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: Liver metastasis is the main cause of death in patients with colorectal cancer. The treatment of liver metastasis of colorectal cancer is the key to prolong the survival of patients. The purpose of this study was to investigate the efficacy and safety of fruquintinib combined with Camrelizumab and HAIC regimen in the treatment of non-MSI-H advanced colorectal cancer patients with liver metastasis after first-line standard treatment failure. Compared with the current standard second-line treatment plan, it provides new decisions for clinical practice, in order to reduce the adverse reactions of treatment and improve the tolerance and efficacy of patients. To provide more and more optimized medication options for patients with non-MSI-H advanced colorectal cancer complicated with liver metastasis. Detailed Description: This is a single-center, open, double-cohort clinical study to explore the non-MSI-H type advanced colorectal cancer patients with liver metastases after the failure of first-line standard treatment with fruquintinib combined with calelizumab and HAIC.Clinically, systemic chemotherapy with 5-FU as the core, combined with irinotecan or oxaliplatin is the first-line and second-line standard chemotherapy regimen for unresectable CRLM patients, but various hepatotoxicity will occur during chemotherapy. HAIC can selectively deliver chemotherapeutic drugs to tumor cells, reduce hepatocyte toxicity, relatively preserve liver parenchyma, and increase the concentration of chemotherapy in the tumor. Tumor cells are exposed to chemotherapy for a longer time, which effectively improves the efficacy and safety of treatment. Anti-angiogenic drugs can hinder the growth of microvessels in tumors and the development of metastatic diseases. At present, multiple retrospective studies have provided evidence support. The response rate of HAIC combined with systemic targeted therapy can reach 74 % -92 %. Previous studies have suggested that anti-angiogenic drugs combined with immunotherapy is expected to be a treatment strategy for patients with advanced colorectal cancer who fail to receive standard treatment or cannot receive standard treatment. Therefore, this study investigated the efficacy and safety of fruquintinib combined with Camrelizumab and HAIC in the treatment of patients with non-MSI-H advanced colorectal cancer complicated with liver metastasis after first-line standard treatment failure. ### Conditions Module Conditions: - Colorectal Cancer ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 129 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Advanced non-MSI-H left-sided colorectal cancer with liver metastasis after first-line standard treatment failure Intervention Names: - Drug: combination therapy Combination: Fruquintinib plus Camrelizumab and HAIC (TOMOX/TOMIRI) Maintenance: Fruquintinib plus Camrelizumab Label: Advanced non-MSI-H left-sided colorectal cancer Type: EXPERIMENTAL #### Arm Group 2 Description: Advanced non-MSI-H right-sided colorectal cancer with liver metastasis after first-line standard treatment failure Intervention Names: - Drug: combination therapy Combination: Fruquintinib plus Camrelizumab and HAIC (TOMOX/TOMIRI) Maintenance: Fruquintinib plus Camrelizumab Label: Advanced non-MSI-H right-sided colorectal cancer Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Advanced non-MSI-H left-sided colorectal cancer - Advanced non-MSI-H right-sided colorectal cancer Description: Procedure/Surgery: HAIC After successful percutaneous hepatic artery cannulation, superior mesenteric arteriogram and hepatic arteriogram were performed, and after confirming that the subjects were eligible for enrollment according to the results, the hepatic artery was cannulated to the predetermined position. The catheter was connected to a syringe pump in the ward for continuous pumping of drugs. TOMOX（Raltitrexed 2 mg/m2, Oxaliplatin 85mg/m2）/ TOMIRI（Raltitrexed 2 mg/m2 ，Irinotecan 120mg/m2） Drug: Fruquintinib 3mg, qd, po, 21 days for a cycle, Suspend medication on the day of HAIC Drug: Camrelizumab 200mg, ivgtt,, 21 days for a cycle Name: combination therapy Combination: Fruquintinib plus Camrelizumab and HAIC (TOMOX/TOMIRI) Maintenance: Fruquintinib plus Camrelizumab Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Defined as percentage of participants achieving assessed complete response (CR) and partial response (PR) by the investigator according to the RECIST 1.1. Measure: objective response rate (ORR) Time Frame: 24 months #### Secondary Outcomes Description: DCR was defined as the percentage of participants who have a confirmed complete response#CR# or partial response#PR# or stable disease#SD# per RECIST 1.1 as assessed by investigator Measure: disease control rate (DCR) Time Frame: 24 months Description: PFS is defined as the time from enrollment to the first documented disease progression or death due to any cause, whichever occurs first. Responses are according to the Response Evaluation Criteria in Solid Tumors version 1.1 (RECIST 1.1) as assessed by investigator Measure: Progression-Free Survival (PFS) Time Frame: 24 months Description: The proportion of patients who did not experience disease progression or death from treatment initiation to 6 months Measure: Progression-Free Survival rate at 6 months Time Frame: 6 months Description: OS is the time from enrollment to death due to any cause. Measure: overall survival (OS) Time Frame: 24 months Description: overall incidence of adverse events (AE); incidence of grade 3 or higher AE; incidence of severe adverse events (SAE); incidence of AEs leading to discontinuation of drug use; incidence of AEs leading to suspension of drug use Measure: Adverse events as assessed by NCI CTCAE v5.0 Time Frame: 24 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * The subjects volunteered to join the study and signed informed consent, with good compliance and follow-up. * Patients with histologically or cytologically confirmed non-MSI-H ( according to the detection criteria of the institutional testing center, immunohistochemistry, PCR or NGS detection can be used ) unresectable advanced colorectal cancer with liver metastasis ; * Age ≥ 18 years, ≤75 years， male or female ; * ECOG PS 0-1; * Expected overall survival ≥3 months * Patients must have at least one measurable liver metastases (RECIST 1.1) * Patients who had only received one standard first-line systemic treatment and were confirmed to be ineffective, or could not tolerate first-line treatment ; * Patients must have adequate organ and bone marrow function( No blood components and cell growth factors were used within 14 days before enrollment ) * Male or female patients with fertility voluntarily used effective contraceptive methods, such as double-barrier contraceptive methods, condoms, oral or injectable contraceptives, intrauterine devices, etc., during the study period and within 6 months of treatment in the last study. All female patients will be considered to have fertility, unless the female patient has natural menopause, artificial menopause or sterilization ( such as hysterectomy, bilateral adnexectomy or radioactive ovarian irradiation, etc. ), otherwise the female patient 's serum or urine test showed no pregnancy within 7 days before the study, and must be non-lactating patients. Exclusion Criteria: * Patients who are allergic or suspected to be allergic to the study drug or similar drugs * Patients had other malignant tumors in the past 5 years or at the same time (except for the cured skin basal cell carcinoma and cervical carcinoma in situ); * Participating in other clinical trials and received at least one treatment within 4 weeks before enrollment * Patients with autoimmune disease or history of autoimmune disease within 4 weeks before enrollment * patients currently have central nervous system (CNS) metastasis or previous brain metastasis and the symptom control time is less than 2 months * Patients cannot take fruquintinib orally * Patients who have received organ transplantation and bone marrow transplantation in the past * Have taken other strong inducers or inhibitors of CYP3A4, P-gp substrates and BCRP substrates within 2 weeks before the First medication * Received any operation (except biopsy) or invasive treatment or operation (except venous catheterization, puncture and drainage, etc.) within 4 weeks before enrollment * Pleural effusion or ascites causing relevant clinical symptoms, including respiratory syndrome (dyspnea≥CTC AE grade 2) * Clinically significant electrolyte abnormality# * Systolic blood pressure \> 140mmHg or diastolic blood pressure \> 90mmHg regardless of any antihypertensive drugs; Or patients need more than two antihypertensive drugs * Proteinuria ≥ 2+ (1.0g/24hr); * Active gastric and duodenal ulcer, ulcerative colitis or uncontrolled hemorrhage in GI, or other conditions that may cause GI bleeding and perforation as determined by the investigator; * Have evidence or history of bleeding tendency within 3 months or thromboembolic events within 12 months before enrollment( Hemorrhage \> 30 mL within 3 months, hematemesis, black feces, hematochezia ), hemoptysis ( fresh blood \> 5 mL within 4 weeks ) or thromboembolic events ( including stroke events and / or transient ischemic attack ) within 12 months ; * Clinically significant cardiovascular disease, including but not limited to acute myocardial infarction, severe/unstable angina pectoris or coronary artery bypass grafting within 6 months before enrollment; NYHA classification \> 2 Grade; ventricular arrhythmia requiring medical therapy; ECG showing QTc interval ≥ 480 ms * Active or uncontrolled serious infection (≥CTCAE grade 2 infection) * Pregnant or lactating women * Any other disease, with clinically significant metabolic abnormalities, physical examination abnormalities or laboratory abnormalities, according to the judgment of investigator that the patient is not suitable for the the study drug (such as having epileptic seizures and require treatment), or would affect the interpretation of study results, or put patients at high risk * Clinical uncontrolled active infections, including human immunodeficiency virus (HIV) infection, active hepatitis B / C (HBV DNA Positive\[1×104 copies/mL or \>2000 IU/ml\], HCV RNA positive\[\>1×103 copies/mL\]); * Patients have other factors that may affect the results of the study or cause the study to be terminated halfway, such as alcoholism, drug abuse, other serious diseases (including mental diseases) that require concomitant treatment, and serious laboratory abnormalities. Accompanied by family or social factors, which will affect the safety of patients. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Tan Li Phone: 158 0068 0751 Role: CONTACT #### Locations Location 1: City: Shanghai Country: China Facility: Fudan University Shanghai Cancer Center Zip: 200062 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000007414 - Term: Intestinal Neoplasms - ID: D000005770 - Term: Gastrointestinal Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000004066 - Term: Digestive System Diseases - ID: D000005767 - Term: Gastrointestinal Diseases - ID: D000003108 - Term: Colonic Diseases - ID: D000007410 - Term: Intestinal Diseases - ID: D000012002 - Term: Rectal Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC06 - Name: Digestive System Diseases ### Condition Browse Module - Browse Leaves - ID: M12307 - Name: Neoplasm Metastasis - Relevance: LOW - As Found: Unknown - ID: M17890 - Name: Colorectal Neoplasms - Relevance: HIGH - As Found: Colorectal Cancer - ID: M10448 - Name: Intestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M6336 - Name: Colonic Diseases - Relevance: LOW - As Found: Unknown - ID: M10444 - Name: Intestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M14844 - Name: Rectal Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000015179 - Term: Colorectal Neoplasms ### Intervention Browse Module - Browse Branches - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Hemat - Name: Hematinics ### Intervention Browse Module - Browse Leaves - ID: M1671 - Name: Irinotecan - Relevance: LOW - As Found: Unknown - ID: M252094 - Name: Raltitrexed - Relevance: LOW - As Found: Unknown - ID: M1674 - Name: Oxaliplatin - Relevance: LOW - As Found: Unknown - ID: M11110 - Name: Liver Extracts - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423924 Brief Title: Second Primary Cancer and Early-onset Colorectal Cancer Official Title: Risk Factors, Cancer Types and Prognostic Significance of Second Primary Cancer Based on the Early-onset and Late-onset Colorectal Cancer #### Organization Study ID Info ID: CRCSPM #### Organization Class: OTHER Full Name: Fudan University ### Status Module #### Completion Date Date: 2024-06-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-05-20 Type: ESTIMATED #### Start Date Date: 2024-05-11 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-11 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: LI XIN-XIANG #### Responsible Party Investigator Affiliation: Fudan University Investigator Full Name: LI XIN-XIANG Investigator Title: professor Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The objective of this study was to analyze the pathological factors influencing the occurrence and prognosis of SPC in CRC patients of varying ages and compare the differences in the patterns of SPC occurrence and prognosis among patients of different age groups. ### Conditions Module Conditions: - Colorectal Cancer - Second Primary Cancer ### Design Module #### Design Info Observational Model: COHORT Time Perspective: RETROSPECTIVE #### Enrollment Info Count: 10000 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Other: no intervention Label: <50 years #### Arm Group 2 Intervention Names: - Other: no intervention Label: 50-69 years #### Arm Group 3 Intervention Names: - Other: no intervention Label: ≥70 years ### Interventions #### Intervention 1 Arm Group Labels: - 50-69 years - <50 years - ≥70 years Description: no intervention Name: no intervention Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The duration from the date of surgery to death for any reason or the last recorded follow-up, whichever comes first. Up to 100 months Measure: overall survival Time Frame: The duration from the date of surgery to death for any reason or the last recorded follow-up, whichever comes first. Up to 100 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Patients undergoing radical surgery for colorectal cancer at Fudan University Shanghai Cancer Center between January 2008 and December 2018. * Stage Ⅰ-Ⅳ colorectal cancer confirmed by clear pathological information Exclusion Criteria: * Previous history of other cancers before surgery * Patients under 18 years old or over 80 years old Maximum Age: 80 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Patients retrieved from the database of Fudan University Shanghai Cancer Center. These patients were diagnosed with CRC primary tumors between January 2008 and December 2018. ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000007414 - Term: Intestinal Neoplasms - ID: D000005770 - Term: Gastrointestinal Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000004066 - Term: Digestive System Diseases - ID: D000005767 - Term: Gastrointestinal Diseases - ID: D000003108 - Term: Colonic Diseases - ID: D000007410 - Term: Intestinal Diseases - ID: D000012002 - Term: Rectal Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M17890 - Name: Colorectal Neoplasms - Relevance: HIGH - As Found: Colorectal Cancer - ID: M18989 - Name: Neoplasms, Second Primary - Relevance: HIGH - As Found: Second Primary Cancer - ID: M10448 - Name: Intestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M6336 - Name: Colonic Diseases - Relevance: LOW - As Found: Unknown - ID: M10444 - Name: Intestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M14844 - Name: Rectal Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000015179 - Term: Colorectal Neoplasms - ID: D000009369 - Term: Neoplasms - ID: D000016609 - Term: Neoplasms, Second Primary ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423911 Acronym: POLARIS-2 Brief Title: A Phase 3 Registrational Study of Olverembatinib (HQP1351) in Patients With CML Official Title: This is a Global, Multi-center, Open-label Randomized and Registrational Phase 3 Study of Olverembatinib (HQP1351) in Patients With Chronic Myeloid Leukemia #### Organization Study ID Info ID: HQP1351CG301 #### Organization Class: INDUSTRY Full Name: Ascentage Pharma Group Inc. ### Status Module #### Completion Date Date: 2026-02 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-12 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Ascentage Pharma Group Inc. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Oversight Has DMC: True ### Description Module Brief Summary: A Global Multicenter, Open Label, Randomized, Phase 3 Registrational Study of Olverembatinib (HQP1351) in Patients with Chronic Phase Chronic Myeloid Leukemia (POLARIS-2) Detailed Description: This is a global, multi-center, open-label randomized and registrational phase 3 study of olverembatinib: Part A is a randomized controlled part that is designed to compare the efficacy and safety of olverembatinib (investigational arm) versus bosutinib (control arm) in patients with CML-CP, previously treated with at least two tyrosine kinase inhibitors (TKIs). Part B is to evaluate the efficacy and safety of olverembatinib in the CML- CP patients with T315I mutation. ### Conditions Module Conditions: - Chronic Myeloid Leukemia - CML - CML, Chronic Phase ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Part A 2:1 ratio Part B: control ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 285 Type: ESTIMATED Phases: - PHASE3 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Randomized controlled part that is designed to compare the efficacy and safety of olverembatinib (investigational arm) versus bosutinib (control arm) in patients with CML-CP, previously treated with at least two TKIs Intervention Names: - Drug: olverembatinib - Drug: Bosutinib Label: Arm A: Type: OTHER #### Arm Group 2 Description: To evaluate the efficacy and safety of olverembatinib in the CML-CP patients with T315I mutation previously Intervention Names: - Drug: olverembatinib Label: Arm B: Type: OTHER ### Interventions #### Intervention 1 Arm Group Labels: - Arm A: - Arm B: Description: olverembatinib QOD Name: olverembatinib Type: DRUG #### Intervention 2 Arm Group Labels: - Arm A: Description: Bosutnib QD Name: Bosutinib Type: DRUG ### Outcomes Module #### Primary Outcomes Description: To compare the major molecular response (MMR) rate at 24 weeks of olverembatinib versus bosutinib Measure: MMR rate Part A Time Frame: 24 weeks Description: To evaluate the MMR rate by 24 weeks of olverembatinib in CML-CP patients with T315I mutation Measure: MMR rate Part B Time Frame: 24 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: Patients eligible for inclusion in this study must meet all of the following criteria. 1. Age ≥ 18 years old. 2. Diagnosis of CML-CP 3. Part A: Previously treated with at least two approved TKIs Part B: T315I mutation at screening. 4. Eastern Cooperative Oncology Group (ECOG) performance status (PS) ≤ 2. 5. Written informed consent obtained prior to any screening procedures. 6. Patients with adequate organ functions Exclusion Criteria: Patients eligible for this study must not meet any of the following criteria. 1. For Part A only: T315I mutation at any time prior to starting study treatment. 2. Active infection that requires systemic drug therapy 3. Impairment of gastrointestinal (GI) function or GI disease that may significantly alter absorption of study drugs 4. Previous treatment with or known / suspected hypersensitivity to olverembatinib or any of its excipients. 5. Previous treatment with or known / suspected hypersensitivity to bosutinib or any of its excipients. 6. Pregnant or nursing (lactating) women. Maximum Age: 99 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Ben Little Phone: 301-509-3222 Role: CONTACT Contact 2: Email: [email protected] Name: Huanshan Guo Role: CONTACT #### Locations Location 1: City: Houston Country: United States Facility: MD Anderson Cancer Center State: Texas Zip: 77030 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000006402 - Term: Hematologic Diseases - ID: D000009196 - Term: Myeloproliferative Disorders - ID: D000001855 - Term: Bone Marrow Diseases - ID: D000002908 - Term: Chronic Disease - ID: D000020969 - Term: Disease Attributes - ID: D000010335 - Term: Pathologic Processes ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC15 - Name: Blood and Lymph Conditions - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M10945 - Name: Leukemia - Relevance: HIGH - As Found: Leukemia - ID: M10955 - Name: Leukemia, Myeloid - Relevance: HIGH - As Found: Myeloid Leukemia - ID: M18123 - Name: Leukemia, Myelogenous, Chronic, BCR-ABL Positive - Relevance: HIGH - As Found: Chronic Myeloid Leukemia - ID: M18125 - Name: Leukemia, Myeloid, Chronic-Phase - Relevance: HIGH - As Found: CML, Chronic Phase - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M9490 - Name: Hematologic Diseases - Relevance: LOW - As Found: Unknown - ID: M12149 - Name: Myeloproliferative Disorders - Relevance: LOW - As Found: Unknown - ID: M5134 - Name: Bone Marrow Diseases - Relevance: LOW - As Found: Unknown - ID: M6147 - Name: Chronic Disease - Relevance: LOW - As Found: Unknown - ID: M22700 - Name: Disease Attributes - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: HIGH - As Found: Chronic - ID: T3995 - Name: Myeloid Leukemia - Relevance: HIGH - As Found: Myeloid Leukemia - ID: T1309 - Name: Chronic Myeloid Leukemia - Relevance: HIGH - As Found: Chronic Myeloid Leukemia - ID: T1311 - Name: Chronic Myeloproliferative Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000007938 - Term: Leukemia - ID: D000007951 - Term: Leukemia, Myeloid - ID: D000015464 - Term: Leukemia, Myelogenous, Chronic, BCR-ABL Positive - ID: D000015466 - Term: Leukemia, Myeloid, Chronic-Phase ### Intervention Browse Module - Ancestors - ID: D000092004 - Term: Tyrosine Kinase Inhibitors - ID: D000047428 - Term: Protein Kinase Inhibitors - ID: D000004791 - Term: Enzyme Inhibitors - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action ### Intervention Browse Module - Browse Branches - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: AA - Name: Amino Acids ### Intervention Browse Module - Browse Leaves - ID: M42200 - Name: Bosutinib - Relevance: HIGH - As Found: Hydromorphone - ID: M2889 - Name: Tyrosine Kinase Inhibitors - Relevance: LOW - As Found: Unknown - ID: M25820 - Name: Protein Kinase Inhibitors - Relevance: LOW - As Found: Unknown - ID: M7951 - Name: Enzyme Inhibitors - Relevance: LOW - As Found: Unknown - ID: T22 - Name: Tyrosine - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: C000471992 - Term: Bosutinib ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423898 Acronym: DOBLEI Brief Title: Ampicillin and Ceftriaxone for the Treatment of Enterococcus Faecalis Infective Endocarditis. Official Title: Efficacy and Safety of Ampicillin and Ceftriaxone Continuous Infusion Versus Intermittent Infusion for the Treatment of Enterococcus Faecalis Infective Endocarditis (DOBLEI) #### Organization Study ID Info ID: DOBLEI #### Organization Class: OTHER Full Name: Fundación Pública Andaluza para la gestión de la Investigación en Sevilla ### Status Module #### Completion Date Date: 2028-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2027-07-31 Type: ESTIMATED #### Start Date Date: 2024-09-30 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-13 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: NETWORK Name: Spanish Clinical Research Network - SCReN #### Lead Sponsor Class: OTHER Name: Fundación Pública Andaluza para la gestión de la Investigación en Sevilla #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Phase IV, open-label, randomized and multicenter clinical trial to prove that patients with Enterococcus faecalis infective endocarditis treated with an antibiotic treatment as a continuous infusion is non-inferior to the standard intermittent infusion regimen, usually administered in hospitalized patients. Detailed Description: The aim of the study is to prove that the continuous infusion of antibiotic treatment for the patients with Enterococcus faecalis infective endocarditis is as effective and safe as the traditional intermittent infusion. The continuous infusion modality of treatment is expected to provide numerous benefits for individual patients, global health, and for the National Health Care System by reducing to hospital stays from 4-6 weeks to approximately 2-3 weeks and hospital-driven complications. The mortality, rate of serious adverse events, total number of days of antibiotic treatment and days of hospitalization, among others, are included as secondary objectives. This is a pragmatic study as the number or visits performed for the study are similar to the normal clinical follow-up for this patients. Final contact and final visit for the study will be performed at 365 days after the 42 days of treatment. ### Conditions Module Conditions: - Endocarditis, Infective Keywords: - Endocarditis, Infective - Enterococcus faecalis - Antibiotics - Outpatient Infusion Therapies - Outpatient Care ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Parallel Assignment Randomized 1:1 to experimental group (continuous infusion arm) or control group (intermittent infusion arm) ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 200 Type: ESTIMATED Phases: - PHASE4 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Ampicillin 2g/4h plus ceftriaxone 2g/12h intermittently infused. The duration of treatment will be 42 days. Intervention Names: - Drug: Experimental regimen Label: Continuous intravenous antibiotic infusion Type: EXPERIMENTAL #### Arm Group 2 Description: Ampicillin 2g/4h plus ceftriaxone 2g/12h intermittent infusion. The duration of treatment will be 42 days. Intervention Names: - Drug: Control regimen Label: Intermittent intravenous antibiotic infusion Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Continuous intravenous antibiotic infusion Description: Continuous intravenous antibiotic infusion during 42 days for Infective Endocarditis Name: Experimental regimen Type: DRUG #### Intervention 2 Arm Group Labels: - Intermittent intravenous antibiotic infusion Description: Intermittent intravenous antibiotic infusion during 42 days for Infective Endocarditis Name: Control regimen Type: DRUG ### Outcomes Module #### Primary Outcomes Description: It is defined as follow: i) Confirmed recurrence of E. faecalis infective endocarditis, ii) all-cause mortality. A composite primary endpoint has been chosen to include both a very clinically relevant variable and a hard variable such as survival Measure: Clinical failure Time Frame: One year after the end of the treatment #### Secondary Outcomes Description: Number of deaths Measure: Therapeutic failure Time Frame: Up to 12 months after treatment administration Description: Number of patient of treatment switching Measure: Treatment switching Time Frame: 42 days Description: Number of unplanned cardiac surgeries Measure: Cardiac surgeries Time Frame: Up to 12 months after treatment administration Description: Number of unplanned readmissions Measure: Readmissions Time Frame: Up to 12 months after treatment administration Description: Number of medication-related adverse events Measure: Serious adverse events Time Frame: From randomisation until 30 days after the last dose administration Description: Number of antibiotic treatment days Measure: Antibiotic treatment days Time Frame: Up to 12 months after treatment administration Description: Number of Outpatient Parenteral Antimicrobial Therapy Measure: Outpatient Parenteral Antimicrobial Therapy Time Frame: Up to 12 months after treatment administration Description: Number of healthcare-associated infections Measure: Healthcare-associated infections Time Frame: Up to 12 months after treatment administration Description: Number of recurrence of Enterococcus faecalis infective endocarditis Measure: Recurrence Time Frame: Up to 12 months after treatment administration Description: Minimum free serum concentration of antibiotics used Measure: Minimum free serum concentration Time Frame: Day 14 Description: Steady-state plasma concentration of antibiotics used Measure: Steady-state plasma concentration Time Frame: Day 14 Description: Volume of distribution, clearance, elimination constant of antibiotics used Measure: Pharmacokinetic parameters Time Frame: Day 14 Description: Minimum Inhibitory Concentration of ampicillin induced by ceftriaxone in the strains responsible for recurrences and control strains Measure: Minimum Inhibitory Concentration Time Frame: Day 14 ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Adult patients * Possible or definitive diagnosis of infective endocarditis due to Enterococcus faecalis * Signed informed consent of patients Exclusion Criteria: * Allergy to penicillins or cephalosporins * Pregnancy and lactation * Polymicrobial infection including microorganisms different to E. faecalis Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Laura Herrera Hidalgo, MD-PhD Phone: +34955013414 Role: CONTACT Contact 2: Email: [email protected] Name: Clara M Rosso Fernández, MD-PhD Phone: +34955013414 Role: CONTACT #### Locations Location 1: City: Alava Contacts: *Contact 1:* - Email: [email protected] - Name: Juan Carlos Gainzarain, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario de Álava Zip: 01009 Location 2: City: Barakaldo Contacts: *Contact 1:* - Email: [email protected] - Name: Ane Josune Goikoetxea, MD - Role: CONTACT *Contact 2:* - Name: MD - Role: CONTACT Country: Spain Facility: Hospital Universitario de Cruces Zip: 48903 Location 3: City: Barcelona Contacts: *Contact 1:* - Email: [email protected] - Name: Nuria Fernández Hidalgo, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Vall d'Hebron Zip: 08035 Location 4: City: Barcelona Contacts: *Contact 1:* - Email: [email protected] - Name: Guillermo Cuervo Requena, MD - Role: CONTACT Country: Spain Facility: Hospital Clínico de Barcelona Zip: 08036 Location 5: City: Donostia Contacts: *Contact 1:* - Email: [email protected] - Name: Muskildav Goyeneche del Rio, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario de Donostia Zip: 20014 Location 6: City: Granada Contacts: *Contact 1:* - Email: [email protected] - Name: Carmen Hidalgo Tenorio, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Virgen de las Nieves Zip: 18014 Location 7: City: La Laguna Contacts: *Contact 1:* - Email: [email protected] - Name: Remedios Alemán, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario de Canarias Zip: 38320 Location 8: City: Logroño Contacts: *Contact 1:* - Email: [email protected] - Name: Jorge Alba Fernandez, MD - Role: CONTACT Country: Spain Facility: Hospital San Pedro Zip: 26006 Location 9: City: Madrid Contacts: *Contact 1:* - Email: [email protected], [email protected] - Name: Víctor José Gonzalez Ramallo, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Gregorio Marañón Zip: 28007 Location 10: City: Madrid Contacts: *Contact 1:* - Email: [email protected] - Name: Belén Loeches, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario La Paz Zip: 28046 Location 11: City: Madrid Contacts: *Contact 1:* - Email: [email protected] - Name: Jorge Calderón Parra - Role: CONTACT Country: Spain Facility: Hospital Universitario Puerta del Hierro Zip: 28222 Location 12: City: Málaga Contacts: *Contact 1:* - Email: [email protected] - Name: Antonio Plata Ciézar, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Regional de Málaga Zip: 29010 Location 13: City: Málaga Contacts: *Contact 1:* - Email: [email protected] - Name: Guillermo Ojeda Burgos, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Virgen de la Victoria Zip: 29010 Location 14: City: Santander Contacts: *Contact 1:* - Email: [email protected] - Name: Mª Carmen Fariñas, MD - Role: CONTACT *Contact 2:* - Name: MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Marqués de Valdecilla Zip: 39008 Location 15: City: Sevilla Contacts: *Contact 1:* - Email: [email protected] - Name: Luis Eduardo López Cortés, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Virgen Macarena Zip: 41009 Location 16: City: Sevilla Contacts: *Contact 1:* - Email: [email protected] - Name: Cesar Aristides de Alarcon gonzalez, MD - Role: CONTACT Country: Spain Facility: Hospital Universitario Virgen del Rocío Zip: 41013 Location 17: City: Terrassa Contacts: *Contact 1:* - Email: [email protected] - Name: Beatriz Dietl Gómez-Luengo, MD - Role: CONTACT Country: Spain Facility: Hospital Universitari MútuaTerrassa Zip: 08221 #### Overall Officials Official 1: Affiliation: Fundación para la Gestión de la Investigación en Salud de Sevilla Name: HUVR Cesar Arístides de Alarcón González, MD-PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: Direct collaborators within the study Description: The results will be shared with the investigators involved in the study, and will be shared when the analysis of the results is performed. Info Types: - STUDY_PROTOCOL - SAP - ICF IPD Sharing: YES Time Frame: 6 months ## Derived Section ### Condition Browse Module - Ancestors - ID: D000006331 - Term: Heart Diseases - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000001424 - Term: Bacterial Infections - ID: D000001423 - Term: Bacterial Infections and Mycoses - ID: D000007239 - Term: Infections - ID: D000053821 - Term: Cardiovascular Infections ### Condition Browse Module - Browse Branches - Abbrev: BC01 - Name: Infections - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M7859 - Name: Endocarditis, Bacterial - Relevance: HIGH - As Found: Infective Endocarditis - ID: M7858 - Name: Endocarditis - Relevance: HIGH - As Found: Endocarditis - ID: M9419 - Name: Heart Diseases - Relevance: LOW - As Found: Unknown - ID: M10283 - Name: Infections - Relevance: LOW - As Found: Unknown - ID: M6368 - Name: Communicable Diseases - Relevance: LOW - As Found: Unknown - ID: M4722 - Name: Bacterial Infections - Relevance: LOW - As Found: Unknown - ID: M12136 - Name: Mycoses - Relevance: LOW - As Found: Unknown - ID: M4721 - Name: Bacterial Infections and Mycoses - Relevance: LOW - As Found: Unknown - ID: M27489 - Name: Cardiovascular Infections - Relevance: LOW - As Found: Unknown - ID: T3065 - Name: Infective Endocarditis - Relevance: HIGH - As Found: Infective Endocarditis ### Condition Browse Module - Meshes - ID: D000004697 - Term: Endocarditis, Bacterial - ID: D000004696 - Term: Endocarditis ### Intervention Browse Module - Browse Branches - Abbrev: Infe - Name: Anti-Infective Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M4222 - Name: Anti-Bacterial Agents - Relevance: LOW - As Found: Unknown - ID: M5693 - Name: Ceftriaxone - Relevance: LOW - As Found: Unknown - ID: M4003 - Name: Ampicillin - Relevance: LOW - As Found: Unknown - ID: M4224 - Name: Antibiotics, Antitubercular - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423885 Brief Title: A Study of BL-M07D1+PD-1 Monoclonal Antibody and BL-M07D1+PD-1 Monoclonal Antibody+Capecitabine in Patients With Locally Advanced or Metastatic HER2-positive Gastric or Gastroesophageal Junction Adenocarcinoma Official Title: A Phase II Clinical Trial to Evaluate the Efficacy and Safety of BL-M07D1+PD-1 Monoclonal Antibody and BL-M07D1+PD-1 Monoclonal Antibody+Capecitabine as First-line Treatment in Patients With Unresectable Locally Advanced or Metastatic HER2-positive Gastric or Gastroesophageal Junction Adenocarcinoma #### Organization Study ID Info ID: BL-M07D1-206 #### Organization Class: INDUSTRY Full Name: Sichuan Baili Pharmaceutical Co., Ltd. ### Status Module #### Completion Date Date: 2026-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-29 Type: ACTUAL Last Update Submit Date: 2024-05-27 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-06 Type: ESTIMATED #### Start Date Date: 2024-06 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: INDUSTRY Name: Baili-Bio (Chengdu) Pharmaceutical Co., Ltd. #### Lead Sponsor Class: INDUSTRY Name: Sichuan Baili Pharmaceutical Co., Ltd. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This study is a multicenter, open-label, phase II clinical trial to evaluate the safety and efficacy of BL-M07D1+PD-1 monoclonal antibody and BL-M07D1+PD-1 monoclonal antibody+ capecitabine in patients with unresectable locally advanced or metastatic HER2-positive gastric or gastroesophageal junction adenocarcinoma. ### Conditions Module Conditions: - HER2-positive Gastric or Gastroesophageal Junction Adenocarcinoma ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 86 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants received BL-M07D1+PD-1 monoclonal antibody and BL-M07D1+PD-1 monoclonal antibody+ capecitabine in the first cycle (3 weeks). Participants who had a clinical benefit could receive additional cycles of additional treatment. Administration will be discontinued because of disease progression or intolerable toxicity or for other reasons. Intervention Names: - Drug: BL-M07D1 - Drug: PD-1 monoclonal antibody - Drug: Capecitabine Label: Study treatment Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Study treatment Description: Administration by intravenous infusion for a cycle of 3 weeks. Name: BL-M07D1 Type: DRUG #### Intervention 2 Arm Group Labels: - Study treatment Description: Administration by intravenous infusion for a cycle of 3 weeks. Name: PD-1 monoclonal antibody Type: DRUG #### Intervention 3 Arm Group Labels: - Study treatment Description: Oral administration for a cycle of 3 weeks. Name: Capecitabine Type: DRUG ### Outcomes Module #### Primary Outcomes Description: ORR is defined as the percentage of participants, who has a CR (disappearance of all target lesions) or PR (at least a 30% decrease in the sum of diameters of target lesions). The percentage of participants who experiences a confirmed CR or PR is according to RECIST 1.1. Measure: Objective Response Rate (ORR) Time Frame: Up to approximately 24 months Description: TEAE is defined as any unfavorable and unintended change in the structure, function, or chemistry of the body temporally emerging, or any worsening (i.e., any clinically significant adverse change in frequency and/or intensity) of a pre-existing condition during the treatment of BL-M07D1. The type, frequency and severity of TEAE will be evaluated during the treatment of BL-M07D1. Measure: Treatment-Emergent Adverse Event (TEAE) Time Frame: Up to approximately 24 months #### Secondary Outcomes Description: The PFS is defined as the time from the participant's first dose of BL-M07D1 to the first date of either disease progression or death, whichever occurs first. Measure: Progression-free Survival (PFS) Time Frame: Up to approximately 24 months Description: Overall survival (OS) is defined as the time between the subject's randomization date and subject's death. Measure: Overall survival (OS) Time Frame: Up to approximately 24 months Description: The DCR is defined as the percentage of participants who has a CR, PR, or Stable Disease (SD: neither sufficient shrinkage to qualify for PR nor sufficient increase to qualify for progressive disease \[PD: at least a 20% increase in the sum of diameters of target lesions and an absolute increase of at least 5 mm. The appearance of one or more new lesions is also considered PD\]). Measure: Disease Control Rate (DCR) Time Frame: Up to approximately 24 months Description: he DOR for a responder is defined as the time from the participant's initial objective response to the first date of either disease progression or death, whichever occurs first. Measure: Duration of Response (DOR) Time Frame: Up to approximately 24 months Description: Maximum serum concentration (Cmax) of BL-M07D1 will be investigated. Measure: Cmax Time Frame: Up to approximately 24 months Description: Time to maximum serum concentration (Tmax) of BL-M07D1 will be investigated. Measure: Tmax Time Frame: Up to approximately 24 months Description: Ctrough is defined as the lowest serum concentration of BL-M07D1 prior to the next dose will be administered. Measure: Ctrough Time Frame: Up to approximately 24 months Description: Frequency of anti-BL-M07D1 antibody (ADA) will be investigated. Measure: ADA (anti-drug antibody) Time Frame: Up to approximately 24 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Voluntarily sign the informed consent and follow the requirements of the protocol; 2. No gender limit; 3. Age ≥18 years old and ≤75 years old at the time of signing the informed consent; 4. Expected survival time ≥3 months; 5. Patients with HER2-positive gastric or gastroesophageal junction adenocarcinoma confirmed by histopathology and/or cytology; 6. Provide tumor tissue samples within 2 years for detection of biomarkers such as HER2; 7. Must have at least one measurable lesion according to RECIST v1.1 definition; 8. ECOG 0 or 1; 9. Toxicity of previous antineoplastic therapy has returned to ≤ grade 1 defined by NCI-CTCAE v5.0; 10. No severe cardiac dysfunction, left ventricular ejection fraction ≥50%; 11. Blood transfusion is not allowed within 14 days before the first use of study drugs, and the use of colony-stimulating factors is not allowed, and the organ function level must meet the requirements; 12. Coagulation function: international normalized ratio (INR) ≤1.5 and activated partial thromboplastin time (APTT) ≤1.5×ULN; 13. Urine protein ≤2+ or ≤1000mg/24h; 14. Fertile female subjects or male subjects with fertile partners must use highly effective contraception from 7 days before the first dose until 24 weeks after the dose. Female subjects of childbearing potential had to have a negative serum pregnancy test within 7 days before the first dose. Exclusion Criteria: 1. Major surgery within 4 weeks before the first dose, palliative radiotherapy within 2 weeks before the first dose, etc; 2. Prior ADC drug therapy with camptothecin derivative as toxin; 3. The history of severe cardiovascular and cerebrovascular diseases in the past six months; 4. Serious impairment of lung function due to pulmonary diseases; 5. QT prolongation, complete left bundle branch block, III degree atrioventricular block, frequent and uncontrollable arrhythmia; 6. Other primary malignancies diagnosed within 5 years before the first dose; 7. Poorly controlled hypertension; 8. A history of ILD requiring steroid therapy, current ILD/interstitial pneumonia or suspected to have such a condition during screening; 9. Patients with active central nervous system metastases; 10. Patients who are allergic to any excipients of the trial drug; 11. Systemic corticosteroids or immunosuppressive agents are required within 2 weeks before study dosing; 12. Patients with massive or symptomatic effusions or poorly controlled effusions; 13. Severe systemic infection within 4 weeks before screening; 14. Active autoimmune and inflammatory diseases; 15. Human immunodeficiency virus antibody positive, active hepatitis B virus infection or hepatitis C virus infection; 16. Previous history of allogeneic stem cell, bone marrow or organ transplantation; 17. A history of severe neurological or psychiatric illness; 18. Pregnant or lactating women; 19. The presence of other serious physical or laboratory abnormalities or poor compliance may increase the risk of participating in the study risk, or interference with the results of the study, and patients who were deemed by the investigators to be unsuitable for participation in the study. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Sa Xiao, PHD Phone: 15013238943 Role: CONTACT #### Locations Location 1: City: Shanghai Contacts: *Contact 1:* - Name: Weijian Guo - Role: CONTACT Country: China Facility: Fudan University Shanghai Cancer Center State: Shanghai #### Overall Officials Official 1: Affiliation: Fudan University Name: Weijian Guo Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000002277 - Term: Carcinoma - ID: D000009375 - Term: Neoplasms, Glandular and Epithelial - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000005770 - Term: Gastrointestinal Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000006258 - Term: Head and Neck Neoplasms - ID: D000004066 - Term: Digestive System Diseases - ID: D000004935 - Term: Esophageal Diseases - ID: D000005767 - Term: Gastrointestinal Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: All - Name: All Conditions - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M3585 - Name: Adenocarcinoma - Relevance: HIGH - As Found: Adenocarcinoma - ID: M8088 - Name: Esophageal Neoplasms - Relevance: HIGH - As Found: Gastroesophageal Junction Adenocarcinoma - ID: M5534 - Name: Carcinoma - Relevance: LOW - As Found: Unknown - ID: M12320 - Name: Neoplasms, Glandular and Epithelial - Relevance: LOW - As Found: Unknown - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M9348 - Name: Head and Neck Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M8085 - Name: Esophageal Diseases - Relevance: LOW - As Found: Unknown - ID: T2141 - Name: Esophageal Cancer - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000000230 - Term: Adenocarcinoma - ID: D000004938 - Term: Esophageal Neoplasms ### Intervention Browse Module - Ancestors - ID: D000007155 - Term: Immunologic Factors - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000000964 - Term: Antimetabolites, Antineoplastic - ID: D000000963 - Term: Antimetabolites - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000000970 - Term: Antineoplastic Agents ### Intervention Browse Module - Browse Branches - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: ANeo - Name: Antineoplastic Agents ### Intervention Browse Module - Browse Leaves - ID: M4225 - Name: Antibodies - Relevance: HIGH - As Found: Given - ID: M4230 - Name: Antibodies, Monoclonal - Relevance: HIGH - As Found: Chemotherapy - ID: M377 - Name: Capecitabine - Relevance: HIGH - As Found: Function - ID: M10184 - Name: Immunoglobulins - Relevance: LOW - As Found: Unknown - ID: M10201 - Name: Immunologic Factors - Relevance: LOW - As Found: Unknown - ID: M4281 - Name: Antimetabolites - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000069287 - Term: Capecitabine - ID: D000000906 - Term: Antibodies - ID: D000000911 - Term: Antibodies, Monoclonal ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423872 Brief Title: A SAD Study of ZT002 Injection in Healthy Participants Official Title: A Phase 1, Randomized, Parallel Assignment, Double Blind, Placebo Controlled, Single and Multiple Ascending Dose, Safety, Tolerability, and Pharmacokinetic Study of ZT002 in Healthy Participants #### Organization Study ID Info ID: BJQLZT002002 #### Organization Class: INDUSTRY Full Name: Beijing QL Biopharmaceutical Co.,Ltd ### Status Module #### Completion Date Date: 2023-12-08 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: COMPLETED #### Primary Completion Date Date: 2023-10-20 Type: ACTUAL #### Start Date Date: 2023-06-19 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER_GOV Name: Beijing Hospital #### Lead Sponsor Class: INDUSTRY Name: Beijing QL Biopharmaceutical Co.,Ltd #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This study will comprise a randomized, parallel assignment, double blind, placebo controlled, single and multiple ascending dose, safety, tolerability and pharmacokinetic study of ZT002 in healthy participants. ### Conditions Module Conditions: - Type 2 Diabetes Mellitus ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: QUADRUPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 28 Type: ACTUAL Phases: - PHASE1 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants will be randomized to receive ZT002 injection or Placebo in 1 of 6 dose cohorts. Intervention Names: - Drug: ZT002 Label: ZT002 Type: EXPERIMENTAL #### Arm Group 2 Description: Participants will be randomized to receive ZT002 injection or Placebo in 1 of 6 dose cohorts. Intervention Names: - Other: Placebo Label: Placebo Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - ZT002 Description: Participants will receive a single subcutaneous (SC) ZT002 injection. Name: ZT002 Type: DRUG #### Intervention 2 Arm Group Labels: - Placebo Description: Participants will receive same volume as of the study drug. Name: Placebo Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Coded by the most updated version of the Medical Dictionary for Regulatory Activities (MedDRA). Measure: Safety and tolerability of a single escalation dose of ZT002 through the incidence and severity of treatment emergent adverse events in SAD Cohorts. Number of participants with treatment-emergent adverse events Time Frame: Up to 50 days Description: Coded by the most updated version of the Medical Dictionary for Regulatory Activities (MedDRA). Measure: Safety and tolerability of a single escalation dose of ZT002 through the incidence severity of serious adverse events in SAD Cohorts. Number of participants with serious adverse events. Time Frame: Up to 50 days #### Secondary Outcomes Description: Parameter: Maximum observed plasma concentration of ZT002 (Cmax) Measure: The Pharmacokinetics (PK) profile of a single escalation dose of ZT002 in healthy participants in SAD Cohorts. Time Frame: Up to 50 days Description: Parameter: Area under the drug-time curve from 0 h after dosing to the last quantifiable concentration time point (AUC0-last) Measure: The Pharmacokinetics (PK) profile of a single escalation dose of ZT002 in healthy participants in SAD Cohorts. Time Frame: Up to 50 days Description: Parameter: Area under the drug-time curve to infinity (AUC0-inf) Measure: The Pharmacokinetics (PK) profile of a single escalation dose of ZT002 in healthy participants in SAD cohorts. Time Frame: Up to 50 days ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Fully understand the purpose, nature, methods, and potential adverse reactions of the experiment, voluntarily participate as a participant, comply with the requirements of this study, and sign an informed consent form. 2. Healthy adults, age 18\~45 years, both inclusive, at time of informed consent. 3. Body Mass Index (BMI) between 19～27.0 kg/m2 both included. Male weight\>55.0kg, famale weight\>50.0kg. 4. In good health, determined by no clinically significant findings from medical history, physical examination, vital signs measurements, anterior and lateral chest X-ray,12-lead ECG, and clinical laboratory evaluations(blood routine, blood biochemistry, coagulation function, and urine routine)at screening and before administration of study drug, as assessed by the Investigator. 5. Female participants are required to abstain or use two effective contraceptive methods simultaneously from 1 month before screening to 6 months after the last dose. Male participants are required to abstain or use two effective contraceptive methods simultaneously from the first dose to 6 months after the last dose: male participants are required to undergo surgical sterilization (such as vas deferens ligation) or use condoms correctly, or their spouse is required to use hormonal contraceptives approved by the National Medical Products Administration (such as contraceptive pills, patches, implantable or injectable preparations) or intrauterine devices (IUDs) or undergo surgical sterilization; Female subjects may undergo surgical sterilization (such as tubal ligation) or intrauterine devices (IUDs), or their spouses may use condoms correctly or undergo surgical sterilization. After the trial, female subjects may also use hormone contraceptives approved by the National Medical Products Administration (such as contraceptive pills, patches, implantable or injectable preparations). Exclusion Criteria: 1. History of drug allergy or allergic related diseases (allergic rhinitis, asthma, urticaria, eczema, etc.)，allergic to experimental drugs and excipients or GLP-1 class drugs. 2. Significant history or clinical manifestation of any neurological, cardiovascular, hematological, hepatic, renal, gastrointestinal, respiratory, metabolic, endocrine, immune or skeletal, as determined by the Investigator. 3. Family or personal history of medullary thyroid carcinoma (MTC). 4. Medical history of multiple endocrine neoplasia type 2(MEN2). 5. History of acute or chronic pancreatitis. 6. History of hypoglycemia. 7. Calcitonin equal or above 50 ng/L at screening. 8. The content of amylase or lipase during the screening period is higher than the upper limit of normal values and has clinical significance. 9. Screening period HbAlc (glycated hemoglobin) ≥ 6.5%. 10. According to the Fridericias formula，QTcF ≥ 450 ms for subjects in 12-lead ECG examination during screening or baseline period. 11. History of drug abuse within the previous year of screening or positive results from drug abuse screening (urine screening). 12. Have smoked ≥5 cigarettes per day in the past 3 month prior to Screening or unable to refrain from smoking during the study. 13. Screening for subjects who have consumed more than 14 units of alcohol per week within the first 3 months (1 unit of alcohol=360 mL of beer or 45 mL of 40% alcohol or 150 mL of wine), or who have taken alcoholic products within 48 hours before administration, or who cannot abstain from alcohol during the trial period. 14. Positive test for hepatitis B surface antigen (HBsAg)，hepatitis C antibody (HCV-Ab), human immunodeficiency virus (HIV-Ab) antibody, treponema pallidum(TP-Ab) antibody at screening. 15. Screening for subjects who have participated in other clinical trials and received drug therapy or medical device intervention within the first 3 months. 16. Blood donation or blood loss - more than 400 mL during the 3 months prior to screening, or received blood transfusion; or blood donation or blood loss - more than 200 mL during the 1 months prior to screening. 17. History of infectious diseases within 4 weeks before screening (judged by the investigator to affect the ability of the subject to participate in the test) 18. Cannot tolerate venous puncture blood collection or have a history of fainting or fainting 19. Received vaccination within 28 days prior to administration or plan to receive vaccination during the study period. 20. Use of prescription or non-prescription or chinese herbal medicine or discontinue medication before 1 month to screening or within 5 half-lives of the medicinal product, (whichever is longest). 21. Participant is unable to refrain from strenuous exercise during the study 22. Breastfeeding or pregnant women, or positive tests of pregnancy in screening or baseline 23. Other unsuitable conditions to participate in the clinical study judged by the investigator. Healthy Volunteers: True Maximum Age: 45 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT ### Contacts Locations Module #### Locations Location 1: City: Beijing Country: China Facility: Beijing Hospital State: Beijing #### Overall Officials Official 1: Affiliation: No.1 Dahua Road, Dongdan, Dongcheng District, Beijing Name: Aixin Shi, Master Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000003920 - Term: Diabetes Mellitus - ID: D000044882 - Term: Glucose Metabolism Disorders - ID: D000008659 - Term: Metabolic Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M7119 - Name: Diabetes Mellitus, Type 2 - Relevance: HIGH - As Found: Type 2 Diabetes Mellitus - ID: M11639 - Name: Metabolic Diseases - Relevance: LOW - As Found: Unknown - ID: M25403 - Name: Glucose Metabolism Disorders - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003924 - Term: Diabetes Mellitus, Type 2 ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423859 Brief Title: Articaine Plus Dexmedetomidine in Supraclavicular Block Official Title: A Comparative Study Between Articaine Alone Versus Articaine Plus Dexmedetomidine for Ambulatory Orthopedic Surgery Under Supraclavicular Block #### Organization Study ID Info ID: RC 19-1-2024 #### Organization Class: OTHER Full Name: Benha University ### Status Module #### Completion Date Date: 2024-08-20 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-22 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-08-01 Type: ESTIMATED #### Start Date Date: 2024-02-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Benha University #### Responsible Party Investigator Affiliation: Benha University Investigator Full Name: Samar Rafik Mohamed Amin Investigator Title: Assistant professor of anaesthesia and intensive care Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: Articaine has emerged as a local anesthetic (LA) that produces sensory and motor blockade shorter than bupivacaine and lower in neurotoxicity than lidocaine. Studies have shown that adding dexmedetomidine to LA produces prolongation of sensory and motor bock duration. Early regain of motor power with adequate analgesia is needed in ambulatory surgery, for early start of physiotherapy. This study was designed to test efficacy of adding dexmedetomidine to articaine on the duration of sensory and motor block. Detailed Description: Articaine is an amide LA produced in the 1960s and first used in clinical trials in 1974. Although it is an amide that is similar to prilocaine in chemical structure, it contains a thiophene ring rather than a benzene ring. Articaine is a rapid and short acting LA, which has low neurotoxicity and appears to diffuse through tissues more readily than other commonly used LA agents. It is metabolized by nonspecific plasma esterases both in blood and tissues, leading to its rapid clearance. α2-adrenergic receptor agonists have been the focus of interest for their sedative, analgesic, perioperative sympatholytic, and cardiovascular stabilizing effects along with providing reduction in anesthetic requirements. Dexmedetomidine may act on supraspinal (locus coeruleus) or spinal level or peripheral α2-adrenoreceptor to reduce nociceptive transmission, leading to analgesia. Previous trials focused on adding dexmedetomidine to either levobupivacaine and bupivacaine, found augmentation of both sensory and motor block along with prolonged duration of effective analgesia. However, there remains limited knowledge of the analgesic efficacy and clinical utility of adding dexmedetomidine to articaine during peripheral nerve block in humans. ### Conditions Module Conditions: - Post Operative Pain, Acute ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: TRIPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 66 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: supraclavicular brachial plexus block will be performed in this group guided by ultrasound. A 30 ml volume local anesthetic will be injected in the form of (29 cc articaine 2% + 1 cc isotonic saline) Intervention Names: - Drug: Articaine Label: Articaine alone Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: supraclavicular brachial plexus block will be performed in this group guided by ultrasound. A 30 ml volume local anesthetic will be injected in the form of (29 cc articaine 2% + 1 cc volume of Dexmedetomidine 1 ug/kg) Intervention Names: - Drug: Articaine - Drug: Dexmedetomidine Label: Articaine and Dexmedetomidine Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Articaine alone - Articaine and Dexmedetomidine Description: supraclavicular brachial plexus block with articaine 2% Name: Articaine Type: DRUG #### Intervention 2 Arm Group Labels: - Articaine and Dexmedetomidine Description: supraclavicular brachial plexus block with articaine 2% in addition with Dexmedetomidine Name: Dexmedetomidine Type: DRUG ### Outcomes Module #### Primary Outcomes Description: the time between the onset of sensory block to the complete resolution of anesthesia on all nerves distribution. Measure: Sensory block duration Time Frame: 24 hours post block #### Secondary Outcomes Description: The time between the end of the drug injection and the total abolition of pinprick sensation along the distribution of any of nerves - median, ulnar, radial, or musculocutaneous Measure: onset time of sensory block Time Frame: 15 minutes after block Description: the time between the end of the drug injection and Grade 1 motor block Measure: onset time for motor block Time Frame: 15 minutes after block Description: the time interval between the onset time of motor block and the recovery of complete motor function of that limb Measure: motor duration block Time Frame: 24 hours post block Description: time interval between the administration of local anesthesia solution and onset of pain at surgical site Measure: Analgesia time Time Frame: 24 hours postoperative ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * aged 18-60 years planned for upper limb surgery below the midhumerus with an expected time of less than 90 min usually under tourniquet. Exclusion Criteria: * allergies to local anesthetic, * those with ASA III and IV, * patients who refuse to participate, * uncooperative patients, * patients who have infection at the site of injection, * patients who have bleeding disorder, and patients on anticoagulant drugs. Maximum Age: 60 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Samar R Amin, MD Phone: +201287793991 Role: CONTACT Contact 2: Email: [email protected] Name: Elsayed M abdelzaam, MD Phone: 0133227518 Role: CONTACT #### Locations Location 1: City: Banhā Contacts: *Contact 1:* - Email: [email protected] - Name: Samar R. Amin, lecturer - Phone: 01287793991 - Role: CONTACT Country: Egypt Facility: Samar Rafik Mohamed Amin State: Qalubia Status: RECRUITING Zip: 13511 ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011183 - Term: Postoperative Complications - ID: D000010335 - Term: Pathologic Processes - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M13069 - Name: Pain, Postoperative - Relevance: HIGH - As Found: Post Operative Pain, Acute - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M14065 - Name: Postoperative Complications - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000010149 - Term: Pain, Postoperative ### Intervention Browse Module - Ancestors - ID: D000006993 - Term: Hypnotics and Sedatives - ID: D000002492 - Term: Central Nervous System Depressants - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000018712 - Term: Analgesics, Non-Narcotic - ID: D000000700 - Term: Analgesics - ID: D000018689 - Term: Sensory System Agents - ID: D000018373 - Term: Peripheral Nervous System Agents - ID: D000058647 - Term: Adrenergic alpha-2 Receptor Agonists - ID: D000000316 - Term: Adrenergic alpha-Agonists - ID: D000000322 - Term: Adrenergic Agonists - ID: D000018663 - Term: Adrenergic Agents - ID: D000018377 - Term: Neurotransmitter Agents - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000000779 - Term: Anesthetics, Local - ID: D000000777 - Term: Anesthetics ### Intervention Browse Module - Browse Branches - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Analg - Name: Analgesics ### Intervention Browse Module - Browse Leaves - ID: M4107 - Name: Anesthetics - Relevance: LOW - As Found: Unknown - ID: M22662 - Name: Dexmedetomidine - Relevance: HIGH - As Found: Twice daily - ID: M5609 - Name: Carticaine - Relevance: HIGH - As Found: Earlier - ID: M4109 - Name: Anesthetics, Local - Relevance: LOW - As Found: Unknown - ID: M10043 - Name: Hypnotics and Sedatives - Relevance: LOW - As Found: Unknown - ID: M4032 - Name: Analgesics - Relevance: LOW - As Found: Unknown - ID: M20786 - Name: Analgesics, Non-Narcotic - Relevance: LOW - As Found: Unknown - ID: M20746 - Name: Adrenergic Agents - Relevance: LOW - As Found: Unknown - ID: M3668 - Name: Adrenergic alpha-Agonists - Relevance: LOW - As Found: Unknown - ID: M3673 - Name: Adrenergic Agonists - Relevance: LOW - As Found: Unknown - ID: M20504 - Name: Neurotransmitter Agents - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000020927 - Term: Dexmedetomidine - ID: D000002355 - Term: Carticaine ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423846 Brief Title: Total Intravenous Anesthesia Versus Inhalation Anesthesia on Postoperative Liver Function Official Title: Comparison of Total Intravenous Anesthesia Versus Inhalation Anesthesia on Postoperative Liver Function in Patients With Non-Alcoholic Steatohepatitis Undergoing Laparoscopic Sleeve Gastrectomy: A Randomized Clinical Trial #### Organization Study ID Info ID: RC-3-4-2024 #### Organization Class: OTHER Full Name: Benha University ### Status Module #### Completion Date Date: 2024-05-12 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: COMPLETED #### Primary Completion Date Date: 2024-05-06 Type: ACTUAL #### Start Date Date: 2024-01-26 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Benha University #### Responsible Party Investigator Affiliation: Benha University Investigator Full Name: Ramy Mousa Investigator Title: Professor Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The pandemic of obesity has become a serious issue of public health worldwide as the size of the obese population has almost tripled over the last four decades and continues to riseزThe epidemic of obesity has led to a significant increase in the prevalence of non-alcoholic fatty liver disease (NAFLD). NAFLD is currently the most common chronic liver disease, with an estimated global prevalence at 25-30%, rising up to 90% in morbidly obese patients Detailed Description: Anesthesia and surgery may deteriorate liver function in patients with elevated liver enzyme levels; therefore, in these patients, choosing anaesthetics with less hepatotoxicity may be important. Halothane, which is a typical inhalational anesthetic, is known for its liver and kidney toxicity. The latest anesthetic agents, including sevoflurane and desflurane, are associated with less hepatotoxicity, although rare cases of acute liver injury have been reported with these agentsزPropofol (2,6-diisopropylphenol) is an intravenous anesthetic. Its pharmacokinetic profile makes it very suitable for total intravenous anesthesia (TIVA) and this is a widely used technique in many centers. Its use results in a rapid onset and offset with fewer side effects including postoperative nausea and vomiting, making it particularly favorable in the ambulatory setting ### Conditions Module Conditions: - Laparoscopic Sleeve Gastrectomy Keywords: - Total Intravenous Anesthesia - Inhalation Anesthesia - Laparoscopic Sleeve Gastrectomy ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: The participants were randomized into two equal groups using a computer-generated list of random numbers sealed in an opaque envelope and were randomly allocated into two groups on a scale of 1:1. ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 80 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients in the TIVA group had anesthesia induced with propofol 2 mg/kg , fentanyl 1 ug/kg and maintained with propofol. Intervention Names: - Drug: Total intravenous anesthesia group Label: total intravenous anesthesia group Type: EXPERIMENTAL #### Arm Group 2 Description: general anesthesia was induced with propofol 2 mg/kg, fentanyl 1 ug/kg and then maintained with sevoflurane in air and oxygen, dexmedetomidine 1 ug/kg/hour. Intervention Names: - Drug: sevoflurane group Label: sevoflurane group Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - total intravenous anesthesia group Description: Patients in the TIVA group had anesthesia induced with propofol 2 mg/kg , fentanyl 1 ug/kg and maintained with propofol. 200 ug/kg/min, fentanyl 0.1ug/kg/min, dexmedetomidine 1 ug/kg/hour Name: Total intravenous anesthesia group Other Names: - TIVA group Type: DRUG #### Intervention 2 Arm Group Labels: - sevoflurane group Description: For patients in the SEVO group, general anesthesia was induced with propofol 2 mg/kg, fentanyl 1 ug/kg and then maintained with sevoflurane in air and oxygen, dexmedetomidine 1 ug/kg/hour. Name: sevoflurane group Other Names: - SEVO group Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Pain was assessed by using the visual analogue scale (VAS) score for pain (0-no pain, 10-worst imaginable pain) Measure: visual analogue scale Time Frame: visual analogue scale was measured at day one and day two postoperatively #### Secondary Outcomes Description: 5-point Likert scale, (1=extremely dissatisfied; 5=extremely satisfied) Measure: Patient satisfaction Time Frame: 24 hours postoperatively ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Obese patients * had ASA I-III * diagnosed with non-alcoholic steatohepatitis (NASH) liver disease * undergoing laparoscopic sleeve gastrectomy Exclusion Criteria: * cases wherein surgeries were performed using anesthetic methods that were not clearly identified as TIVA or INHA * heart surgery or cesarean section, and cases of neuromuscular diseases Maximum Age: 70 Years Minimum Age: 20 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Banha Country: Egypt Facility: Benha University Zip: 13511 #### Overall Officials Official 1: Affiliation: Anesthesia and surgical ICU department, Faculty of Medicine, Benha University, Egypt Name: Ramy Saleh, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ### References Module #### References Citation: Ahmed OT, Gidener T, Mara KC, Larson JJ, Therneau TM, Allen AM. Natural History of Nonalcoholic Fatty Liver Disease With Normal Body Mass Index: A Population-Based Study. Clin Gastroenterol Hepatol. 2022 Jun;20(6):1374-1381.e6. doi: 10.1016/j.cgh.2021.07.016. Epub 2021 Jul 13. PMID: 34265444 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012120 - Term: Respiration Disorders - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000010335 - Term: Pathologic Processes ### Condition Browse Module - Browse Branches - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M27137 - Name: Respiratory Aspiration - Relevance: HIGH - As Found: Inhalation - ID: M8375 - Name: Fatty Liver - Relevance: LOW - As Found: Unknown - ID: M14957 - Name: Respiration Disorders - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: T5868 - Name: Visceral Steatosis - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000053120 - Term: Respiratory Aspiration ### Intervention Browse Module - Ancestors - ID: D000000777 - Term: Anesthetics - ID: D000002492 - Term: Central Nervous System Depressants - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000010975 - Term: Platelet Aggregation Inhibitors - ID: D000018685 - Term: Anesthetics, Inhalation - ID: D000018681 - Term: Anesthetics, General ### Intervention Browse Module - Browse Branches - Abbrev: AdjAn - Name: Adjuvants, Anesthesia - Abbrev: Analg - Name: Analgesics - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: PlAggInh - Name: Platelet Aggregation Inhibitors - Abbrev: Hemat - Name: Hematinics ### Intervention Browse Module - Browse Leaves - ID: M8418 - Name: Fentanyl - Relevance: LOW - As Found: Unknown - ID: M4107 - Name: Anesthetics - Relevance: LOW - As Found: Unknown - ID: M22662 - Name: Dexmedetomidine - Relevance: LOW - As Found: Unknown - ID: M18307 - Name: Propofol - Relevance: LOW - As Found: Unknown - ID: M1673 - Name: Sevoflurane - Relevance: HIGH - As Found: Less - ID: M11110 - Name: Liver Extracts - Relevance: LOW - As Found: Unknown - ID: M13865 - Name: Platelet Aggregation Inhibitors - Relevance: LOW - As Found: Unknown - ID: M20765 - Name: Anesthetics, Inhalation - Relevance: LOW - As Found: Unknown - ID: M20761 - Name: Anesthetics, General - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000077149 - Term: Sevoflurane ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423833 Brief Title: Trendelenburg Maneuver Versus Passive Leg Raising Test for Fluid Responsiveness in High-Risk Surgical Patients Official Title: Trendelenburg Maneuver Versus Passive Leg Raising Test for Fluid Responsiveness in High-Risk Surgical Patients #### Organization Study ID Info ID: 36264MD32/2/23 #### Organization Class: OTHER Full Name: Tanta University ### Status Module #### Completion Date Date: 2025-05-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-05-01 Type: ESTIMATED #### Start Date Date: 2023-02-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Tanta University #### Responsible Party Investigator Affiliation: Tanta University Investigator Full Name: Fatma Mohamed Samy Elaiashy Investigator Title: Assistant Lecturer of Anesthesiology, Surgical Intensive Care and Pain Medicine, Faculty of Medicine, Tanta University, Tanta, Egypt Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: The aim of this study is to evaluate whether Trendelenburg maneuver can be used to predict fluid responsiveness in high-risk surgical patients in intensive care unit as compared to Passive Leg Raising test. Detailed Description: Passive Leg Raising test is a well validated dynamic method to predict fluid responsiveness with many advantages as it doesn't use fluid loading, its effect is reversible, and it doesn't rely on heart-lung interaction. However, it has many limitations as (has false negative effect in patients with intra-abdominal hypertension), also, it may not be suitable in some surgical patients. Trendelenburg maneuver (TM) is often used to treat hemodynamic unstable patients when hypovolemia is suspected, through a mechanism similar to Passive Leg Raising test Yonis, et al reports that change in cardiac output during Trendelenburg maneuver is a reliable predictor of fluid responsiveness in patients with acute respiratory distress syndrome in prone position under protective ventilation. Another study reports that change in velocity time integral during trendelenburg maneuver predicts fluid responsiveness in cardiac surgical patients in operating rooms ### Conditions Module Conditions: - Trendelenburg Maneuver - Passive Leg Raising - High-Risk Surgical Patients ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: DIAGNOSTIC #### Enrollment Info Count: 60 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The investigator will measure changes in velocity time integral (VTI) and stroke volume (SV) during Trendelenburg maneuver (TM) in high-risk surgical patients by trans-thoracic Doppler echo cardiography Intervention Names: - Diagnostic Test: Trendelenburg maneuver (TM) Label: Trendelenburg maneuver Type: EXPERIMENTAL #### Arm Group 2 Description: The investigator will measure changes in velocity time integral (VTI) and stroke volume (SV) during passive leg raising (PLR) test in high-risk surgical patients by trans-thoracic Doppler echo cardiography Intervention Names: - Diagnostic Test: Passive leg raising test Label: Passive leg raising test Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Trendelenburg maneuver Description: The investigator will measure changes in velocity time integral (VTI) and stroke volume (SV) during Trendelenburg maneuver (TM) in high-risk surgical patients by trans-thoracic Doppler echo cardiography. Name: Trendelenburg maneuver (TM) Type: DIAGNOSTIC_TEST #### Intervention 2 Arm Group Labels: - Passive leg raising test Description: The investigator will measure changes in velocity time integral (VTI) and stroke volume (SV) during Passive leg raising (PLR) test in high-risk surgical patients by trans-thoracic Doppler echo cardiography. Name: Passive leg raising test Type: DIAGNOSTIC_TEST ### Outcomes Module #### Primary Outcomes Description: Measurement of the validity of Trendelenburg maneuver to predict fluid responsiveness by measuring the percentage change in velocity time integral (VTI) by Doppler echocardiography in high risk-surgical patients. Measure: The validity of Trendelenburg maneuver Time Frame: At the end of Trendelenburg maneuver within 1 minute #### Secondary Outcomes Description: Correlation between the accuracy of the percentage change in velocity time integral (VTI)during Trendelenburg maneuver and passive leg raising test will be measured. Measure: Correlation between the accuracy of the percentage change in velocity time integral (VTI) during Trendelenburg maneuver and passive leg raising test (PLR) test Time Frame: At the end of Trendelenburg maneuver and passive leg raising test within 1 minute ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Aged ≥ 18 years old. * Criteria of high-risk surgical patients: 1. Elderly ≥ 70 years old undergoing major surgery. 2. Physical status ≥ 3 or more undergoing major surgery. 3. Major intraoperative hemorrhage with Surgical Apgar Score (SAS 0-4). 4. Emergency of upper abdominal surgery. * Criteria of hypoperfusion ≥ 2 or more the following: 1. Mean arterial blood pressure \< 65 mmHg. 2. Urine output \< 0.5 ml/Kg/hr. 3. Capillary refilling time \> 4 seconds. 4. Blood lactate \> 2 mmol/L. 5. ScvO2 \< 70%. 6. CO2 gap \> 6 mmHg. * Provided that:SpO2 ≥ 90% and Hb ≥ 7 g/dl. Exclusion Criteria: * Patients with body mass index \> 35 kg/m2. * Pregnant female. * Contraindications to the Trendelenburg position or PLR test (major head trauma, intra-abdominal hypertension and gastric retention). * Poor echo window or unsatisfactory cardiac echogenicity (an inability to correctly align the Doppler beam to generate reliable velocity time integral measurements at the left ventricular outflow tract \[LVOT\]). Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Fatma M Elaiashy, Master Phone: 00201022514528 Role: CONTACT #### Locations Location 1: City: Tanta Contacts: *Contact 1:* - Email: [email protected] - Name: Fatma M Elaiashy, Master - Phone: 00201022514528 - Role: CONTACT *Contact 2:* - Name: Salah E Elsherif, MD - Role: SUB_INVESTIGATOR *Contact 3:* - Name: Hala M El-Gendy, MD - Role: SUB_INVESTIGATOR *Contact 4:* - Name: Sameh M Sadek, MD - Role: SUB_INVESTIGATOR *Contact 5:* - Name: Taysser M Abdalraheem, MD - Role: SUB_INVESTIGATOR Country: Egypt Facility: Tanta University Hospitals State: El-Gharbia Status: RECRUITING Zip: 31527 ### IPD Sharing Statement Module Access Criteria: The data will be available upon a reasonable request from the corresponding author Description: The data will be available upon a reasonable request from the corresponding author after the end of study for one year. Info Types: - STUDY_PROTOCOL IPD Sharing: YES Time Frame: After the end of study for one year. ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423820 Brief Title: Preoperative Ondansetron Lozenge for Prevention of Postoperative Nausea and Vomiting in Pediatrics Undergoing Squint Surgeries Official Title: Preoperative Ondansetron Lozenge for Prevention of Postoperative Nausea and Vomiting in Pediatrics Undergoing Squint Surgeries: A Randomized Controlled Trial #### Organization Study ID Info ID: 36264PR640/4/24 #### Organization Class: OTHER Full Name: Tanta University ### Status Module #### Completion Date Date: 2024-12-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-22 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-12-01 Type: ESTIMATED #### Start Date Date: 2024-05-21 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Tanta University #### Responsible Party Investigator Affiliation: Tanta University Investigator Full Name: Mohammed Said ElSharkawy Investigator Title: Lecturer of Anesthesiology, Surgical Intensive Care and Pain Medicine, Faculty of Medicine, Tanta University, Tanta, Egypt. Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: The aim of this study is to evaluate the role of ondansetron lozenge on prevention of postoperative nausea and vomiting (PONV) in pediatrics undergoing squint surgeries. Detailed Description: Post-operative nausea and vomiting (PONV) are two of the most common and distressing complications related to surgery and anesthesia. In several studies PONV occurred in 13% to 42% of pediatric surgical patients, while severe cases are less common, occurring in 1-3% of patients. Volatile anesthetics are the main cause in the early post-operative period (0-2 h), with dose-response relationship. In the delayed post-operative period (2-24 h) the main predictors are childhood, PONV in the early period, and the use of postoperative opioids. Ondansetron is generally considered to be the first-line antiemetic for patients because of its favorable side effect profile. Ondansetron reduces the activity of the vagus nerve, which deactivates the vomiting center in the medulla oblongata, and also blocks serotonin receptors in the chemoreceptor trigger zone, Ondansetron is an effective drug in the prevention and treatment of PONV by having low side effects. ### Conditions Module Conditions: - Ondansetron Lozenge - Postoperative Nausea and Vomiting - Pediatrics - Squint ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 80 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Pediatric patients will receive ondansetron lozenge 4 mg (Ondalenz ©), 2 hours before surgery as a study group. Intervention Names: - Drug: Ondansetron lozenge Label: Group S (Ondansetron lozenge) Type: EXPERIMENTAL #### Arm Group 2 Description: Pediatric patients will not receive ondansetron as a control group. Label: Group C (Control) Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Group S (Ondansetron lozenge) Description: Pediatric patients will receive ondansetron lozenge 4 mg (Ondalenz ©), 2 hours before surgery. Name: Ondansetron lozenge Type: DRUG ### Outcomes Module #### Primary Outcomes Description: The incidence of postoperative nausea and vomiting (PONV) will be measured in the first 24 postoperative hours at the intervals of 0-2h (early PONV), 2-12h (delayed PONV), and 12- 24h (late PONV) Measure: Incidence of postoperative nausea and vomiting Time Frame: 24 hours postoperatively #### Secondary Outcomes Description: The severity of postoperative nausea and vomiting (PONV) will be scored as follows: \[0 = no nausea and no retching; 1 complaining of sickness and retching; vomiting one or two times in 30 min; and 3 vomiting more than two times in 30 min\] in the first 24 hours postoperatively. Measure: Severity of postoperative nausea and vomiting (PONV) Time Frame: 24 hours postoperatively Description: Number of emetic episodes will be measured from the end of surgery till 24 hours postoperatively. Measure: Number of emetic episodes Time Frame: 24 hours postoperatively Description: Time to onset of emesis will be measured from the end of surgery till 24 hours postoperatively. Measure: Time to onset of emesis Time Frame: 24 hours postoperatively Description: Incidence of oculo-cardiac reflex (OCR) will be recorded. OCR is defined as a 10-20% decrease in the resting heart rate and/or the occurrence of any arrhythmia. Measure: Incidence of oculo-cardiac reflex (OCR) Time Frame: 24 hours postoperatively Description: Degree of parental satisfaction by using an 11-pointverbal numeric scoring system (0 = not at all satisfied, 10 = fully satisfied). Measure: Parental satisfaction Time Frame: 24 hours postoperatively ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age from 4 to 15 years. * American Society of Anesthesiology (ASA) physical status I, II. * Pediatric patients undergoing squint surgeries. Exclusion Criteria: * Patients who had received any medication with antiemetic properties within 24 h before surgery. * Post-operative period (for reasons other than rescue antiemetic therapy). * Patients with known liver or renal disease. * Patients with a history of vomiting or retching within 24 h before surgery. Maximum Age: 15 Years Minimum Age: 4 Years Sex: ALL Standard Ages: - CHILD ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Mohammed S Elsharkawy, MD Phone: 00201148207870 Role: CONTACT #### Locations Location 1: City: Tanta Contacts: *Contact 1:* - Email: [email protected] - Name: Mohammed S Elsharkawy, MD - Phone: 00201148207870 - Role: CONTACT *Contact 2:* - Name: Saad A Moharam, MD - Role: PRINCIPAL_INVESTIGATOR Country: Egypt Facility: Tanta University State: El-Gharbia Status: RECRUITING Zip: 31527 ### IPD Sharing Statement Module Access Criteria: The data will be available upon a reasonable request from the corresponding author. Description: The data will be available upon a reasonable request from the corresponding author after the end of study for one year. Info Types: - STUDY_PROTOCOL IPD Sharing: YES Time Frame: After the end of study for one year. ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012817 - Term: Signs and Symptoms, Digestive - ID: D000011183 - Term: Postoperative Complications - ID: D000010335 - Term: Pathologic Processes - ID: D000015835 - Term: Ocular Motility Disorders - ID: D000003389 - Term: Cranial Nerve Diseases - ID: D000009422 - Term: Nervous System Diseases - ID: D000005128 - Term: Eye Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC11 - Name: Eye Diseases ### Condition Browse Module - Browse Leaves - ID: M12273 - Name: Nausea - Relevance: HIGH - As Found: Nausea - ID: M17582 - Name: Vomiting - Relevance: HIGH - As Found: Vomiting - ID: M22074 - Name: Postoperative Nausea and Vomiting - Relevance: HIGH - As Found: Postoperative Nausea and Vomiting - ID: M16075 - Name: Strabismus - Relevance: HIGH - As Found: Squint - ID: M15622 - Name: Signs and Symptoms, Digestive - Relevance: LOW - As Found: Unknown - ID: M14065 - Name: Postoperative Complications - Relevance: LOW - As Found: Unknown - ID: M18386 - Name: Ocular Motility Disorders - Relevance: LOW - As Found: Unknown - ID: M6605 - Name: Cranial Nerve Diseases - Relevance: LOW - As Found: Unknown - ID: M8271 - Name: Eye Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000013285 - Term: Strabismus - ID: D000009325 - Term: Nausea - ID: D000014839 - Term: Vomiting - ID: D000020250 - Term: Postoperative Nausea and Vomiting ### Intervention Browse Module - Ancestors - ID: D000000932 - Term: Antiemetics - ID: D000001337 - Term: Autonomic Agents - ID: D000018373 - Term: Peripheral Nervous System Agents - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000005765 - Term: Gastrointestinal Agents - ID: D000000982 - Term: Antipruritics - ID: D000003879 - Term: Dermatologic Agents - ID: D000058831 - Term: Serotonin 5-HT3 Receptor Antagonists - ID: D000012702 - Term: Serotonin Antagonists - ID: D000018490 - Term: Serotonin Agents - ID: D000018377 - Term: Neurotransmitter Agents - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action ### Intervention Browse Module - Browse Branches - Abbrev: AnEm - Name: Antiemetics - Abbrev: Derm - Name: Dermatologic Agents - Abbrev: Gast - Name: Gastrointestinal Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M19588 - Name: Ondansetron - Relevance: HIGH - As Found: Dual - ID: M4251 - Name: Antiemetics - Relevance: LOW - As Found: Unknown - ID: M8881 - Name: Gastrointestinal Agents - Relevance: LOW - As Found: Unknown - ID: M7074 - Name: Dermatologic Agents - Relevance: LOW - As Found: Unknown - ID: M15512 - Name: Serotonin - Relevance: LOW - As Found: Unknown - ID: M29246 - Name: Serotonin 5-HT3 Receptor Antagonists - Relevance: LOW - As Found: Unknown - ID: M20504 - Name: Neurotransmitter Agents - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000017294 - Term: Ondansetron ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423807 Brief Title: Preoperative Ondansetron Lozenge for Prevention of Post-Spinal Shivering in Caesarean Section Official Title: Preoperative Ondansetron Lozenge for Prevention of Post-Spinal Shivering in Caesarean Section: A Randomized Controlled Trial #### Organization Study ID Info ID: 36264PR642/4/24 #### Organization Class: OTHER Full Name: Tanta University ### Status Module #### Completion Date Date: 2024-12-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-22 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-12-01 Type: ESTIMATED #### Start Date Date: 2024-05-21 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Tanta University #### Responsible Party Investigator Affiliation: Tanta University Investigator Full Name: Mohammed Said ElSharkawy Investigator Title: Lecturer of Anesthesiology, Surgical Intensive Care and Pain Medicine, Faculty of Medicine, Tanta University, Tanta, Egypt. Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: The aim of this study is to estimate the role of ondansetron lozenge on prevention of post-spinal shivering in cesarean section. Detailed Description: Spinal anesthesia (SA) is preferred for cesarean section (CS) compared with general anesthesia(GA) because of several advantages, including prevention of the potential risk of GA-related neurotoxicity. Post-spinal shivering (PSS) could be a provocative factor for postoperative pain and its appropriate treatment prevents non-thermoregulatory tremors. Shivering also causes aggravating postoperative pain by stretching of sutures. Ondansetron is a selective antagonist for receptor 5-hydroxytryptamine 3 and is very effective in the prevention and treatment of shivering intra- and post-operation. Ondansetron can affect the body temperature and shivering in rats since the balance of nor-epinephrine and 5-hydroxytryptamine (5-HT) in the preoptic-anterior hypothalamus controls the temperature set point. ### Conditions Module Conditions: - Ondansetron Lozenge - Post-Spinal Shivering - Cesarean Section ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 60 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients will receive ondansetron lozenge 4 mg (Ondalenz ©), 2 hours before surgery as a study group. Intervention Names: - Drug: Ondansetron lozenge Label: Group S (Ondansetron lozenge) Type: EXPERIMENTAL #### Arm Group 2 Description: Patients will not receive ondansetron as a control group. Label: Group C (Control) Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Group S (Ondansetron lozenge) Description: Patients will receive ondansetron lozenge 4 mg (Ondalenz ©), 2 hours before surgery. Name: Ondansetron lozenge Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Shivering will be graded during the intraoperative and postoperative period using the scale validated by Crossley and Mahajan and Tsai and Chu. 0=No shivering, 1=Piloerection or peripheral vasoconstriction but no visible shivering, 2=Muscular activity in only one muscle group, 3=Muscular activity in more than one muscle group but not generalized shivering, 4=Shivering involving the whole body. Grades 3, and 4 shivering for at least 3 min will be considered positive, and maximum shivering will be considered if generalized shivering interfering with ECG monitoring or ability of the mother to hold the baby. Measure: Incidence of shivering Time Frame: 24 hours postoperatively #### Secondary Outcomes Description: The incidence of nausea and vomiting will be evaluated through the Bellville scoring scale (lack of nausea and vomiting=0, nausea=1, nausea with belching=2, and vomiting=3). Measure: Incidence of postoperative nausea and vomiting (PONV) Time Frame: 24 hours postoperatively Description: • Degree of patient satisfaction will be assessed on a 5-point Likert scale patient satisfaction (1, extremely dissatisfied; 2, unsatisfied; 3, neutral; 4, satisfied; 5, extremely satisfied). Measure: Patients' satisfaction Time Frame: 24 hours postoperatively Description: Adverse events such as bradycardia, hypotension, respiratory depression, or any other complication will be recorded. Measure: Adverse effects Time Frame: 24 hours postoperatively ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age from 18 to 40 years. * American Society of Anesthesiology (ASA) physical status II. * Parturient women undergoing CS under spinal anesthesia. Exclusion Criteria: * Parturient women with any contraindication or hypersensitivity to the study drugs. * Any history of cardiovascular diseases, psychosis, hypertension, fetal distress, cord prolapse initial. * Temperature more than 38°C or less than 36°C. * Body Mass Index (BMI)\> 40 kg/m2. * Medical history of alcohol or drug abuse. * Parkinson's disease or any extrapyramidal disease. * Intraoperative blood transfusion. * History of chemotherapy treatment. Gender Based: True Gender Description: Parturient women undergoing cesarean section under spinal anesthesia Maximum Age: 40 Years Minimum Age: 18 Years Sex: FEMALE Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Mohammed S Elsharkawy, MD Phone: 00201148207870 Role: CONTACT #### Locations Location 1: City: Tanta Contacts: *Contact 1:* - Email: [email protected] - Name: Mohammed S Elsharkawy, MD - Phone: 00201148207870 - Role: CONTACT *Contact 2:* - Name: Saad A Moharam, MD - Role: PRINCIPAL_INVESTIGATOR Country: Egypt Facility: Tanta University State: El-Gharbia Status: RECRUITING Zip: 31527 #### Overall Officials Official 1: Affiliation: Faculty of Medicine Tanta University, Egypt Name: Mohammed S Elsharkawy, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: The data will be available upon a reasonable request from the corresponding author. Description: The data will be available upon a reasonable request from the corresponding author after the end of study for one year. Info Types: - STUDY_PROTOCOL IPD Sharing: YES Time Frame: After the end of study for one year. ## Derived Section ### Intervention Browse Module - Ancestors - ID: D000000932 - Term: Antiemetics - ID: D000001337 - Term: Autonomic Agents - ID: D000018373 - Term: Peripheral Nervous System Agents - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000005765 - Term: Gastrointestinal Agents - ID: D000000982 - Term: Antipruritics - ID: D000003879 - Term: Dermatologic Agents - ID: D000058831 - Term: Serotonin 5-HT3 Receptor Antagonists - ID: D000012702 - Term: Serotonin Antagonists - ID: D000018490 - Term: Serotonin Agents - ID: D000018377 - Term: Neurotransmitter Agents - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action ### Intervention Browse Module - Browse Branches - Abbrev: AnEm - Name: Antiemetics - Abbrev: Derm - Name: Dermatologic Agents - Abbrev: Gast - Name: Gastrointestinal Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M19588 - Name: Ondansetron - Relevance: HIGH - As Found: Dual - ID: M4251 - Name: Antiemetics - Relevance: LOW - As Found: Unknown - ID: M8881 - Name: Gastrointestinal Agents - Relevance: LOW - As Found: Unknown - ID: M7074 - Name: Dermatologic Agents - Relevance: LOW - As Found: Unknown - ID: M15512 - Name: Serotonin - Relevance: LOW - As Found: Unknown - ID: M29246 - Name: Serotonin 5-HT3 Receptor Antagonists - Relevance: LOW - As Found: Unknown - ID: M20504 - Name: Neurotransmitter Agents - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000017294 - Term: Ondansetron ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423794 Brief Title: BHV-7000 Open-Label Extension Bipolar Mania Study Official Title: A Phase 2, Multicenter, Open-Label Extension Study to Assess the Long-Term Safety and Tolerability of BHV-7000 in Treatment of Bipolar I Disorder #### Organization Study ID Info ID: BHV7000-202 #### Organization Class: INDUSTRY Full Name: Biohaven Pharmaceuticals, Inc. ### Status Module #### Completion Date Date: 2026-04 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-03 Type: ESTIMATED #### Start Date Date: 2024-06 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Biohaven Therapeutics Ltd. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True ### Description Module Brief Summary: The purpose of this study is to evaluate the long-term safety and tolerability of BHV-7000 in subjects with bipolar I disorder. ### Conditions Module Conditions: - Bipolar Disorder Keywords: - bipolar - mania - manic episode - manic state - bipolar disorder type 1 - manic depressive - manic bipolar - mixed features - mixed episode - mixed mania - bipolar episode - bipolar disorder ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 200 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Drug: BHV-7000 Label: BHV-7000 Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - BHV-7000 Description: BHV-7000 75 mg taken once daily Name: BHV-7000 Type: DRUG ### Outcomes Module #### Primary Outcomes Description: To assess the safety and tolerability of BHV-7000. This objective will be measured by assessing the number of unique subjects with grade 3 and 4 laboratory abnormalities. Measure: Number of Participants With Clinically Significant Laboratory Abnormalities Time Frame: Up to 52 weeks Description: To assess the safety and tolerability of BHV-7000. This objective will be measured by assessing the number of unique subjects with SAEs, AEs leading to discontinuation, AEs judged to be related to study medication that are observed during the Double-blind Treatment Phase (21 days). Measure: Number of Participants With Serious AEs (SAEs), AEs Leading to Study Drug Discontinuation, and AEs judged to be related to study medication Time Frame: Up to 52 weeks ### Eligibility Module Eligibility Criteria: Key Inclusion Criteria: 1. Subjects must have successfully completed the parent study, BHV7000-204. 2. WOCBP must have a negative urine pregnancy test at Baseline visit. 3. WOCBP must not be breastfeeding or lactating at Baseline visit or any point in the study. Key Exclusion Criteria: 1. Any medical condition, based on the judgement of the Investigator, that would confound the ability to adequately assess safety and efficacy outcome measures. 2. Subjects who, in the opinion of the Investigator, will not be able to adhere to the Schedule of Assessments and/or may have difficulties complying with the treatment regimen over an extended duration of a long-term, outpatient study. 3. Investigator deems subject at imminent risk of danger to others or themself. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Chief Medical Officer Phone: 203-404-0410 Role: CONTACT ## Derived Section ### Condition Browse Module - Ancestors - ID: D000068105 - Term: Bipolar and Related Disorders - ID: D000019964 - Term: Mood Disorders - ID: D000001523 - Term: Mental Disorders ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M4996 - Name: Bipolar Disorder - Relevance: HIGH - As Found: Bipolar Disorder - ID: M2598 - Name: Mania - Relevance: LOW - As Found: Unknown - ID: M226 - Name: Bipolar and Related Disorders - Relevance: LOW - As Found: Unknown - ID: M21835 - Name: Mood Disorders - Relevance: LOW - As Found: Unknown - ID: M4815 - Name: Mental Disorders - Relevance: LOW - As Found: Unknown - ID: M14473 - Name: Psychotic Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000001714 - Term: Bipolar Disorder ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423781 Brief Title: Long-term Safety Study of BHV-7000 in Participants With Major Depressive Disorder (MDD) Official Title: A Phase 2, Multicenter, Open-Label Extension Study to Assess the Long-Term Safety and Tolerability of BHV-7000 in Treatment of Major Depressive Disorder (MDD) #### Organization Study ID Info ID: BHV7000-203 #### Organization Class: INDUSTRY Full Name: Biohaven Pharmaceuticals, Inc. ### Status Module #### Completion Date Date: 2027-11 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-22 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2027-11 Type: ESTIMATED #### Start Date Date: 2024-07 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Biohaven Therapeutics Ltd. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True ### Description Module Brief Summary: The purpose of this study is to evaluate the long-term safety and tolerability of BHV-7000, in participants with Major Depressive Disorder (MDD). ### Conditions Module Conditions: - Major Depressive Disorder Keywords: - depression - major depression - antidepressant - major depressive disorder - MDD ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 480 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Drug: BHV-7000 Label: BHV-7000 Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - BHV-7000 Description: BHV-7000 75 mg taken once daily Name: BHV-7000 Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Safety and tolerability of BHV-7000 as assessed by frequency of unique subjects with SAEs; AEs leading to discontinuation; AEs judged to be related to study medication Measure: Number of Participants With Serious AEs (SAEs), AEs Leading to Study Drug Discontinuation, and AEs judged to be related to study medication Time Frame: Up to 52 weeks Description: To assess the safety and tolerability of BHV-7000. This objective will be measured by assessing the number of unique subjects with grade 3 and 4 laboratory abnormalities. Measure: Number of Participants With Clinically Significant Laboratory Abnormalities Time Frame: Up to 52 weeks ### Eligibility Module Eligibility Criteria: Key Inclusion Criteria: 1. Eligible participants must have successfully completed the Treatment/Randomization Phase of parent studies. 2. WOCBP must have a negative urine pregnancy test at Baseline Visit. 3. WOCBP must not be breastfeeding or lactating at Baseline Visit or at any point during the study. Key Exclusion Criteria: 1. Any medical condition, based on the judgement of the Investigator, that would confound the ability to adequately assess safety and efficacy outcome measures. 2. Participant non-compliance with study procedures, study drug or visit attendance in the parent study that the Investigator deems as clinically significant or unacceptable risk potential for this study. 3. Investigator deems participant at imminent risk of danger to others. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Chief Medical Officer Phone: 203-404-0410 Role: CONTACT ## Derived Section ### Condition Browse Module - Ancestors - ID: D000019964 - Term: Mood Disorders - ID: D000001523 - Term: Mental Disorders - ID: D000001526 - Term: Behavioral Symptoms ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M7058 - Name: Depression - Relevance: HIGH - As Found: Depressive Disorder - ID: M7061 - Name: Depressive Disorder - Relevance: HIGH - As Found: Depressive Disorder - ID: M7060 - Name: Depressive Disorder, Major - Relevance: HIGH - As Found: Major Depressive Disorder - ID: M21835 - Name: Mood Disorders - Relevance: LOW - As Found: Unknown - ID: M4815 - Name: Mental Disorders - Relevance: LOW - As Found: Unknown - ID: M14473 - Name: Psychotic Disorders - Relevance: LOW - As Found: Unknown - ID: M4818 - Name: Behavioral Symptoms - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003866 - Term: Depressive Disorder - ID: D000003863 - Term: Depression - ID: D000003865 - Term: Depressive Disorder, Major ### Intervention Browse Module - Browse Branches - Abbrev: PsychDr - Name: Psychotropic Drugs - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M4247 - Name: Antidepressive Agents - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423768 Acronym: FACE-UP Brief Title: fMRI in CardiaC arrEst With Uncertain Prognosis Official Title: The fMRI in CardiaC arrEst With Uncertain Prognosis (FACE-UP) Study #### Organization Study ID Info ID: 2024P000703 #### Organization Class: OTHER Full Name: Brigham and Women's Hospital ### Status Module #### Completion Date Date: 2027-12-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: ACTIVE_NOT_RECRUITING #### Primary Completion Date Date: 2027-06-01 Type: ESTIMATED #### Start Date Date: 2024-05-16 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: American Heart Association #### Lead Sponsor Class: OTHER Name: Brigham and Women's Hospital #### Responsible Party Investigator Affiliation: Brigham and Women's Hospital Investigator Full Name: Samuel Snider, MD Investigator Title: MD Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The goal of this observational study is to determine whether specific advanced MRI measures are associated with functional outcomes in patients who are comatose after cardiac arrest. The main question\[s\] it aims to answer are: Aim 1: Determine if stimulus-based functional MRI (fMRI)-measured activations are independently associated with favorable neurological outcomes after cardiac arrest Aim 2: Determine if resting state functional MRI (rs-fMRI)-measured functional network connectivity is independently associated with favorable neurological outcomes after cardiac arrest. Aim 3: Determine if diffusion tensor imaging (DTI)-measured white matter integrity is associated with favorable neurological outcomes after cardiac arrest. Participants will undergo advanced MRI sequences at time of clinical MRI, and will be followed for 6 months post-arrest. Detailed Description: Our goal here is to determine whether advanced functional MRI and DTI sequences add actionable prognostic information relative to standard clinical MRI in patients who remain comatose after cardiac arrest. We plan the following specific analyses: Aim 1: We will use logistic regression to measure the association between our primary outcome and fMRI BOLD response to (a) passive language stimuli, (b) motor imagery or (c) passive sensory stimuli, in a model with age, Glasgow Coma Scale (GCS) score at time of MRI, and presence of anoxic injury on clinical diffusion weighted MRI. Aim 2: We will use logistic regression to measure the association between our primary outcome and default mode network resting state functional connectivity, in a model with age, Glasgow Coma Scale (GCS) score at time of MRI, and presence of anoxic injury on clinical diffusion weighted MRI. Aim 3: We will use logistic regression to measure the association between our primary outcome and diffusion tensor imaging (DTI)-measured mean white matter fractional anisotropy, in a model with age, Glasgow Coma Scale (GCS) score at time of MRI, and presence of anoxic injury on clinical diffusion weighted MRI. ### Conditions Module Conditions: - Cardiac Arrest ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 50 Type: ESTIMATED Study Type: OBSERVATIONAL ### Outcomes Module #### Primary Outcomes Description: A standardized scale describing a patients overall level of independent function. Levels 1-2 reflect patients who are functionally independent in their iADLs. Measure: Cerebral Performance Category Score 1-2 Time Frame: 6 months #### Secondary Outcomes Description: Any patient who has recovered consciousness (follows verbal commands), regardless of their disability level at 2-weeks Measure: Cerebral Performance Category Score 1-3 Time Frame: 2 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * survive of an in or out of hospital cardiac arrest Exclusion Criteria: * Drug overdose * Opinion of medical team patient unlikely to survive more than 24 hours (severe concurrent medical illness, dilated and unreactive pupils, etc..) * Following verbal commands (MD or RN note) once TTM is complete and normothermia is achieved (Day 2 or 3; Day of admission is Hospital Day 0). If no TTM is administered, this can be assessed on Hospital Day 2. * Following verbal commands (study team assessment) at time of MRI * Family planning to WLST at time of enrollment * Non English speaker (okay if English not primary language, as long as they can understand it) * Permanent Contraindication to MRI (some kind of implanted metal) * Pregnant Healthy Volunteers: True Minimum Age: 18 Years Sampling Method: PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Participants who have survive a cardiac arrest but remain unresponsive after completion of targeted temperature management (TTM). We will enroll a separate sample of 15 healthy controls to provide a normative range for our advanced MRI imaging measures. ### Contacts Locations Module #### Locations Location 1: City: Boston Country: United States Facility: Brigham and Women's Hospital State: Massachusetts Zip: 02115 ### IPD Sharing Statement Module Description: Plan to post to openneuro.org IPD Sharing: YES ## Derived Section ### Condition Browse Module - Ancestors - ID: D000006331 - Term: Heart Diseases - ID: D000002318 - Term: Cardiovascular Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC14 - Name: Heart and Blood Diseases ### Condition Browse Module - Browse Leaves - ID: M21089 - Name: Facies - Relevance: LOW - As Found: Unknown - ID: M9411 - Name: Heart Arrest - Relevance: HIGH - As Found: Cardiac Arrest - ID: M9419 - Name: Heart Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000006323 - Term: Heart Arrest ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423755 Brief Title: Swimming Versus Standard Physiotherapy Care as Rehabilitation Modalities for Persistent Low Back Pain: Feasibility Study Official Title: Swimming Versus Standard Physiotherapy Care as Rehabilitation Modalities for Persistent Low Back Pain: A Feasibility Study #### Organization Study ID Info ID: 264307 #### Organization Class: OTHER Full Name: Canterbury Christ Church University ### Status Module #### Completion Date Date: 2022-10-01 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: COMPLETED #### Primary Completion Date Date: 2022-10-01 Type: ACTUAL #### Start Date Date: 2021-09-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER_GOV Name: East Kent Hospitals University NHS Foundation Trust #### Lead Sponsor Class: OTHER Name: Canterbury Christ Church University #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Study four: A small scale RCT will be conducted to pilot the swimming lessons developed in study three, to compare the lessons to standard physiotherapy care and to assess the feasibility of conducting a large RCT in the future. The results from this feasibility study will give the researcher some initial feedback on the swimming lessons and will inform and support the development of an RCT in the future; if the initial findings are positive. This will include whether an RCT can be carried out and evaluating recruitment and retention rates, willingness to be randomised, adverse events, outcomes, acceptability and cost analysis. Detailed Description: Low back pain is very common; globally it is the number one cause of disability. National guidelines recommend exercise for the management of back pain; swimming is frequently advised despite little supporting evidence. Swimming is considered to be low impact and might target conditions associated with back pain such as obesity, inactivity, and depression. Swimming lessons are not funded by the NHS, many adults cannot swim and there are no guidelines regarding what type of swimming program to recommend. This multi-phase mixed methods research project aims to develop a swimming class to be used as a form of rehabilitation for persistent low back pain. There are many barriers to exercise and this can affect uptake and adherence; Study 1 will be an online survey finding out what stops and what encourages people with back pain to go swimming. Some people already use swimming to manage back pain; in Study 2, individuals who use swimming to manage back pain will be interviewed to explore their experience including discussion about swimming stroke and adaptations. The swimming class will be developed in Study 3 using the data from Study 1 and 2 and by consulting physiotherapists, swimming teachers, and patients, through a series of surveys, known as the Delphi method. Study 4 will be a feasibility study; comparing the swimming class developed in Study 3 over 3 weeks to standard physiotherapy care. Data will be collected on the running of the study, outcomes including function and quality of life, with further follow up at on completion of the trial and 6 months. These studies will be carried out at East Kent Hospitals NHS Trust and the Hotel Burstin swimming pool; people with back pain for more than 3 months would be eligible to take part. ### Conditions Module Conditions: - Chronic Low-back Pain Keywords: - Rehabilitation - Swimming - Physiotherapy ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Non-randomised comparative trial design ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 32 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants allocated to the swimming programme will be invited to complete three short questionnaires to assess general health, back pain, and swimming ability and experience, see Appendix H, I and J. Both the swimming and physiotherapy groups will complete the three outcome measures, the Oswestry low back pain disability index (ODI), the pain self-efficacy questionnaire (PSEQ), and the EQ-5D-3L, before the intervention, after the last appointment and 6 months later. Data will be collected to report participant characteristics: including age, gender, and length of time with LBP. A follow up participant feedback questionnaire will be distributed to the participants in the swimming arm on completion of the programme and 6 months later. Intervention Names: - Other: Swimming programme Label: Swimming programme Type: EXPERIMENTAL #### Arm Group 2 Description: The participants in the physiotherapy arm will attend the physiotherapy department in the hospital. Treatment delivered by the physiotherapist could include exercise, advice, education, and manual therapy; they will be offered up to 6 sessions. Some appointments will be delivered in a cubicle and others in the physiotherapy gym. The time between appointments varied from person to person. Intervention Names: - Other: Standard Physiotherapy care Label: Standard Physiotherapy care Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Swimming programme Description: A session plan will be followed, which included aims, objectives, learning outcomes and suggested core aquatic skills and swimming activities under each section. The session will consist of a session brief, a warmup, core aquatic skills, swimming strokes (front crawl, backstroke, breaststroke, and hybrid strokes), a cool down and a session debrief; following the guidance developed in study three. Name: Swimming programme Type: OTHER #### Intervention 2 Arm Group Labels: - Standard Physiotherapy care Description: Treatment delivered by the physiotherapist could include exercise, advice, education, and manual therapy; they will be offered up to 6 sessions. Name: Standard Physiotherapy care Type: OTHER ### Outcomes Module #### Primary Outcomes Description: 10 questions scored on a Likert scale asking the participant how confident they are to do an activity despite the pain. Measure: Pain Self efficacy questionnaire Time Frame: Baseline, 3 weeks and 6 months #### Secondary Outcomes Description: This questionnaire is composed of 10 questions with 6 response statements to assess disability Measure: Oswestry low back pain disability index Time Frame: Baseline, 3 weeks and 6 months Description: Measure of health related quality of life Measure: EQ-5D-3L Time Frame: Baseline, 3 weeks and 6 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * The inclusion criteria for the study were that participants should have experienced CLBP for more than three months, be at least 18 years old and have a small amount of swimming experience. Exclusion Criteria: * Exclusion criteria for the study included the following: unable to read or speak English, allergy to chlorine, severe fear of the water, pregnancy, ear infection, already a competent regular swimmer, visual impairment not correctable with glasses, medical contraindication to aquatic exercise or precaution that cannot be resolved. The following back conditions were excluded; red flag conditions (cauda equina syndrome, cancer or tumour related back pain, spinal infection, spinal cord compression, back pain from visceral source), inflammatory back pain, fractures of the spine during the last 6 months, severe spinal stenosis, nerve root compromise causing neurological deficit or constant pain in the leg, back surgery in the last 6 months, and fitted with a spinal cord stimulator. Healthy Volunteers: True Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Canterbury Country: United Kingdom Facility: David Stephensen State: Kent Zip: CT1 3NG #### Overall Officials Official 1: Affiliation: Canterbury Christ Church University Name: Hayley Mills, PhD Role: STUDY_CHAIR ### IPD Sharing Statement Module Description: There is no plan but we are happy to share data with other researchers IPD Sharing: NO ### References Module #### References Citation: Oakes H, de Vivo M, Mills H, Stephensen D. Recommending swimming to people with low back pain: A scoping review. J Bodyw Mov Ther. 2023 Oct;36:274-281. doi: 10.1016/j.jbmt.2023.05.012. Epub 2023 Aug 25. PMID: 37949572 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M4714 - Name: Back Pain - Relevance: HIGH - As Found: Back Pain - ID: M19433 - Name: Low Back Pain - Relevance: HIGH - As Found: Low Back Pain - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000001416 - Term: Back Pain - ID: D000017116 - Term: Low Back Pain ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423742 Brief Title: Consecutive Dual-Session tDCS in Chronic Subjective Severe to Catastrophic Tinnitus With Normal Hearing Official Title: Consecutive Dual-Session tDCS in Chronic Subjective Severe to Catastrophic Tinnitus With Normal Hearing #### Organization Study ID Info ID: 2021-11-009 #### Organization Class: OTHER Full Name: Dongtan Sacred Heart Hospital ### Status Module #### Completion Date Date: 2022-09-30 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: COMPLETED #### Primary Completion Date Date: 2022-09-30 Type: ACTUAL #### Start Date Date: 2021-12-15 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Dongtan Sacred Heart Hospital #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: We aimed to analyze the effect of continuous dual session tDCS in patients with severe chronic subjective tinnitus without any evidence of hearing loss in terms of relief of tinnitus perception, distress, and loudness. Also, we investigated the difference in the maintenance duration of the tinnitus suppression effect of consecutive dual session tDCS compared to other groups followed up for 2 months. Detailed Description: The participants were randomly allocated with three different arms (control, single-session, and dual session) using block to balance the size of each group. Pure tone audiometry, speech audiometry, tinnitogram (pitch matching, loudness, minimal masking level and residual inhibition), auditory evoked potential, THI, visual analogue scale (VAS) of loudness, awareness and annoyance, and BDI were evaluated as a baseline tests. Participants who assigned to the control group underwent dual sham stimulation per day, twice a week for 1 month. Patients were received sham and true stimulation once alternately in the single session group and two true stimulation per day in the dual session group for the same period as the control group. All subjects who enrolled this study were given a conventional treatment such as tinnitus retraining therapy, sound therapy using sound generator, and medications like clonazepam, selective serotonin reuptake inhibitors for patients who wanted to take for relief of symptoms. ### Conditions Module Conditions: - Tinnitus, Subjective Keywords: - Transcranial direct current stimulation - Tinnitus ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: The participants were randomly allocated with three different arms (control, single-session, and dual session) using block to balance the size of each group. . Participants who assigned to the control group underwent dual sham stimulation per day, twice a week for 1 month. Patients were received sham and true stimulation once alternately in the single session group and two true stimulation per day in the dual session group for the same period as the control group. All subjects who enrolled this study were given a conventional treatment such as tinnitus retraining therapy, sound therapy using sound generator, and medications like clonazepam, selective serotonin reuptake inhibitors for patients who wanted to take for relief of symptoms. ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: TREATMENT #### Enrollment Info Count: 42 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The subjects in control group were received two consecutive sessions of sham stimulation twice a week for 4 weeks (8 sessions in total). Intervention Names: - Device: Transcranial direct current stimulation Label: control Type: SHAM_COMPARATOR #### Arm Group 2 Description: Patients enrolled to the single-session group received tDCS on one random session out of two consecutive sessions. Intervention Names: - Device: Transcranial direct current stimulation Label: single-session Type: ACTIVE_COMPARATOR #### Arm Group 3 Description: In the dual-session group, the patients underwent two consecutives tDCS. Intervention Names: - Device: Transcranial direct current stimulation Label: dual-session Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - control - dual-session - single-session Description: The device used for tDCS in this study was DC-Stimulator Plus (NeuroConn GmbH, Ilmenau, Germany). The localization of stimulation area (DLPFC) was determined according to the 10/20 EEG system. Non-conducting, elastic head strap was placed around the head to prevent displacement during stimulation. The recording electrode covered with 5 x 7 cm sized traditional rectangular sponge was soaked with 6-7 mL of 0.9% NaCl saline solution per side and placed on the F3 (anode, left frontal) and F4 (cathode, right frontal) EEG location. Subjects were given 2 mA stimulation intensity for 20 min per session including fade-in and fade-out times for 20 seconds each. Interval between each session was 20 min. Sham procedure has been adopted a Fade In of current, Short Stimulation, Fade Out (FISSFO) protocol that consist of initial ramp up for 20 seconds, 2 mA stimulation for 40 seconds, and 20 seconds for ramp down. To check to impendence, brief current of 110 µA over 15ms every 550ms was delivered. Name: Transcranial direct current stimulation Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: To achieve a more quantitative evaluation of tinnitus reduction, we assessed the Visual Analog Scale (VAS). Measure: Visual analogue scale (VAS) related to tinnitus Time Frame: All participants were checked the VAS immediately after the last stimulation of every week for 4 weeks and 8th week (4 weeks after the end of treatment). Description: The subjective improvement of tinnitus was evaluated using THI. Measure: Tinnitus Handicap Inventory (THI) Time Frame: THI was assessed at the 4th and 8th week visits. Description: To assess the association between tinnitus relief and depression, we evaluated the Beck Depression Inventory (BDI). Measure: Beck depression inventory (BDI) Time Frame: THI was assessed at the 4th and 8th week visits. ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Individuals who have experienced subjective tinnitus for over 3 months. * Individuals with normal hearing, defined as an average pure tone threshold of less than 25 dB between 0.5-4 kHz, and the presence of the V wave at 30 dBnHL with a difference in V wave latency of less than 0.2 ms in both ears during the ABR test. * Individuals with severe tinnitus, as indicated by a Tinnitus Handicap Inventory (THI) score of 58 or higher, and who have been assessed for symptoms of anxiety and depressive mood using the Beck Depression Inventory (BDI) questionnaire. Exclusion Criteria: * Those requiring treatment for neurological disorders such as epilepsy, migraine, or intracranial masses. * Pregnant individuals on the day of providing consent and those with metal-based electric implantable prosthetics. * Individuals with objective or somatic tinnitus, auditory hallucinations, unwillingness to provide written consent, or unwillingness to continue the trial, and those who have participated in previous trials involving tDCS for tinnitus. Healthy Volunteers: True Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Hwaseong Si Country: Korea, Republic of Facility: Dongtan Sacred Heart Hospital State: Gyeonggi-Do Zip: 445-170 #### Overall Officials Official 1: Affiliation: University of Michigan Name: Sung Kyun Kim Role: STUDY_DIRECTOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000006311 - Term: Hearing Disorders - ID: D000004427 - Term: Ear Diseases - ID: D000010038 - Term: Otorhinolaryngologic Diseases - ID: D000012678 - Term: Sensation Disorders - ID: D000009461 - Term: Neurologic Manifestations - ID: D000009422 - Term: Nervous System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC09 - Name: Ear, Nose, and Throat Diseases - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M16769 - Name: Tinnitus - Relevance: HIGH - As Found: Tinnitus - ID: M9400 - Name: Hearing Disorders - Relevance: LOW - As Found: Unknown - ID: M7601 - Name: Ear Diseases - Relevance: LOW - As Found: Unknown - ID: M12961 - Name: Otorhinolaryngologic Diseases - Relevance: LOW - As Found: Unknown - ID: M15490 - Name: Sensation Disorders - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000014012 - Term: Tinnitus ### Intervention Browse Module - Browse Branches - Abbrev: PhSol - Name: Pharmaceutical Solutions - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M21860 - Name: Pharmaceutical Solutions - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423729 Brief Title: Effect of Nicorandil in Type 2 Diabetic Obese Patients Official Title: Clinical Study Evaluating the Effect of Nicorandil in Type 2 Diabetic Obese Patients Treated With Sulfonylurea #### Organization Study ID Info ID: Nicorandil in DM #### Organization Class: OTHER Full Name: Tanta University ### Status Module #### Completion Date Date: 2025-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-12 Type: ESTIMATED #### Start Date Date: 2024-06-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Tanta University #### Responsible Party Investigator Affiliation: Tanta University Investigator Full Name: Merna Mohamed Seddik Ali Investigator Title: Merna Mohamed Seddik Ali , Master degree in Clinical Pharmacy, Tanta University Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: 1. Evaluating the effect of nicorandil on glycemic control of diabetic obese patients treated with sulfonylureas. 2. Investigating the effect of nicorandil on body weight of diabetic obese patients treated with sulfonylureas. ### Conditions Module Conditions: - Diabetes Mellitus, Type 2 Keywords: - Type 2 DM, Nicorandil, Obesity ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 46 Type: ESTIMATED Phases: - PHASE2 - PHASE3 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: 23 patients who will receive 2nd generation sulfonylureas only, for three months. Label: Control Arm Type: NO_INTERVENTION #### Arm Group 2 Description: 23 patients who will receive a combination of 2nd generation sulfonylureas and nicorandil 10 mg twice daily,for three months. Intervention Names: - Drug: Nicorandil 10 MG Label: Nicorandil Arm Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Nicorandil Arm Description: Patients will receive oral Nicorandil 10 MG twice daily in addition to 2nd generation sulfonylureas , for 3 months. Name: Nicorandil 10 MG Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Change in HbA1c (From baseline to 12 weeks) Measure: Change in HbA1c level Time Frame: The participants will be assessed before initiation of the study (baseline), and at the end of the study after 3 months. Description: Change in body weight (From baseline to 12 weeks). Measure: Change in body weight. Time Frame: The participants will be assessed before initiation of the study (baseline), and at the end of the study after 3 months. Description: Change in Body mass index (BMI) (From baseline to 12 weeks). Measure: Change in Body mass index (BMI) Time Frame: The participants will be assessed before initiation of the study (baseline), and at the end of the study after 3 months. Description: Change in Visceral adiposity index (VAI) (From baseline to 12 weeks). Measure: Change in Visceral adiposity index (VAI). Time Frame: The participants will be assessed before initiation of the study (baseline), and at the end of the study after 3 months. #### Secondary Outcomes Description: Assessment of Adiponenctin, Interleukin-6 (IL-6) and Nitric oxide levels by ELISA Kits according to manufacturer's instructions. Measure: Change in Adiponenctin, Interleukin-6 (IL-6) and Nitric oxide (NO) serum levels. Time Frame: The participants will be assessed before initiation of the study (baseline), and at the end of the study after 3 months. ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Diabetes duration ranged from 1 to 10 years. * Body mass index (BMI) \>30 Kg/m2. * The selected patients are treated with sulfonylureas alone. * The age of selected patient ranged from 18 and 60 years. Exclusion Criteria: * Pregnant and lactating females. * Patients with hypersensitivity to nicorandil. * Uncontrolled hypertension and its antihypertensive medications * Severe renal or hepatic disease. Maximum Age: 60 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Merna Mohamed Seddik Ali Phone: +201026064628 Role: CONTACT #### Locations Location 1: City: Tanta Contacts: *Contact 1:* - Email: [email protected] - Name: Merna Mohamed Seddik Ali, Master degree - Phone: +201026064628 - Role: CONTACT *Contact 2:* - Name: Merna Mohamed Seddik Ali - Role: PRINCIPAL_INVESTIGATOR Country: Egypt Facility: Faculty of Pharmacy, Tanta University Status: RECRUITING Zip: 31511 ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000003920 - Term: Diabetes Mellitus - ID: D000044882 - Term: Glucose Metabolism Disorders - ID: D000008659 - Term: Metabolic Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC19 - Name: Gland and Hormone Related Diseases ### Condition Browse Module - Browse Leaves - ID: M12701 - Name: Obesity - Relevance: LOW - As Found: Unknown - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M7119 - Name: Diabetes Mellitus, Type 2 - Relevance: HIGH - As Found: Diabetes Mellitus, Type 2 - ID: M11639 - Name: Metabolic Diseases - Relevance: LOW - As Found: Unknown - ID: M25403 - Name: Glucose Metabolism Disorders - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003924 - Term: Diabetes Mellitus, Type 2 ### Intervention Browse Module - Ancestors - ID: D000000889 - Term: Anti-Arrhythmia Agents - ID: D000000959 - Term: Antihypertensive Agents - ID: D000014665 - Term: Vasodilator Agents - ID: D000014803 - Term: Vitamin B Complex - ID: D000014815 - Term: Vitamins - ID: D000018977 - Term: Micronutrients - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: Micro - Name: Micronutrients - Abbrev: AnArAg - Name: Anti-Arrhythmia Agents - Abbrev: AnAg - Name: Antihypertensive Agents - Abbrev: VaDiAg - Name: Vasodilator Agents - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Hemat - Name: Hematinics - Abbrev: Vi - Name: Vitamins ### Intervention Browse Module - Browse Leaves - ID: M21946 - Name: Nicorandil - Relevance: HIGH - As Found: Enabling - ID: M4213 - Name: Anti-Arrhythmia Agents - Relevance: LOW - As Found: Unknown - ID: M4277 - Name: Antihypertensive Agents - Relevance: LOW - As Found: Unknown - ID: M17412 - Name: Vasodilator Agents - Relevance: LOW - As Found: Unknown - ID: M8618 - Name: Folic Acid - Relevance: LOW - As Found: Unknown - ID: M17558 - Name: Vitamins - Relevance: LOW - As Found: Unknown - ID: M17546 - Name: Vitamin B Complex - Relevance: LOW - As Found: Unknown - ID: M21009 - Name: Micronutrients - Relevance: LOW - As Found: Unknown - ID: M16885 - Name: Trace Elements - Relevance: LOW - As Found: Unknown - ID: T446 - Name: Folic Acid - Relevance: LOW - As Found: Unknown - ID: T448 - Name: Folate - Relevance: LOW - As Found: Unknown - ID: T475 - Name: Vitamin B9 - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000020108 - Term: Nicorandil ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423716 Acronym: RELIFE Brief Title: Effect of peRiopErative duLoxetIne Administration on Opioid Consumption Following Total kneE Arthroplasty (RELIFE) Official Title: Effect of Perioperative Duloxetine Administration on Opioid Consumption Following Total Knee Arthroplasty #### Organization Study ID Info ID: SBK 6156 #### Organization Class: OTHER Full Name: Sunnybrook Health Sciences Centre ### Status Module #### Completion Date Date: 2026-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-07-01 Type: ESTIMATED #### Start Date Date: 2024-05-15 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Sunnybrook Health Sciences Centre #### Responsible Party Investigator Affiliation: Sunnybrook Health Sciences Centre Investigator Full Name: Dr. Colin McCartney Investigator Title: Anesthesiologist, Pain Physician Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Knee replacement surgery for osteoarthritis is a commonly performed procedure in Canada with 75,000 of these surgeries performed each year. Success rate for knee replacement surgery is high but more than 20% of patients are still dissatisfied mainly due to reports of ongoing pain. Pain control following knee surgery is important in order to allow patients to engage in recovery and rehabilitation. The current standard of pain management after surgery centers around the use of opioids which is a concerning practice as highlighted by the opioid epidemic. Duloxetine is an antidepressant that has pain relieving properties and it has been studied in patients undergoing knee replacement surgery. Studies to date have not been designed optimally to demonstrate the full effects of opioid dose reduction and the use of duloxetine as a medication following knee replacement surgery. This research study seeks to start duloxetine before surgery, at the recommended therapeutic dose, and for the duration of the early rehabilitation period. If the study is successful, this low-cost medication can improve satisfaction rates and change the standard way the pain management is typically carried out for patients undergoing the knee replacement surgery. Detailed Description: The use of duloxetine around the time of total knee arthroplasty has emerged as a promising intervention to help with pain management after surgery and in particular as an opioid sparing agent. Duloxetine is an antidepressant with serotonin and norepinephrine reuptake inhibition effects that also independently exerts an analgesic effect. Duloxetine is Health Canada approved for several indications including pain arising from osteoarthritis of the knee. Pain inhibition action of duloxetine is believed to be a result of potentiation of descending inhibitory pain pathways within the central nervous system. Existing studies examining duloxetine use at the time of surgery has demonstrated statistically significant but less clinically meaningful impacts on opioid sparing and pain reduction. The deficiencies in study design of existing studies have either underdosed duloxetine (30mg instead of the recommended 60mg) and/or utilized non-standard duration of therapy (started too late, continued for only 2 weeks). Our study seeks to definitively address whether duloxetine administered 2 weeks preoperatively at 60mg once daily, in addition to standard analgesic practice, will decrease opioid consumption at 1 week postoperatively. Prospective, randomized, blinded (investigators, clinicians, participant, data collectors/analysts) trial. Primary Outcome •Cumulative opioid consumption at 1 week post-operatively. Secondary Outcomes * Nausea/vomiting * Discharged according to plan (ie. same day went home same day, or day 1 went home day 1) and if not, reason * Pain at rest and with activity (NRS-11) at 1, 6, and 12 weeks and 4.5 months * Additional analgesic use (anti-neuropathic medications, family physician or orthopaedic surgeon opioid prescription) * Physical function (BPI, Oxford Knee Scale, range of motion * Emotional function (GAD-7, PHQ-9 at 6 weeks and 12 weeks) * Number of rehabilitation sessions attended (in-person or virtual) * Patient satisfaction (PGIC) at 1, 6, and 12 weeks after medication initiation * Presence of neuropathic pain (S-LANSS) at 6 and 12 weeks * Presence of chronic post-surgical pain at 12 weeks (based on NRS \> 0) * Adverse events relating to study medication (dizziness, drowsiness, nausea, vomiting, insomnia) * Intervention adherence Interventional medication supply: Duloxetine 60mg OD for 2 weeks preoperatively then 60mg OD for 6 weeks post-surgery. Standard of care: On the day of surgery, participants will be premedicated with acetaminophen (1000mg) and celecoxib (400mg). Per standard of care, all participants will receive an ultrasound guided adductor canal catheter (bolus ropivacaine 0.5% 10ml). This will be followed by a spinal anesthetic with mepivacaine 2% 3ml and 10mcg of fentanyl. Intraoperative sedation will consist of a propofol infusion titrated to SAS (Sedation Agitation Scale) of 3-4. All TKAs will be performed using a standard medial parapatellar approach and the same cemented total knee system. Tourniquet will be applied and used as part of the case. Periarticular local infiltration will be used per standard practice using ropivacaine 0.2% with 1:200 000 epinephrine up to 50ml. Post-surgery: Participants will be evaluated on POD-0, POD-1 and POD-2 while in hospital or at home through phone call and at 1, 6, and 12 weeks. Participant satisfaction will be assessed using the Patients' Global Impression of Change (PGIC) Scale at 1, 6, and 12 weeks post-surgery. Pain scores and opioid consumption will be recorded daily for 1 week post-operatively. Patients will record their pain and opioid consumption on a weekly basis until week 12 post-operatively. Physical function, emotional function, and presence of neuropathic pain will be collected at 6 and 12 weeks. Active and passive range of motion will be assessed by orthopedic surgeon using goniometer at 6 (+/-1 week) and 12 (+/-1 week) weeks and 4.5 month (+/-2 weeks) postoperatively. Group 1: Intervention Duloxetine 60mg OD for 2 weeks preoperatively then 60mg OD for 6 weeks post-surgery. Group 2: Control Placebo OD for 2 weeks preoperatively then OD for 6 weeks post-surgery. Both Groups: On the day of surgery, standard post-anesthetic care unit (PACU) orderset will be employed and the postoperative analgesic regimen will follow standard of care including: acetaminophen 1g QID, celecoxib 200mg BID, and hydromorphone 1-3mg PO q2h PRN. * Nurse administered IV hydromorphone push (0.3mg) followed by IV PCA hydromorphone if pain is not controlled * ACB catheter ropivacaine 0.15% at 5cc/hr, stopped at 6:00am on POD-1 Participants will be discharged on POD-0, POD-1 or POD-2 with acetaminophen 1000mg TID, celecoxib 100mg BID, and hydromorphone (2-4mg PO q4h PRN). Patients for same-day discharge (POD-0) will have ACB catheter bolus of 10cc of 0.5% ropivacaine prior to removal. ### Conditions Module Conditions: - Knee Osteoarthritis Keywords: - total knee arthroplasty - duloxetine - postoperative pain ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Group 1: Intervention Duloxetine 60mg OD for 2 weeks preoperatively then 60mg OD for 6 weeks post-surgery. Group 2: Control Placebo OD for 2 weeks preoperatively then OD for 6 weeks post-surgery. ##### Masking Info Masking: QUADRUPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 150 Type: ESTIMATED Phases: - PHASE4 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Duloxetine 60mg OD for 2 weeks preoperatively then 60mg OD for 6 weeks post-surgery. Intervention Names: - Drug: Duloxetine Label: Intervention Type: EXPERIMENTAL #### Arm Group 2 Description: Placebo OD for 2 weeks preoperatively then OD for 6 weeks post-surgery. Intervention Names: - Drug: Placebo Label: Control Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Intervention Description: 60mg duloxetine given 2 weeks prior to total knee arthroplasty and continued for 6 weeks after surgery. Name: Duloxetine Type: DRUG #### Intervention 2 Arm Group Labels: - Control Description: Placebo given 2 weeks prior to total knee arthroplasty and continued for 6 weeks after surgery. Name: Placebo Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Cumulative opioid consumption at 1 week post-operatively Measure: Opioid consumption Time Frame: Cumulative opioid consumption at 1 week post-operatively #### Secondary Outcomes Description: Presence of nausea or vomiting Measure: Nausea/vomiting Time Frame: 8 weeks (i.e., duration of study) Description: Maximum pain score on 0-10 Likert Scale (NRS) Measure: Pain at rest and with activity Time Frame: 10-14 days preoperative; 1,6,12 weeks and 4.5 months Description: Anti-neuropathic medications Measure: Additional analgesic use Time Frame: 8 weeks (i.e., duration of study) Description: Family physician or orthopaedic surgeon opioid prescription Measure: Additional analgesic use: opioid prescription Time Frame: 8 weeks (i.e., duration of study) Description: Brief Pain Inventory Measure: Physical function measured by BPI Time Frame: Preoperative, 6, 12 weeks and 4.5 months Description: Oxford Knee Scale Measure: Physical function measured by Oxford Knee Scale Time Frame: Preoperative, 6, 12 weeks and 4.5 months Measure: Range of motion: Physical function Time Frame: Preoperative, 6, 12 weeks and 4.5 months Description: GAD-7 Measure: Emotional function measured by GAD-7 Time Frame: Preoperative, 6, 12 weeks and 4.5 months Description: PHQ-9 Measure: Emotional function measured by PHQ-9 Time Frame: Preoperative, 6, 12 weeks and 4.5 months Description: Patient global impression of change (PGIC) Measure: Patient satisfaction Time Frame: 1, 6, and 12 weeks after surgery Description: Presence of neuropathic pain (S-LANSS) Measure: Neuropathic pain Time Frame: 6 and 12 weeks post-surgery Description: Presence of chronic post-surgical pain (based on NRS \> 0) Measure: Chronic post-surgical pain Time Frame: 12 weeks post-surgery Description: Adverse events relating to study medication (dizziness, drowsiness, nausea, vomiting, insomnia) Measure: Adverse events Time Frame: in hospital at POD1-3, 1 week post-discharge ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Age \>=50 2. Presence of knee osteoarthritis 3. Planned for elective unilateral total knee arthroplasty 4. ASA I - III Exclusion Criteria: 1. Lack of patient consent; unlikely to comply with follow-up 2. Presence of contraindications to study drug use: * Known hypersensitivity to the drug or components of the product * Known liver disease - history of cirrhosis, non-alcoholic steatohepatitis * Uncontrolled narrow - angle glaucoma * Severe renal impairment (CrCl\<30mL/min) * Concurrent use of thioridazine * Concurrent use of potent CYP1A2 inhibitors (e.g. fluvoxamine) and some quinolone antibiotics (e.g. ciprofloxacin or enoxacin) * Concurrent use of antidepressants (e.g. MAOI, SSRI, SNRI, TCA, St. John's Wort, buspirone) * Concurrent use of triptan or lithium 3. Chronic and high dose opioid use (\>30mg oral morphine equivalent per day) 4. Substance use disorder (cannabis and related products, alcohol use disorder, opioid used disorder, illicit drugs) 5. Uncontrolled hypertension (systolic BP \> 180mmHg) 6. Untreated psychiatric illness (e.g. depression, suicidal ideation, bipolar disorder) 7. Involved in worker's compensation case/law suit (verbally declared by patient) Minimum Age: 50 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Howard Meng, MD Phone: 416-480-4864 Role: CONTACT Contact 2: Email: [email protected] Name: Stephen Choi Phone: 416-480 -4864 Role: CONTACT #### Locations Location 1: City: Toronto Contacts: *Contact 1:* - Email: [email protected] - Name: Lilia Kaustov, PhD - Phone: 416-480-6100 - Phone Ext: 89607 - Role: CONTACT *Contact 2:* - Name: Stephen Choi, MD - Role: SUB_INVESTIGATOR *Contact 3:* - Name: Sebastian Tomescu, MD - Role: SUB_INVESTIGATOR *Contact 4:* - Name: Howard Meng, MD - Role: SUB_INVESTIGATOR Country: Canada Facility: Sunnybrook Health Sciences Centre State: Ontario Zip: M4N 3M5 ### IPD Sharing Statement Module Access Criteria: Contact study investigators Description: De-identified data will be available upon request Info Types: - STUDY_PROTOCOL - SAP - ICF IPD Sharing: YES Time Frame: Upon publication, no limit on time ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001168 - Term: Arthritis - ID: D000007592 - Term: Joint Diseases - ID: D000009140 - Term: Musculoskeletal Diseases - ID: D000012216 - Term: Rheumatic Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC05 - Name: Musculoskeletal Diseases - Abbrev: BC17 - Name: Skin and Connective Tissue Diseases ### Condition Browse Module - Browse Leaves - ID: M13069 - Name: Pain, Postoperative - Relevance: LOW - As Found: Unknown - ID: M12926 - Name: Osteoarthritis - Relevance: HIGH - As Found: Osteoarthritis - ID: M22168 - Name: Osteoarthritis, Knee - Relevance: HIGH - As Found: Knee Osteoarthritis - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M4476 - Name: Arthritis - Relevance: LOW - As Found: Unknown - ID: M10621 - Name: Joint Diseases - Relevance: LOW - As Found: Unknown - ID: M12097 - Name: Musculoskeletal Diseases - Relevance: LOW - As Found: Unknown - ID: M15045 - Name: Rheumatic Diseases - Relevance: LOW - As Found: Unknown - ID: M6323 - Name: Collagen Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000010003 - Term: Osteoarthritis - ID: D000020370 - Term: Osteoarthritis, Knee ### Intervention Browse Module - Ancestors - ID: D000068760 - Term: Serotonin and Noradrenaline Reuptake Inhibitors - ID: D000014179 - Term: Neurotransmitter Uptake Inhibitors - ID: D000049990 - Term: Membrane Transport Modulators - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000018377 - Term: Neurotransmitter Agents - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000000700 - Term: Analgesics - ID: D000018689 - Term: Sensory System Agents - ID: D000018373 - Term: Peripheral Nervous System Agents - ID: D000000928 - Term: Antidepressive Agents - ID: D000011619 - Term: Psychotropic Drugs - ID: D000015259 - Term: Dopamine Agents ### Intervention Browse Module - Browse Branches - Abbrev: Analg - Name: Analgesics - Abbrev: PsychDr - Name: Psychotropic Drugs - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: VaCoAg - Name: Vasoconstrictor Agents - Abbrev: CaAg - Name: Cardiotonic Agents ### Intervention Browse Module - Browse Leaves - ID: M299 - Name: Duloxetine Hydrochloride - Relevance: HIGH - As Found: American - ID: M4033 - Name: Analgesics, Opioid - Relevance: LOW - As Found: Unknown - ID: M12575 - Name: Norepinephrine - Relevance: LOW - As Found: Unknown - ID: M15512 - Name: Serotonin - Relevance: LOW - As Found: Unknown - ID: M305 - Name: Serotonin and Noradrenaline Reuptake Inhibitors - Relevance: LOW - As Found: Unknown - ID: M20504 - Name: Neurotransmitter Agents - Relevance: LOW - As Found: Unknown - ID: M4032 - Name: Analgesics - Relevance: LOW - As Found: Unknown - ID: M4247 - Name: Antidepressive Agents - Relevance: LOW - As Found: Unknown - ID: M14474 - Name: Psychotropic Drugs - Relevance: LOW - As Found: Unknown - ID: M7473 - Name: Dopamine - Relevance: LOW - As Found: Unknown - ID: M17962 - Name: Dopamine Agents - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000068736 - Term: Duloxetine Hydrochloride ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423703 Acronym: ALLEVIATE2 Brief Title: A Study of Cebranopadol for the Treatment of Acute Pain After Bunionectomy Official Title: A Multicenter, Randomized, Double-Blind, Placebo- and Active-Controlled Study to Evaluate the Efficacy and Safety of Cebranopadol for the Treatment of Moderate to Severe Acute Pain After Primary Unilateral Bunionectomy #### Organization Study ID Info ID: TRN-228-302 #### Organization Class: INDUSTRY Full Name: Tris Pharma, Inc. ### Status Module #### Completion Date Date: 2024-12 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-11 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Tris Pharma, Inc. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Oversight Has DMC: False ### Description Module Brief Summary: The purpose of this study is to evaluate the efficacy and safety of Cebranopadol for acute pain after a bunionectomy. Detailed Description: This study is a Phase 3, multicenter, randomized, double-blind, placebo- and active-controlled parallel-group study to evaluate the efficacy and safety of cebranopadol in the treatment of postoperative pain following primary unilateral bunionectomy with first metatarsal osteotomy. The study will be conducted in 3 phases: Screening, Treatment, and Follow-up. ### Conditions Module Conditions: - Acute Pain Keywords: - Bunionectomy ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: QUADRUPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 240 Type: ESTIMATED Phases: - PHASE3 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: once daily for 3 days Intervention Names: - Drug: Cebranopadol - Drug: Placebo Label: Cebranopadol Type: EXPERIMENTAL #### Arm Group 2 Description: four times per day for 3 days Intervention Names: - Drug: Oxycodone IR Label: Oxycodone IR Type: ACTIVE_COMPARATOR #### Arm Group 3 Description: three times per day 3 days (with cebranopadol); four times per day for 3 days (placebo arm) Intervention Names: - Drug: Placebo Label: Placebo Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Cebranopadol Description: once daily for 3 days Name: Cebranopadol Type: DRUG #### Intervention 2 Arm Group Labels: - Oxycodone IR Description: four times per day for 3 days Name: Oxycodone IR Type: DRUG #### Intervention 3 Arm Group Labels: - Cebranopadol - Placebo Description: three times per day 3 days (with cebranopadol), four times per day for 3 days (placebo arm) Name: Placebo Type: DRUG ### Outcomes Module #### Other Outcomes Measure: Incidence of Respiratory Safety Events Time Frame: 0-72 hours #### Primary Outcomes Measure: Pain NRS area under the curve: cebranopadol vs. placebo Time Frame: 2-48 hours #### Secondary Outcomes Measure: Proportion of subjects who require opioid rescue medication Time Frame: 0-72 hours Measure: Global Assessment of Satisfaction Time Frame: 0-72 hours Measure: Total oxycodone rescue consumption Time Frame: 0-72 hours ### Eligibility Module Eligibility Criteria: Key Inclusion Criteria Before Surgery: * Scheduled to undergo primary unilateral bunionectomy with first metatarsal osteotomy and internal fixation with no collateral procedures, using anesthesiologic and surgical procedures planned * Must be able to adhere to the visit schedule, complete all study assessments and protocol requirements, including self-reported questionnaires. Key Exclusion Criteria Before Surgery: * Any clinically significant disease, medical condition, or laboratory finding that in the investigator's opinion may interfere with the study procedures or data integrity, or compromise the safety of the subject. * Secondary (i.e., unrelated to bunion) current painful condition that could confound the interpretation of efficacy, safety, or tolerability data in the study, in the opinion of the investigator. * Subjects who require any analgesic for secondary (i.e., unrelated to bunion) painful condition that might impact the subject's ability to properly assess their postoperative pain, or that may require treatment during the Treatment Phase. * History of allergy or hypersensitivity to any opioid analgesics, anesthetics, ibuprofen, or other NSAIDs. Immediate Postoperative Exclusion Criteria: * Surgical, postsurgical, or anesthetic complication that could confound the interpretation of efficacy, safety, or tolerability data in the study. * Deviation from the surgical, postsurgical, or anesthetic protocol that could confound the interpretation of efficacy, safety, or tolerability data in the study. * Evidence of hemodynamic instability or respiratory insufficiency. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Antonio Pardo, MD Phone: 732-823-4755 Role: CONTACT #### Locations Location 1: City: Sheffield Country: United States Facility: ALLEVIATE 2 Site 001108 State: Alabama Zip: 35660 Location 2: City: Little Rock Country: United States Facility: ALLEVIATE 2 Site 001106 State: Arkansas Zip: 72211 Location 3: City: Tampa Country: United States Facility: ALLEVIATE 2 Site 001103 State: Florida Zip: 33613 Location 4: City: Atlanta Country: United States Facility: ALLEVIATE 2 Site 001102 State: Georgia Zip: 30331 Location 5: City: Overland Park Country: United States Facility: ALLEVIATE 2 Site 001107 State: Kansas Zip: 66212 Location 6: City: Pasadena Country: United States Facility: ALLEVIATE 2 Site 001105 State: Maryland Zip: 21122 Location 7: City: McAllen Country: United States Facility: ALLEVIATE 2 Site 001104 State: Texas Zip: 78501 Location 8: City: Salt Lake City Country: United States Facility: ALLEVIATE 2 Site 001101 State: Utah Zip: 84107 #### Overall Officials Official 1: Affiliation: CenExel JBR Name: Todd M Bertoch, MD Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M29525 - Name: Acute Pain - Relevance: HIGH - As Found: Acute Pain - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000059787 - Term: Acute Pain ### Intervention Browse Module - Ancestors - ID: D000000701 - Term: Analgesics, Opioid - ID: D000009294 - Term: Narcotics - ID: D000002492 - Term: Central Nervous System Depressants - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000000700 - Term: Analgesics - ID: D000018689 - Term: Sensory System Agents - ID: D000018373 - Term: Peripheral Nervous System Agents ### Intervention Browse Module - Browse Branches - Abbrev: Analg - Name: Analgesics - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M13020 - Name: Oxycodone - Relevance: HIGH - As Found: Valve - ID: M4032 - Name: Analgesics - Relevance: LOW - As Found: Unknown - ID: M4033 - Name: Analgesics, Opioid - Relevance: LOW - As Found: Unknown - ID: M12245 - Name: Narcotics - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000010098 - Term: Oxycodone ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423690 Brief Title: First in Human Study for the Assessment of Safety and Initial Performance of the EAS1 System Official Title: Snipe Medical First In Human Study #### Organization Study ID Info ID: PRC015 #### Organization Class: INDUSTRY Full Name: Snipe Medical ### Status Module #### Completion Date Date: 2025-02-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-01-15 Type: ESTIMATED #### Start Date Date: 2024-07-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Snipe Medical #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: A Prospective, open label, multi center, single arm, First in Human study to assess the safety and initial performance of EAS1 system for Irreversible Electroporation (IRE) ablation of lung cancer in subjects eligible for tumor resection ### Conditions Module Conditions: - Lung Cancer ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 15 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Ablation of the lung tumor via Irreversible Electroporation (IRE) method, followed by resection of the tumor up to 14 days after the ablation Intervention Names: - Device: EAS1 System Label: Treatment Arm - Ablation with EAS1 System Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Treatment Arm - Ablation with EAS1 System Description: tumor ablation system in IRE method Name: EAS1 System Type: DEVICE ### Outcomes Module #### Other Outcomes Description: Investigator satisfaction, as determined by completing an internal ease-of-use questionnaire following each procedure. The questionnaire consists of 10 questions, each ranging from 1 (not at all) to 5 (very much). Range of total score is 10-50, where the higher the total score, the more satisfied the investigator is from device use Measure: Investigator's Impression of the Treatment (Investigator's Satisfaction) Time Frame: 30 days Description: Immunological response, as determined by change from baseline to 30 day FU in immunological blood markers. Measure: Assessment of Immunological Response Following Ablation Time Frame: 30 days #### Primary Outcomes Description: Accumulative rate of device related Serious Adverse Events (SAEs) during the ablation and up to 48 hours post ablation Measure: Safety of the EAS1 System in Lung Tumor Ablation During Procedure Time Frame: 48 hours post procedure #### Secondary Outcomes Description: Rate of device related SAEs during the follow up period Measure: Safety of the EAS1 System in Lung Tumor Ablation Throughout Follow Up Time Frame: 30 days Description: - Technical success, defined as the investigator's ability to access the target tumor and successfully perform the irreversible electroporation, as confirmed by histology analysis Measure: Investigator's Ability to Approach and Ablate the Tumor (Technical Success) Time Frame: 30 days ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Adult male and female subjects (age ≥18 years at the date of informed consent signature) * Subject is capable and willing to provide an informed consent * Subjects with a known diagnosis of lung cancer at cT1a-T1c, cN0 stages * At least one pulmonary tumor (primary or metastasis) ≤ 30 mm in maximal diameter, as confirmed by the latest standard of care imaging (CT/MRI), performed preferably up to 30 days prior to screening * Subjects who are scheduled or deemed eligible by a thoracic surgeon for lung tumor resection * Subject is able and willing to comply with the study procedures and visits * There is ≥ 5mm of nodule-free lung parenchyma between target nodule and pleura or fissure, as confirmed by the latest standard of care imaging (CT/MRI), performed preferably up to 30 days prior to screening * ECOG 0-1 * Stable doses of concomitant medications for at least four (4) weeks prior to enrollment Exclusion Criteria: * An inability to provide informed consent * Subjects with contraindication for tumor resection * Subjects with life expectancy \<12 months * Target nodule is abutting main stem bronchus, main pulmonary vasculature, esophagus and/or trachea * Subjects with Forced Expiratory Volume (FEV1) \<50% * Total Lung Capacity (TLC)\< 80% of expected for age * Diffusing Capacity (DCO) \< 60% of expected * Oxygen saturation in free air of \<88%, or requiring more than 2 l/min oxygen to achieve saturation of 92% * PCO2 of ≥ 45mm/Hg * Subjects in exacerbations group E (high risk; ≥2 exacerbations per year or ≥1 requiring hospitalization and any level of symptoms) * Severe emphysema, Bullous Emphysema or chronic obstructive pulmonary disease (COPD) (GOLD III/IV) * Active and/or prolonged lung or bronchi infection, required an antibiotic treatment up to 21 days prior to screening and for more than 10 days of treatment * Known history or current evidence of a significant bronchiectasis * Evidence of lung Bullae the occupies more than one third of the lung intended for ablation * Previous surgery in the lung intended for ablation; thoracic major surgery at the side intended for ablation * Anticoagulation treatment that cannot be discontinued prior to the ablation, or a bleeding diathesis or platelets \<100 )K/µl) * Pregnant or breastfeeding female subjects or female subjects who plan pregnancy during participation in the study * Highly hypoxemic patients, according to investigator's discretion * Subjects with implanted metal or electronic thoracic devices objects (such as pacemaker) that cannot be removed prior to procedure * Subjects with contraindication for bronchoscopy * Participation in any other interventional clinical trial with medication, medical device and/or supplements within 30 days prior to informed consent signature * Any subject who, at the discretion of the investigator, may be jeopardized by study participation Maximum Age: 80 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Emily Ben Shlomo Phone: 972523212687 Role: CONTACT #### Locations Location 1: City: Kfar Saba Contacts: *Contact 1:* - Email: "[email protected]" <[email protected]> - Name: Emily Ben Shlomo - Role: CONTACT *Contact 2:* - Name: Eyal Romem, Dr - Role: PRINCIPAL_INVESTIGATOR Country: Israel Facility: Meir Medical Center Location 2: City: Salamanca Contacts: *Contact 1:* - Email: [email protected] - Name: Marcelo Jimenez, Dr - Phone: +34923291100 - Phone Ext: 55383 - Role: CONTACT *Contact 2:* - Name: Marcelo Jimenez, Dr. - Role: PRINCIPAL_INVESTIGATOR Country: Spain Facility: University Hospital Complex of Salamanca Location 3: City: London Contacts: *Contact 1:* - Email: [email protected] - Name: Anand Tana - Phone: +44 207 352 8121 - Role: CONTACT *Contact 2:* - Name: Pallav Shah, Dr - Role: PRINCIPAL_INVESTIGATOR Country: United Kingdom Facility: Royal Brompton Hospital #### Overall Officials Official 1: Affiliation: Principal investigator at Meir Medical Center Name: Eyal Romem, Dr Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M11172 - Name: Lung Neoplasms - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423677 Brief Title: Analgesic Efficacy of Serratus Posterior Superior Intercostal Plane (SPSIP) Block in Shoulder Arthroscopies Official Title: Evaluation of the Analgesic Efficacy of Serratus Posterior Superior Intercostal Plane (SPSIP) Block in Shoulder Arthroscopies: A Randomized Controlled Prospective Multicenter Study #### Organization Study ID Info ID: Serratus Posterior Superior #### Organization Class: OTHER Full Name: Kanuni Sultan Suleyman Training and Research Hospital ### Status Module #### Completion Date Date: 2024-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-29 Type: ACTUAL Last Update Submit Date: 2024-05-27 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-12-01 Type: ESTIMATED #### Start Date Date: 2024-06-25 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Kanuni Sultan Suleyman Training and Research Hospital #### Responsible Party Investigator Affiliation: Kanuni Sultan Suleyman Training and Research Hospital Investigator Full Name: Engin Ihsan Turan Investigator Title: Specialist Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Patients in the block group will be placed in a lateral position with the operated shoulder on top before awakening from surgery. After ensuring aseptic conditions (the block site will be wiped three times with 10% povidone-iodine), the linear ultrasound probe will be covered in a sterile manner. While performing the block, the Hitachi brand linear ultrasound probe will be placed parallel to the scapular spine on the surgical side and will be slid medially. After imaging the 2nd and 3rd ribs on the medial side of the scapular spine, the block needle will be advanced under ultrasound guidance onto the 3rd rib. After contacting the rib with the needle, it will be retracted by 1mm, and the block site will be confirmed by injecting sterile 0.9% NaCl. Subsequently, patients will be administered 30ml of 0.25% bupivacaine in a controlled manner. Before awakening, both the block group and the non-block group will be administered 1g of paracetamol and 1mg/kg of tramadol intravenously. In the postoperative period, these patients will be provided with multimodal analgesia, including intravenous patient-controlled analgesia (PCA) with 4mg/ml Tramadol HCl in 100ml NaCl. There will be no basal infusion, with bolus doses of 20mg and a lockout period of 20 minutes, and a total dose limitation of 200mg over 4 hours. Patients will be visited at 0, 1, 6, 12, and 24 hours, and they will be asked to draw their visual analog scale (VAS) score on a paper scale. The amount of opioid used in the PCA and the need for rescue analgesia (Arveles 50mg intravenously) will be assessed. Patients will routinely receive 4x1g paracetamol in the postoperative period. ### Conditions Module Conditions: - Pain, Postoperative - Shoulder Pain - Block ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 52 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: serratus posterior superior intercostal plane block will be administered to these group. after the extubation intravenous patient controlled analgesia (PCA) will also be administered to patients. Intervention Names: - Procedure: Serratus Posterior Superior Intercostal Plane Block - Device: patient controlled analgesia Label: serratus posterior superior intercostal plane block + intravenous patient controlled analgesia Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: After the extubation, only intravenous patient controlled analgesia (PCA) will be administered to patients. Intervention Names: - Device: patient controlled analgesia Label: intravenous patient controlled analgesia Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - serratus posterior superior intercostal plane block + intravenous patient controlled analgesia Description: The Serratus Posterior Superior Intercostal Plane Block will be performed under ultrasound guidance. During the block, a linear ultrasound probe will be placed parallel to the spine of the scapula on the surgical side and then slid medially. The block needle will be advanced under ultrasound guidance over the 3rd rib. After the needle touches the rib, it will be withdrawn by 1mm, and the block site will be confirmed by injecting sterile 0.9% NaCl. Subsequently, patients will be administered 50mg of bupivacaine and 100mg of lidocaine in a controlled manner. Name: Serratus Posterior Superior Intercostal Plane Block Type: PROCEDURE #### Intervention 2 Arm Group Labels: - intravenous patient controlled analgesia - serratus posterior superior intercostal plane block + intravenous patient controlled analgesia Description: intravenous patient-controlled analgesia (PCA) with 4mg/ml Tramadol HCl in 100ml NaCl. There will be no basal infusion, with bolus doses of 20mg and a lockout period of 20 minutes, and a total dose limitation of 200mg over 4 hours Name: patient controlled analgesia Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: Patients will be visited at 0, 1, 6, 12, and 24 hours, and they will be asked to draw their visual analog scale (VAS) score on a paper scale.0 means no pain, 10 means the most intense pain. 4 or more Visual analog scale scores means patients need rescue analgesia. Measure: visual analog scale score Time Frame: 0, 1, 6, 12, and 24 hours Description: Patients will be visited at 0, 1, 6, 12, and 24 hours and opioid consumption in the patient controlled analgesia device will be noted.0 means no pain, 10 means the most intense pain. 4 or more Visual analog scale scores means patients need rescue analgesia. Measure: opioid consumption Time Frame: 0, 1, 6, 12, and 24 hours ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Obtaining consent from the patient and their relative * ASA score of I-II * No bleeding diathesis * No history of anticoagulant use * No history of neuropathic diseases such as Diabetes Mellitus * Patients aged 18-65 years undergoing shoulder arthroscopy surgery Exclusion Criteria: * Lack of consent from the patient or their relative * Patients with an ASA score of III or above * Patients with a history of bleeding diathesis * Conditions where regional anesthesia is contraindicated * Patients with a history of neuropathic diseases * Patients under 18 years or over 65 years of age * Patients with a history of allergies to the aforementioned medications * Patients with an infection at the site where the block will be administered Maximum Age: 65 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Engin ihsan Turan Phone: +9005382431114 Role: CONTACT #### Locations Location 1: City: Istanbul Country: Turkey Facility: Health Science University İstanbul Kanuni Sultan Süleyman Education and Training Hospital Zip: 34303 #### Overall Officials Official 1: Affiliation: Health Science University İstanbul Kanuni Sultan Süleyman Education and Training Hospital Name: Engin ihsan Turan Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011183 - Term: Postoperative Complications - ID: D000010335 - Term: Pathologic Processes - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations - ID: D000018771 - Term: Arthralgia - ID: D000007592 - Term: Joint Diseases - ID: D000009140 - Term: Musculoskeletal Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC05 - Name: Musculoskeletal Diseases - Abbrev: BC10 - Name: Nervous System Diseases ### Condition Browse Module - Browse Leaves - ID: M13069 - Name: Pain, Postoperative - Relevance: HIGH - As Found: Pain, Postoperative - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M21907 - Name: Shoulder Pain - Relevance: HIGH - As Found: Shoulder Pain - ID: M14065 - Name: Postoperative Complications - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: M20833 - Name: Arthralgia - Relevance: LOW - As Found: Unknown - ID: M10621 - Name: Joint Diseases - Relevance: LOW - As Found: Unknown - ID: M12097 - Name: Musculoskeletal Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000020069 - Term: Shoulder Pain - ID: D000010149 - Term: Pain, Postoperative ### Intervention Browse Module - Browse Branches - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: AnArAg - Name: Anti-Arrhythmia Agents - Abbrev: ChanBlk - Name: Channel Blockers - Abbrev: Analg - Name: Analgesics ### Intervention Browse Module - Browse Leaves - ID: M5315 - Name: Bupivacaine - Relevance: LOW - As Found: Unknown - ID: M11014 - Name: Lidocaine - Relevance: LOW - As Found: Unknown - ID: M4032 - Name: Analgesics - Relevance: LOW - As Found: Unknown - ID: M16901 - Name: Tramadol - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423664 Acronym: INTACT Brief Title: Improving Neurodevelopmental ouTcomes After Prenatal Cannabinoid in uTero Exposure Official Title: Pilot Feasibility Trial of Improving Neurodevelopmental ouTcomes After Prenatal Cannabinoid in uTero Exposure (INTACT) #### Organization Study ID Info ID: 276534 #### Organization Class: NETWORK Full Name: IDeA States Pediatric Clinical Trials Network ### Status Module #### Completion Date Date: 2024-09-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-09-01 Type: ESTIMATED #### Start Date Date: 2024-06-17 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: University of New Mexico Class: OTHER Name: University of Vermont Class: UNKNOWN Name: Avera Research Institute Class: NIH Name: National Institutes of Health (NIH) #### Lead Sponsor Class: NETWORK Name: IDeA States Pediatric Clinical Trials Network #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: The INTACT trial is a multisite pilot feasibility study aimed at testing the effectiveness of the INTACT Intervention program in improving neurodevelopmental outcomes in infants prenatally exposed to cannabinoids. The trial will enroll 20 birthing parent/infant dyads across three sites and will evaluate feasibility endpoints rather than clinical outcomes. The study duration is 22 months, including study start-up, enrollment and intervention, and data analysis and manuscript preparation. Detailed Description: The INTACT trial is designed to address the need for interventions to improve neurodevelopmental outcomes in infants exposed to cannabinoids in utero. It is a multi-site pilot study conducted across three Institutional Development Award (IDeA) States Pediatric Clinical Trials Network (ISPCTN) sites. The trial aims to evaluate the feasibility of the INTACT Intervention program, which focuses on training birthing parents in contingent responding to promote early language, cognitive, and social development in their infants. The study intervention consists of 12 monthly INTACT intervention coaching sessions, each comprising online module completion followed by personalized coaching sessions with interventionists certified to deliver the Play and Learn Strategies (PALS) methodology, which forms the basis for the INTACT intervention. The online modules focus on strengthening effective parenting practices, while the coaching sessions guide birthing parents in contingent responding techniques, such as reading infant signals and responding with warm and sensitive behaviors. There are three objectives for this study, examining 1) Participant Recruitment, 2) Participant Completion, and 3) Participant Adherence. Objective 1 examines if birthing parents can be recruited and enrolled in the study. The endpoint of this objective is the percentage of potential participants approached for the study that are consented and determined to be eligible for study participation. Objective 2 evaluates participant completion, as measured by the percent of birthing parent/infant dyads that complete the coaching session scheduled when the child is 12 months of age. Objective 3 evaluates the number of individual INTACT intervention coaching sessions completed. The study duration is planned for 22 months, including 1-4 months for study development and start-up, 3 months for enrollment, 12 months for the intervention, and 3 months for data organization, clean-up, and manuscript preparation. The INTACT trial will not assess clinical outcomes but will inform the design of a future larger-scale clinical trial to evaluate the effectiveness of the INTACT Intervention program in improving neurodevelopmental outcomes in infants prenatally exposed to cannabinoids. ### Conditions Module Conditions: - Developmental Delay Keywords: - Infants exposed to cannabinoids in-utero and their birthing parent. ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP Intervention Model Description: A single-arm pilot study to assess feasibility of study procedures. ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 20 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: A novel program to train birthing parents in contingent responding with the goal of improving neurodevelopmental outcomes in infants prenatally exposed to cannabinoids. 1 personalized coaching session per month for 12 months. Intervention Names: - Behavioral: Play and Learn Strategies (PALS) Program Label: Personalized coaching sessions Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Personalized coaching sessions Description: Monthly modules and personalized coaching sessions designed to strengthen maternal responsiveness and sensitivity which, in turn, improves infant social-emotional behavior and development outcomes. Name: Play and Learn Strategies (PALS) Program Other Names: - ePALS Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: Whether a potential participant approached for study participation will eventually be consented and determined to be eligible for study participation. Measure: Participant Recruitment Time Frame: 3 months Description: Whether a birthing parent/infant dyad will complete the final coaching session when the child is 12 months of age. Measure: Participant Completion Time Frame: 12 months following enrollment Description: Whether a participant will complete the sufficient number of INTACT intervention coaching sessions, defined as completion of at least 8 out of 12 coaching sessions. Measure: Participant Adherence Time Frame: 12 months following enrollment ### Eligibility Module Eligibility Criteria: Inclusion Criteria: Birthing Parent * Age of majority, as defined by the state of residency * Cannabinoid use during pregnancy confirmed with self-report * Have the ability to speak, read, and understand English * Birthing parent who delivered at one of the hospitals where study team members have clinical privileges to access medical records * Has parental custody of the infant * Singleton pregnancy with live birth * Has an electronic device capable of watching videos and able to stream/download videos for viewing and permitting video conferencing * Has study access to the internet Infant * Term infants at birth (\>37 weeks' gestation) * Biological child of the birthing parent Exclusion Criteria: Birthing Parent * Other illicit drug use, excluding cannabinoids, during pregnancy (such as heroin or cocaine) per self-reported or toxicology results * Opiate use (prescribed or unprescribed) per self-report or toxicology results during this pregnancy * Prolonged hospitalization following delivery longer than 7 days Infant * Has major birth defect(s) including physical anomalies including limb malformations/absence of limbs or chromosomal abnormalities * Diagnosed with neonatal encephalopathy, metabolic disorder, stroke, intracranial hemorrhage, or meningitis during birth hospitalization * Received any major surgical intervention during the birth hospitalization or required a prolonged birth hospitalization (prolonged hospitalization being any hospitalization longer than 7 days) Healthy Volunteers: True Maximum Age: 7 Days Sex: ALL Standard Ages: - CHILD ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Jessica Snowden, MD Phone: (501) 686-5647 Role: CONTACT Contact 2: Email: [email protected] Name: Matthew Henry, MSc Phone: (501) 686-5647 Role: CONTACT #### Locations Location 1: City: Albuquerque Contacts: *Contact 1:* - Email: [email protected] - Name: Jessie Maxwell, MD - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Sandra Beauman, MSN - Role: CONTACT Country: United States Facility: University of New Mexico Health Sciences Center State: New Mexico Zip: 87131 Location 2: City: Sioux Falls Contacts: *Contact 1:* - Email: [email protected] - Name: Maria Barber, DO - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Meggie McCoy, BS - Phone: (605) 504-3154 - Role: CONTACT *Contact 3:* - Name: Maria Barber, DO - Role: PRINCIPAL_INVESTIGATOR Country: United States Facility: Avera Research Institute State: South Dakota Zip: 57108 Location 3: City: Burlington Contacts: *Contact 1:* - Email: [email protected] - Name: Leigh-Anne Cioffredi, MD - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Laurie Chassereau, RN - Role: CONTACT Country: United States Facility: University of Vermont Medical Center State: Vermont Zip: 05401 #### Overall Officials Official 1: Affiliation: University of New Mexico Name: Jessie Maxwell, MD Role: PRINCIPAL_INVESTIGATOR Official 2: Affiliation: University of Vermont Name: Leigh-Anne Cioffredi, MD Role: PRINCIPAL_INVESTIGATOR Official 3: Affiliation: Avera Research Institute Name: Maria Barber, DO Role: PRINCIPAL_INVESTIGATOR Official 4: Affiliation: University of Arkansas Name: Song Ounpraseuth, PhD Role: STUDY_DIRECTOR ### IPD Sharing Statement Module Access Criteria: to be announced Description: We will conduct this trial in accordance with the following publication and data sharing policies and regulations: NIH Public Access Policy. It requires scientists to submit final peer-reviewed journal manuscripts that arise from NIH funds to the digital archive PubMed Central upon acceptance for publication. ECHO ISPCTN Publications and Presentations Policy. It ensures accurate, responsible, and efficient communication of findings from ECHO ISPCTN clinical trials. NIH Data Sharing Policy and the policy on the Dissemination of NIH-Funded Clinical Trial Information and the Clinical Trials Registration and Resulting Information Submission Rule. Other researchers may request data from this trial by contacting Song Ounpraseugh, PhD, at the ISPCTN Data Coordinating and Operations Center (DCOC). Info Types: - SAP - ICF IPD Sharing: YES Time Frame: Per data sharing polices of NIH and the ISPCTN ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423651 Acronym: CR+MCTp Brief Title: Benefits of Combining MCT With CR in the Recovery of Patients With Psychotic Spectrum Disorders Official Title: Benefits of Combining Metacognitive Training (MCT) With Cognitive Remediation (CR) in the Recovery of Patients With Psychotic Spectrum Disorders (CR+MCTp) #### Organization Study ID Info ID: PID2020-118907RA-I00 #### Organization Class: OTHER Full Name: Universitat Autonoma de Barcelona ### Status Module #### Completion Date Date: 2025-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-12-31 Type: ESTIMATED #### Start Date Date: 2022-09-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Parc Sanitari Sant Joan de Déu Class: OTHER Name: Consorci Sanitari de Terrassa Class: OTHER Name: Hospital de Mataró Class: OTHER Name: Centre d'Higiene Mental Les Corts Class: UNKNOWN Name: Fundació Els 3 Turons Class: OTHER Name: Hospital San Carlos, Madrid Class: OTHER_GOV Name: Andaluz Health Service Class: OTHER Name: Institut d'Assistència Sanitària Class: UNKNOWN Name: Ministerio de Ciencia, Innovación y Universidades Class: OTHER Name: Hospital Son Espases Class: OTHER Name: Parc Taulí Hospital Universitari Class: OTHER Name: Servicio Cántabro de Salud #### Lead Sponsor Class: OTHER Name: Universitat Autonoma de Barcelona #### Responsible Party Investigator Affiliation: Universitat Autonoma de Barcelona Investigator Full Name: Ana Barajas Velez Investigator Title: Associate Professor Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: The goal of this clinical trial is to compare the efficacy of combined REHACOP + MCT alone in persons with nonaffective psychotic disorder in terms of recovery. The main questions it aims to answer are: * Does combined REHACOP + MCT therapy increase the clinical recovery in persons with nonaffective psychotic disorder (compared to MCT alone)? * What is the impact of combined REHACOP + MCT therapy compared to MCT therapy alone on personal/psychological recovery, cognitive biases, and social cognition, taking gender differences into account? * What is the durability of the effects of combined REHACOP + MCT therapy compared to MCT therapy alone on clinical recovery, personal recovery, cognitive biases, and social cognition in the long term? Researchers will compare REHACOP+MCT therapy to MCT alone to see if there are differences in personal/psychological recovery. Participants will: * Participate in Metacognitive Training or in combined REHACOP + Metacognitive training therapy. * Do 8 weekly sessions of 45-60 minutes (MCT group). * Do 12 weekly sessions of 45-60 minutes (RECHACOP+MCT group). * Visit the clinic for checkups and tests. * Answer self-administered tests. Detailed Description: This project is aimed at responding to one of the Challenges of the Spanish Strategy for Science, Technology and Innovation, specifically Challenge 1: Health, demographic change and well-being. One of the work areas that are located within this challenge is the Clinical and Translational Research based on the evidence of scientific and technological knowledge.The present proposal is clearly within the framework of clinical-translational investigation, since most of the entities participating attend persons with psychotic disorders, thereby ensuring the translation of investigation to the clinical setting. In addition, this project includes investigators with wide experience in psychological interventions in the target population and with previous experience in investigation in this area. Lastly, it is of note that the benefits of this investigation are not only of a scientific nature but also involve clinical investigation with a direct repercussion on improvement in the health care of people with psychotic disorders, enabling the design of new strategies of psychological interventions. Besides, the present proposal is aimed at responding to the challenges of our society, contributing to covering the needs of persons with psychotic disorder as well as developing the most effective therapeutic strategies to improve aspects related to clinical and personal recovery. Specifically, this project will allow making changes that will improve the quality of health care to the target population incorporating the combinated use of scientifically proven therapeutic strategies to health care services. In short, this project aims to promote innovation in the provision of mental health services, being the starting point in analyzing the efficacy of combined psychological therapies versus monotherapies address to improve of metacognitive processes. - General and specific objectives. General objective: Compare the efficacy of combined REHACOP + MCT therapy vs. MCT alone in persons with nonaffective psychotic disorder in terms of recovery. Specific objectives: * Evaluate the effects of combined REHACOP + MCT therapy vs. MCT alone on clinical recovery (clinical remission and functional recovery, the latter understood in terms of cognitive, occupational and social functioning). * Evaluate the effects of combined REHACOP + MCT therapy vs. MCT alone on personal/psychological recovery. * Evaluate the effects of combined REHACOP + MCT therapy vs. MCT alone on cognitive biases and social cognition. * Evaluate the effects of combined REHACOP + MCT therapy vs. MCT alone according to gender. * Evaluate the effects of combined REHACOP + MCT therapy vs. MCT alone according to self-esteem, quality of life and stigma. * Evaluate the maintenance of the effects of combined REHACOP + MCT therapy vs. MCT alone on clinical recovery, personal recovery, cognitive biases and social cognition in the long term. * Methodology Design: This will be a randomised clinical trial in which one group will receive combined REHACOP + MCT therapy and another group will receive therapy with MCT alone. The metacognitive treatment will have the same characteristics in the two treatment conditions. Randomisation of the patients for receiving one of the two treatments will be carried out using a random number list based on the order of access to their reference centre. The evaluator will be blinded to the treatment group to which the patient assessed belongs. Study subjects: The sample will be made up of people with non-affective psychotic disorder who are attended in any of the centres participating in the study which belong to the following entities:Consorci Sanitari de Terrassa; Hospital de Mataró; Instituto de Investigación Biomédica de Gerona (IdIBG); Parc Sanitari Sant Joan de Déu; Asociación Centro de Higiene Mental Les Corts; Hospital Sierrallana-Tres Mares; and UGC Salud Mental de Jaén. Sample size: Considering that the investigators have no preliminary data on our principal objective in relation to clinical and personal recovery, the score obtained in the global assessment of functioning (GAF) at follow-up will be taken as a measure of outcome, since it is implicated in both clinical and functional recovery. The investigators used the data published in the article by Ochoa et al. (2017) in order to calculate the required sample size for this study. In this article, a difference of means of 5.73 points (SD=11.51) is obtained in the GAF scale from baseline and the follow-up at 6 months after the intervention. With these data, the necessary sample size has been estimated with an alpha of 0.05 and a power of 0.8. Taking into account 20% of possible losses to follow-up, the sample size has been calculated as 160 cases, 80 in each experimental arm (REHACOP + MCT vs. MCT). In this way, taking into account that the intervention groups will be carried out in the health care centers of 7 different entities each will have to recruit 24 patients, 12 for each experimental condition. Data collection: the professional who makes the referral of the patients to the study will be responsible for reviewing fulfillment of the inclusion and exclusion criteria. Patients fulfilling the inclusion criteria will receive an explanation of the study and if they accept to participate, they must provide signed informed consent. The evaluation will be carried out at 3 time points: T0 (basal assessment, prior to initiation of treatment). All the previously described scales will be administered; T1 (post-treatment evaluation), all the scales will be administered and, in addition, the satisfaction perceived with the interventions received will be evaluated; T2 (follow-up evaluation ) at 6 months after completing the intervention all the scales will again be administered. In addition, the number of relapses and hospitalizations during the time interval will be registered. Assessment of the PANSS and GAF should take into account the temporal criterium mentioned in the section of 'Outcomes'. A contingency plan will be considered in the event that difficulties are detected in carrying out any of the phases of the study due to external causes, such as the continuity of the COVID-19 pandemic. This plan will consist of the implementation of interventions and evaluations making use of new technologies. All the centers already have the adequate infrastructure to carry out the project under these conditions. Data analysis: Firstly, the two groups will be compared with the aim of verifying that there are no significant differences at baseline to confirm that they are comparable after randomization. Comparisons of means for independent samples will be carried out using the Student's t-test for continuous variables and the Chi-square test for categorical variables. The variables of the principal analysis will be the difference between the scores of the two groups (REHACOP+MCT and MCT) in the scores of the scales assessing clinical and personal/psychological recovery. The secondary results will be the differences in other assessments of social functioning, cognitive biases, and social cognition on comparing the two experimental conditions. Changes in the scores of these scales will be analyzed using regression methods for repeated measures, with the post-treatment score of the scales as the dependent variable and the basal score and the REHACOP+MCT group as the co-variables. Temporal stability of the results at 6 months will be assessed using the follow-up score as the dependent variable and evaluating how this affects the basal score, post treatment and the experimental condition. The statistical analyses will be performed according to intention to treat (ITT) without imputing the lost values. Gender, antipsychotic medication, and disease evolution time will be considered as control variables. Limitations: One of the limitations of this clinical trial might be the loss to follow-up. To compensate for these losses the sample size will be increased by 20%. It is expected that the losses to follow-up will be similar in the two groups. Otherwise, this variable will be considered as an indicator of the acceptability of treatment. - Ethical considerations: All the people who participate in the trial will sign the informed consent that takes into account the Declaration of Helsinki and the Organic Law 03/2018 of December 5. In the cases of minors informed consent will be signed by the legal guardians The project will be evaluated by each of the Ethics Committees of the participating centers. Participants will be informed that the data obtained will only be used for purposes related to the investigation and data confidentiality will be guaranteed according to the provisions of Organic Law 03/2018, of December 5 and Regulation (EU) 2016/679 of the European Parliament and of the Council, of April 27, 2016 and data protection (RGPD). The data management plan generated by the project, all information will be stored and managed in a secure and confidential manner, in accordance with the provisions of Organic Law 03/2018. In order to scrupulously respect the current legislation, the following measures will be taken: 1. Personal data will be pseudonymized. The identifying data are separated from the variables studied in the study. Therefore, a technical and functional separation will be made between the research team and those who perform the pseudonymization and retain the information that allows the reidentification of the participant. Pseudonymized data will only be accessible to the research team when: i) there is an express commitment to confidentiality and no re-identification activity, and ii) specific security measures are taken to prevent re-identification and access to unauthorized personal. 2. The person receiving the informed consent and custody will be different from the person who will process the data, or if this is not possible, the entire research team will sign an express commitment of confidentiality not to carry out re-identification activities. The signed informed consents will be kept under lock and key and out of the reach of the research team in a generic sense. ### Conditions Module Conditions: - Schizophrenia - Schizophreniform Disorders - Delusional Disorder - Brief Psychotic Disorder - Schizoaffective Disorder - Schizophrenia Spectrum and Other Psychotic Disorders Keywords: - Metacognitive Training - MCT - Cognitive Remediation - Psychotic disorder - Psychosis - Cognitive functions - Cognitive biases - Neurocognitive improvement ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: This will be a randomized clinical trial in which one group will receive combined REHACOP + MCT therapy and another group will receive therapy with MCT alone. The metacognitive treatment will have the same characteristics in the two treatment conditions. Randomisation of the patients for receiving one of the two treatments will be carried out using a random number list based on the order of access to their reference centre. The evaluator will be blinded to the treatment group to which the patient assessed belongs. ##### Masking Info Masking: TRIPLE Who Masked: - PARTICIPANT - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 160 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The participants will receive a combined therapy: Metacognitive Training (MCT) with Cognitive Remediation (CR). Intervention Names: - Behavioral: Cognitive Remediation (REHACOP) - Behavioral: Metacognitive Training (MCT) Label: REHACOP+MCT therapy Type: EXPERIMENTAL #### Arm Group 2 Description: The participants will receive Metacognitive Training (MCT) Intervention Names: - Behavioral: Metacognitive Training (MCT) Label: MCT alone Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - REHACOP+MCT therapy Description: REHACOP is a structured neuropsychological rehabilitation program that covers most of the cognitive deficits present in psychotic disorder: attention, learning and memory, executive functions, language, social cognition, daily life activities, social skills and psychoeducation. The modules of language, social cognition and psychoeducation will not be used in the present clinical trial. Each module includes a hierarchy of exercises based on the cognitive subarea to be worked on and the grade of difficulty demanded for the performance of each task.The format of the sessions will be the same as MCT, that is, groups of 6-10 patients who will receive weekly sessions of 45-60 minutes in length. In this case, the duration of the intervention will be 12 sessions. Name: Cognitive Remediation (REHACOP) Type: BEHAVIORAL #### Intervention 2 Arm Group Labels: - MCT alone - REHACOP+MCT therapy Description: The MCT consists in 8 weekly sessions of 45-60 minutes in length. Each group of patients should be made up of 6-10 patients. The material of the training program is available online at: http://www.uke.de/mkt. The material contains 16 powerpoint presentations (2 per each module), one manual and 6 pamphlets of tasks to do at home. The modules are as follows: Module 1: Attribution; Module 2: Jumping to conclusions (1st part); Module 3: Changing beliefs; Module 4: To emphatise (1st part); Module 5: Memory; Module 6: To emphatise (2nd part); Module 7: Jumping to conclusions (2nd part); and Module 8: Self-esteem and mood. Name: Metacognitive Training (MCT) Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: Includes: a) CLINICAL REMISSION: based on the criteria of the Remission in Schizophrenia Working Group (RSWA) of Andreasen et al. (2005), which includes one criterium of severity measured with 7 items of the PANSS scale and one temporal criterium that requires the maintenance of the criterium of severity during 6 months or more; and b) FUNCTIONAL RECOVERY: based on the criteria defined by the German Research Network on Schizophrenia (GRNS group) (Schennach-Wolff et al., 2009), which includes one criterium of severity based on the GAF scale and one temporal criterium of maintaining the criterium of severity during 6 months or more. Measure: CLINICAL RECOVERY Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: To be measured with the STORI test. Measure: FUNCTIONAL RECOVERY Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. #### Secondary Outcomes Description: A sociodemographic and clinical questionnaire created by the investigators of this study will be given with the aim of collecting the following data: age, gender, education, civil status, coexistence, current professional situation, total number of psychotic episodes, age at the first episode, substance use, type of treatments received (past and present), duration of untreated psychosis (DUP), relapses, number of hospitalisations, diagnosis according to the DSM-5, referral centre, family history, grade of satisfaction with care received, among others. Measure: Assesment instruments Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: The facial emotion recognition test will be used (Baron-Cohen et al., 1997; Huerta-Ramos et al., 2017) constituted by 20 photographs expressing 10 basic and 10 complex emotions. Measure: Social Cognition. Recognition of emotion Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Includes different stories for evaluating the interpretation of social situations. Measure: Social Cognition. Hinting Task (Corcoran et al., 1995; Gil et al., 2012) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: The IPSAQ has 32 items which describe 16 positive and 16 negative social situations. For each situation the person must decide whether the cause is internal, personal or situational. Measure: Social Cognition. Internal, Personal and Situational Attributions Questionnaire (IPSAQ) (Kinderman & Bentall, 1996; Diez-Alegría, 2006) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Jumping to conclusions (JTC) will be evaluated with the ball task. This is a task of probabilities in which the persons have to make a decision as to which box a ball belongs. The task will be used with a probability of 85%-15%, 60%-40% and with emotional tasks. JTC will be considered as making a decision after the extraction of one or two balls (Dudley et al., 2016). Measure: Ball task (Dudley et al.,1997). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: This questionnaire evaluates themost frequent cognitive biases in psychotic disorders. intentionality, catastrophism, dichotomic thinking, JTC and reasoning based on emotions. Measure: Cognitive Bias Questionnaire (CBQ) (Peters et al., 2013; Gutiérrez-Zotes, in press). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: This is a self applied questionnaire including 15 items which collect information on the capacity to correct erroneous judgements in two subscales: self-reflection and self-certainty. Measure: Beck Cognitive Insight Scale (BCIS) (Beck et al., 2004; Guitiérrez-Zotes et al., 2012). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: This scale was designed with the aim of evaluating areas of social functioning that are crucial for persons with schizophrenia to remain in the community. Measure: Social Functioning Scale (SFS) (Birchwood et al., 1990; Torres and Olivares, 2000). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: A battery of neuropsychological tests will be carried out to evaluate the domain of general cognitive functioning (Weschler Intelligence Scale \[WAIS\] (Weschler, 1999), to estimate the IQ using 4 subtests (vocabulary, similarities, block design and matrix reasoning), and specific domains of cognitive functioning. Measure: Cognitive functioning. Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: This scale measures the general functioning of the patient on a scale from 0 to 100, with higher scores indicating better functioning. This scale can offer a score on clinical functioning (GAF-C) and another on social functioning (GAF-S). Measure: Global Assessment Functioning (GAF) (Endicott et al., 1976). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: The PANSS evaluates positive and negative symptoms and provides a score of general psychopathology. Measure: Positive and negative syndrome scale (PANSS) (Kay et al., 1987; Peralta and Cuesta, 1995). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Attention Measure: Continuous Performance Test II (CPT-II) (Conners, 2000); Trail Making Test (TMT) (Reitan,1993). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Learning and verbal memory Measure: Rey Auditory Verbal Learning Test (RAVLT) (Rey, 1964) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Executive functions Measure: Wisconsin Card Sorting Test (WCST) (Bergs et al., 1948) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Executive functions Measure: Trail Making Test (TMT-B) (Reitan, 1993) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Executive functions Measure: Stroop Color and Word Test (Stroop, 1935) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Processing Speed Measure: Trail Making Test (TMT-A) (Reintan, 1993) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Processing Speed Measure: Controlled Oral Word Association Test (COWAT) (Benton&Hamsher, 1976) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Processing Speed Measure: Letter-number sequencing (Wechsler Adult Intelligence Scale [WAIS]) (Weschler, 1999) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Will be used to assess 4 components (search and maintain hope, reestablishment of positive identity, find the meaning of life and assume responsibility of one's own life) and 5 stages of the recovery process (moratorium, awareness, preparation, rebuilding and growth). This instrument is made up of 50 items which score in the Likert type scale from 0 to 5. The resulting scores represent the 5 phases of personal/psychological recovery. The scale showing the highest score indicates the stage of recovery in which the patient is at that time. Measure: The Stages of Recovery Instrument (STORI) (Andresen et al., 2006; Lemos et al., 2015) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Quality of life Measure: WHO Quality of Life-BREF 26. (WHOQOL-BREF) (Üstun et al., 1988; Vázquez-Barquero et al., 2000). Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: It's an instrument designed to assess functioning and disability in six main domains: cognition, mobility, self-care, interpersonal relationships, activities of daily living, and participation in society. Measure: World Health Organization Disability Assessment Schedule (WHO-DAS-II) (Üstun et al., 1988; Vázquez-Barquero et al., 2000) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Stigma Measure: Internalized Stigma of Mental Illness Scale (ISMI) (Ritsher, Otilingama, Grajalesa, 2003) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. Description: Self-esteem Measure: Rosenberg self-esteem scale (RSES) (Rosenberg et al., 1965; Atienza, Balaguer & Moreno, 2000) Time Frame: It will be administered 1 time before de treatment, 1 time after finishing the treatment and 1 time after 6 months completing the intervention. ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Presence of one of the e following diagnostics according to the criteria of the Diagnostic and Statistical Manual of Mental Disorders (DSM-5): schizophrenia, schizophreniform disorder, delusional disorder, brief psychotic disorder, schizoaffective disorder, and non specified schizophrenia spectrum disorder and other psychotic disorders. * Be in a stable clinical phase (without psychiatric hospitalization in the last 3 months). * Have good adherence to pharmacological treatment. * T-score \< 40 in any cognitive outcome measured by TAVEC, CPT-IP, TMT, Stroop, WSCT, FAS and WAIS (Vocabulary, Digit Forward, Digit Backwards and Digit Symbol Coding. * Willing to participate in the study expressed by providing signed informed consent. Exclusion Criteria: * Presence of traumatic brain lesion, dementia or intellectual discapacity (IQ \<70). * Positive and Negative Syndrome Scale (PANSS) score \>= 5 in hostility and lack of cooperation and \>= 6 in suspiciousness. * Presence of an additional diagnosis of severe disorder related to substances. * Having participated in a CR and/or MCT intervention in the year prior to incorporation into the study. Maximum Age: 55 Years Minimum Age: 16 Years Sex: ALL Standard Ages: - CHILD - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Ana Barajas Velez Phone: +34935814452 Role: CONTACT #### Locations Location 1: City: Cerdanyola Del Vallès Contacts: *Contact 1:* - Email: [email protected] - Name: Ana Barajas Velez - Phone: +34935814452 - Role: CONTACT Country: Spain Facility: Universitat Autonoma de Barcelona State: Barcelona Status: RECRUITING Zip: 08193 #### Overall Officials Official 1: Affiliation: Universitat Autonoma de Barcelona Name: Ana Barajas Velez Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M4815 - Name: Mental Disorders - Relevance: HIGH - As Found: Psychotic - ID: M15376 - Name: Schizophrenia - Relevance: HIGH - As Found: Schizophrenia - ID: M14473 - Name: Psychotic Disorders - Relevance: HIGH - As Found: Psychotic Disorders - ID: M21838 - Name: Schizophrenia Spectrum and Other Psychotic Disorders - Relevance: HIGH - As Found: Schizophrenia Spectrum and Other Psychotic Disorders - ID: M6902 - Name: Delusions - Relevance: LOW - As Found: Unknown - ID: M15380 - Name: Schizophrenia, Paranoid - Relevance: HIGH - As Found: Delusional Disorder ### Condition Browse Module - Meshes - ID: D000012559 - Term: Schizophrenia - ID: D000001523 - Term: Mental Disorders - ID: D000011618 - Term: Psychotic Disorders - ID: D000019967 - Term: Schizophrenia Spectrum and Other Psychotic Disorders - ID: D000012563 - Term: Schizophrenia, Paranoid ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423638 Acronym: TCERN Brief Title: Feasibility of Virtual Tai Chi Easy for Registered Nurses Official Title: The Feasibility of Tai Chi Easy Training for Registered Nurses #### Organization Study ID Info ID: STUDY00003718 #### Organization Class: OTHER Full Name: University of Arizona ### Status Module #### Completion Date Date: 2024-07-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-07-15 Type: ESTIMATED #### Start Date Date: 2023-12-22 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: University of Arizona #### Responsible Party Investigator Affiliation: University of Arizona Investigator Full Name: Carlie Felion Investigator Title: PI Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This study will examine the feasibility of virtual Tai Chi Easy training for registered nurses and see if participation results in changes in symptoms of transition shock, healthcare-related psychological traumatic stress, burnout, somatic symptoms, and intention to quit. Participants will do virtual Tai Chi Easy for 2 hours per week and practice on their own for 40 minutes per week. The study will last six weeks. Surveys will be completed in REDCap before, during, and after the intervention. Detailed Description: Nurses are the backbone of the healthcare system, comprising 59% of the healthcare workforce (Salmond, 2021); however, research indicates that 32.8% of newly hired Registered Nurses (RNs) voluntarily terminate their positions within the first year and must then be replaced (NSI Nursing Services, 2023). The turnover problem among nurses threatens the delivery of adequate, safe, and timely patient care, the health and well-being of nurses and other healthcare professionals, and the sustainability of the organizations for which they work. High job turnover among nurses is a problem that has inspired the design, implementation, and study of numerous organization/system-driven interventions over at least the past sixty years. Numerous researchers have identified the first year of practice as the most stressful time in a nurse\'s career (Chesak, 2019), with the highest levels occurring at four and eight months of employment (Fang, 2022). These nurses can experience a phenomenon known as \'transition shock,\' comprising cognitive, psychological, and emotional distress (Duchscher, 2009). Transition shock can lead to nurses feeling overwhelmed by the stark and unanticipated realities of nursing practice, especially if that reality conflicts with previously held ideals, beliefs, and expectations. In addition to experiencing elevated stress levels and transition shock, exposure to healthcare-related psychological trauma plays a key role in why nurses have left and continue to leave their positions and the profession in droves (Foli, 2019). Burnout is a common phenomenon among nurses. Key contributors to the development of burnout among healthcare workers include exposure to traumatic events such as witnessing death and suffering, the psychological and physical demands of the job, shift work, low autonomy, inadequate social support, incivility in the workplace, low staffing, and poor communication and collaborative relationships with other healthcare professionals (Chesak, 2019). Despite the significant human and financial resources invested in solutions that attempt to mitigate nurse turnover, there is surprisingly little evidence in the published literature on the use of integrative mind-body self-care interventions to help individual nurses cope with prolonged or toxic levels of stress, burnout, traumatic stress, and somatic symptoms. Self-care deficits are common among nurses, who typically focus on helping and serving others. While altruism, compassion, and a commitment to help others draw many people to a career in nursing, the desire to help others deal with their health problems can sometimes overshadow a nurse\'s motivation or ability to care for themselves (Crane, 2016). A 2017 survey by the American Nurses Association (ANA, 2017) found that 68% of nurses put their patients' safety, health, and wellness ahead of their own. Furthermore, although nurses are well-educated and often teach patients about the importance of health-promoting behaviors, that knowledge does not always translate into engagement in healthy lifestyle behaviors among nurses themselves (Albert, 2014). In the wake of the COVID-19 pandemic, when nurses are more traumatized, stressed, and spread thinner than ever (American Nurses Foundation, 2021), some are resorting to employing maladaptive coping strategies, such as substance or alcohol abuse, to cope with stress and negative emotions (Foli, 2021). This highly problematic engagement in maladaptive coping strategies highlights and underscores the need for safe, cost-effective, accessible, and acceptable self-care options for nurses. Mind-body psychoneuroimmunology-based interventions, such as Tai Chi, have been used for centuries by people all over the world and may be a feasible self-care intervention for new graduate nurses. Mind-body therapies are defined as those that emphasize using the brain in conjunction with the body to harness innate healing powers. Mind-body exercise often includes multiple components, such as breathing practices, focused attention, meditation, and gentle physical movements (Bower, 2016). Numerous conceptual models propose that the primary mechanism by which mind-body therapies produce their effects is through self-regulation, which has a top-down effect on numerous physiological processes that impact health and health behaviors (Bower, 2016). Mind-body modalities can improve nurses\' general health and well-being and may help prevent or reduce burnout by reducing psychological stress and alleviating somatic symptoms (Jung, 2021) through alterations in inflammatory processes (Irwin, 2015). Tai Chi Easy™ (TCE) is a safe, cost-effective, non-pharmacological intervention developed by Dr. Roger Jahnke. TCE is a simplified and streamlined practice that draws from the four main recognized styles of tai chi (Ward, 2023). According to Jahnke (2003), the deliberate attention to breathing, movement, and meditation in tai chi integrates the nervous, endocrine, cardiovascular, digestive, and immune systems with the psyche. TCE practice comprises four baskets: Self-applied massage, mindful movement, breathing exercises, and meditation exercises (Ward, 2023). TCE is appropriate for people of all ages and health conditions because it is easy to learn and perform and is extremely adaptable (Ward, 2023).TCE is a cost-effective and sustainable mind-body intervention that does not require any special clothing, footwear, or equipment and can be practiced virtually anywhere, at any time. Therefore, TCE is the ideal behavioral intervention for this study to help new nurses cope with stress and improve their overall health and well-being. Offering TCE in an asynchronous, virtual format will allow nurses (who often work the night shift and may need to sleep when in-person classes would typically be offered) to allow for greater flexibility and opportunities to access the intervention. The purpose of this study is to a) gain a deeper understanding of factors contributing to high turnover among nurses, including past exposure to adverse childhood experiences and adverse life events, b) determine whether virtual TCE training is a feasible, acceptable, safe, and appropriate mind-body self-care intervention among NGNs, and c) explore whether changes in stress, transition shock, posttraumatic stress symptoms, and transition shock occur after participation in a six-week asynchronous virtual TCE training intervention. The specific aims of this study are as follows: Aim 1: Feasibility - Evaluate whether Tai Chi Easy™ is a feasible, acceptable, and appropriate self-care intervention for registered nurses. Recruitment, retention, intervention adherence, and safety data will also be obtained. Aim 2: Changes in Symptoms of Distress - Explore whether changes in stress, transition shock, burnout, somatic symptoms, posttraumatic stress symptoms, and intention to quit occur post-intervention. The results of this study will 1) fill an important knowledge gap in the nursing literature, 2) inform future studies regarding the use of virtual Tai Chi Easy™ as a safe, acceptable, cost-effective, and sustainable intervention for nurses who may be experiencing the phenomena of interest, and 3) provide information with potential utility for the academic and healthcare industry sectors. There is a demonstrated need to better prepare nurses for the tumultuous and highly stressful entry to professional practice and to guide the design and implementation of programs to help new nurses adjust and remain in their roles. ### Conditions Module Conditions: - Transition Shock - Nurses' Intention to Quit - Stress - Somatic Symptoms - Burnout - Trauma and Stressor Related Disorders Keywords: - Tai Chi Easy - Healthcare-Related Psychological Trauma - Virtual - Transition Shock - burnout - nurse - somatic symptoms - stress ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: SUPPORTIVE_CARE #### Enrollment Info Count: 40 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants will complete two 60 minute virtual Tai Chi Easy classes per week and practice on their own 10 minutes per day on 4 other days each week for six weeks. Intervention Names: - Behavioral: Virtual Tai Chi Easy Label: Intervention Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Intervention Description: The TCE intervention will be delivered asynchronously online. Participants can complete the classes at a time and in a location that is convenient for them. The classes will be offered for one hour twice weekly and were developed and recorded by a certified Tai Chi Easy practice leader. TCE is a simple form of mind-body self-care that focuses on four components: * Mindful movements that help to stretch, and relax the body while improving balance and coordination * Breathing practices that reduce stress by inducing a relaxation response while improving energy and circulation and enhancing innate healing responses * Self-applied massage to stimulate blood flow, relax the body, and improve circulation and energy * Meditation practices to relax the body, center the mind, and calm the emotions Name: Virtual Tai Chi Easy Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: Evaluating the feasibility, acceptability, and appropriateness of intervention, as well as recruitment and retention Measure: Feasibility of Virtual Tai Chi Easy training Time Frame: 8 weeks #### Secondary Outcomes Description: Changes in characteristics of transition shock post-intervention Measure: Transition Shock Time Frame: 8 weeks Description: Changes in burnout symptoms post intervention Measure: Burnout Time Frame: 8 weeks Description: Changes in somatic symptoms post intervention Measure: Somatic Symptoms Time Frame: 8 weeks Description: Changes in intention to quit post-intervention Measure: Intention to Quit Time Frame: 8 weeks Description: Changes in stress and post-traumatic stress symptoms post-intervention Measure: Stress and post-traumatic stress symptoms Time Frame: 8 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: Registered Nurses from any racial/ethnic, socioeconomic group, sex/gender. Access to a computer, tablet, or smartphone Reliable internet access Ability to read and write in English Exclusion Criteria: Refusal to provide informed consent Regularly participating in Tai Chi or other mind-body exercise (as defined by participating more than once per week) Refusal or inability to fully participate in the study protocol Previously diagnosed post-traumatic stress disorder not due to a healthcare-related exposure event, active substance use disorder, or serious mental illness. An acute or chronic medical or mental health condition that would otherwise limit the person's ability to fully participate in study activities. Healthy Volunteers: True Maximum Age: 99 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Carlie Felion, PhDc Phone: (480) 749-4550 Role: CONTACT Contact 2: Email: [email protected] Name: Ruth Taylor-Piliae, PhD Phone: (520) 626-4881 Role: CONTACT #### Locations Location 1: City: Tucson Contacts: *Contact 1:* - Email: [email protected] - Name: Carlie Felion, PhDc - Phone: 480-749-4550 - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Ruth Taylor-Piliae, PhD - Phone: (520) 626-4881 - Role: CONTACT Country: United States Facility: University of Arizona State: Arizona Status: RECRUITING Zip: 85721 #### Overall Officials Official 1: Affiliation: University of Arizona Name: Carlie M Felion Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Description: No plan to share data with other researchers IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000013315 - Term: Stress, Psychological - ID: D000001526 - Term: Behavioral Symptoms - ID: D000001523 - Term: Mental Disorders ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC26 - Name: Wounds and Injuries - Abbrev: BXM - Name: Behaviors and Mental Disorders ### Condition Browse Module - Browse Leaves - ID: M15577 - Name: Shock - Relevance: LOW - As Found: Unknown - ID: M17685 - Name: Wounds and Injuries - Relevance: LOW - As Found: Unknown - ID: M222 - Name: Trauma and Stressor Related Disorders - Relevance: HIGH - As Found: Trauma and Stressor Related Disorders - ID: M885 - Name: Medically Unexplained Symptoms - Relevance: HIGH - As Found: Somatic Symptom - ID: M1658 - Name: Burnout, Psychological - Relevance: HIGH - As Found: Burnout - ID: M113 - Name: Psychological Trauma - Relevance: LOW - As Found: Unknown - ID: M16105 - Name: Stress, Psychological - Relevance: LOW - As Found: Unknown - ID: M4818 - Name: Behavioral Symptoms - Relevance: LOW - As Found: Unknown - ID: M4815 - Name: Mental Disorders - Relevance: LOW - As Found: Unknown - ID: M14473 - Name: Psychotic Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000071896 - Term: Medically Unexplained Symptoms - ID: D000077062 - Term: Burnout, Psychological - ID: D000068099 - Term: Trauma and Stressor Related Disorders ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423625 Acronym: MIRON-PREDICT Brief Title: Hemorrhagic MI Prediction Score Model Official Title: Developing a Prediction Score Model for Predicting the Likelihood of Hemorrhagic MI Before Percutaneous Coronary Reperfusion Therapy #### Organization Study ID Info ID: 19978d #### Organization Class: OTHER Full Name: Indiana University ### Status Module #### Completion Date Date: 2024-03-31 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-24 Type: ACTUAL Last Update Submit Date: 2024-05-23 Overall Status: COMPLETED #### Primary Completion Date Date: 2024-03-31 Type: ACTUAL #### Start Date Date: 2023-06-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Rohan Dharmakumar #### Responsible Party Investigator Affiliation: Indiana University School of Medicine Investigator Full Name: Rohan Dharmakumar Investigator Title: Executive Director, Krannert Cardiovascular Research Center Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Developing a prediction score model for predicting the likelihood of Hemorrhagic MI ### Conditions Module Conditions: - Acute Myocardial Infarction Keywords: - Acute Myocardial Infarction - Prediction Score - Machine Learning - Hemorrhagic MI ### Design Module #### Design Info Observational Model: COHORT Time Perspective: RETROSPECTIVE #### Enrollment Info Count: 1100 Type: ACTUAL Study Type: OBSERVATIONAL ### Outcomes Module #### Primary Outcomes Description: Risk factor model before reperfusion Measure: Hemorrhagic MI Time Frame: Emergency admission to Percutaneous Intervention ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age \> 18 yrs * Index MI * Primary PCI Exclusion Criteria: * History of prior myocardial infarction, * Thrombolysis before PCI * Contraindication to Cardiac MRI Maximum Age: 80 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: The study population consists of individuals aged 18 - 80 yrs who have been diagnosed with acute ST-elevation myocardial infarction (STEMI) and are scheduled for emergency percutaneous coronary intervention (PCI). ### Contacts Locations Module #### Locations Location 1: City: Indianapolis Country: United States Facility: Krannert Cardiovascular Research Center, Indiana University School of Medicine State: Indiana Zip: 46202 #### Overall Officials Official 1: Affiliation: Indiana University School of Medicine, Krannert Cardiovascular Research Center Name: Keyur P Vora, MD FACC Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000007511 - Term: Ischemia - ID: D000010335 - Term: Pathologic Processes - ID: D000009336 - Term: Necrosis - ID: D000017202 - Term: Myocardial Ischemia - ID: D000006331 - Term: Heart Diseases - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000014652 - Term: Vascular Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M12155 - Name: Myocardial Infarction - Relevance: HIGH - As Found: Myocardial Infarction - ID: M10282 - Name: Infarction - Relevance: HIGH - As Found: Infarction - ID: M10543 - Name: Ischemia - Relevance: LOW - As Found: Unknown - ID: M12284 - Name: Necrosis - Relevance: LOW - As Found: Unknown - ID: M6546 - Name: Coronary Artery Disease - Relevance: LOW - As Found: Unknown - ID: M19506 - Name: Myocardial Ischemia - Relevance: LOW - As Found: Unknown - ID: M9419 - Name: Heart Diseases - Relevance: LOW - As Found: Unknown - ID: M17400 - Name: Vascular Diseases - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000009203 - Term: Myocardial Infarction - ID: D000007238 - Term: Infarction ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423612 Acronym: ROVING-PUMA Brief Title: Randomized Trial to Optimize Virologic Suppression Rates Using a Point-of-Care Urine Monitoring Assay (ROVING PUMA) Official Title: Randomized Trial to Optimize Virologic Suppression Rates Using a Point-of-Care Urine Monitoring Assay (ROVING PUMA) #### Organization Study ID Info ID: A143057 #### Organization Class: OTHER Full Name: University of California, San Francisco #### Secondary ID Infos ID: R01AI143340-06 Link: https://reporter.nih.gov/quickSearch/R01AI143340-06 Type: NIH ### Status Module #### Completion Date Date: 2029-08-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-24 Type: ACTUAL Last Update Submit Date: 2024-05-22 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2029-08-30 Type: ESTIMATED #### Start Date Date: 2024-07-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Desmond Tutu HIV Foundation Class: OTHER Name: University of Cape Town Class: NIH Name: National Institute of Allergy and Infectious Diseases (NIAID) #### Lead Sponsor Class: OTHER Name: University of California, San Francisco #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Antiretroviral therapy (ART) has significantly decreased the morbidity and mortality of HIV infection. However, adherence challenges in taking daily oral ART persist. A retrospective cohort study across 31 countries from 2010-19 reported that only 65% of people with HIV (PWH) on ART exhibited virologic suppression (VS) three years after starting ART;1 the rate of VS in South Africa among PWH on ART is 60-65%. Adherence barriers span individual and structural factors, such as stigma, recall difficulties, housing and/or food insecurity, mental illness, substance use, transportation, stock-outs, and other factors that vary by country and population. Adherence interventions can benefit from direct objective adherence monitoring. Pharmacologic metrics of adherence assess drug levels in plasma, dried blood spots, hair (a metric our group pioneered) or urine and predict outcomes more accurately than self-reported adherence. However, most of these metrics preclude real-time assessment, requiring expensive laboratory equipment and trained laboratory personnel. Thus, few adherence interventions have successfully incorporated objective metrics, likely due to laboratory and shipping delays. A low-cost (\<$2/test) point-of-care adherence metric - developed by our group - should allow for real-time biofeedback and improve the impact of metric-driven adherence interventions. Detailed Description: This is a randomized hybrid type 1 effectiveness study design to assess the factors related to implementation of a point-of-care urine TFV assay test into routine HIV clinical care. We plan to recruit a total of 500 adults living with HIV who received primary HIV care from one of the selected study clinics in BCM, Eastern Cape. Individuals who have been prescribed ART for at least 6 months who have not achieved VS will be randomized in a 1:1 fashion at the baseline visit to the intervention arm vs. the SoC arm. Total duration of the study is 18 months from the time of enrollment. ### Conditions Module Conditions: - ART Adherence Keywords: - ART - Adherence - South Africa - Viral Suppression - ART resistance - POC urine assay - TDF assay ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Randomized hybrid type 1 effectiveness trial ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 500 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Conduct enhanced ART adherence counselling informed by the results of the point-of-care urine assay for TFV to increase viral suppression. Intervention Names: - Behavioral: POC urine assay informed enhanced ART adherence counselling for viral suppression Label: POC Urine Test Informed ART Adherence Counselling Type: EXPERIMENTAL #### Arm Group 2 Description: Follow South Africa's standard-of-care enhanced ART adherence counselling for viral suppression. Label: Standard-of-care Enhanced Adherence Counselling Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - POC Urine Test Informed ART Adherence Counselling Description: Collect urine on intervention participants and screen for presence of TFV. Feedback will be provided to the participant based on the results on their ART adherence with provision of enhanced ART adherence counseling for viral suppression. Name: POC urine assay informed enhanced ART adherence counselling for viral suppression Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: The primary outcome of effectiveness will be viral suppression at 6 months. Measure: Viral Suppression at 6 months Time Frame: 18 months #### Secondary Outcomes Description: Durability of the 6-month intervention on viral suppression at 9, 12, and 18months Measure: Viral suppression at 9, 12, and 18months Time Frame: 18 months Description: The effect of the intervention on need for resistance testing and genotype results @ 6 and 18 months Measure: Resistance testing and genotype results @ 6 and 18 months Time Frame: 18 months Description: Assess the feasibility and acceptability of the intervention using a survey and in-depth interviews Measure: Feasibility and Acceptability of the intervention Time Frame: 18 months Description: Assess the cost per patient, cost per additional patient with VS, and cost per disability-adjusted life-year averted from a society perspective with using the urine-based TFV adherence assay to inform adherence counseling vs. standard of care counseling. Measure: Cost-effectiveness of the intervention Time Frame: 18 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: Aim 1: Individuals ≥16 years of age at the initial screening visit living with HIV, prescribed ART for at least three months, and are not virally suppressed. Aim 2: Same as Aim 1 for the acceptability survey and in-depth interviews. HIV care providers in the selected clinic sites for the feasibility survey and in-depth interviews. Aim 3: Same as Aim 1 for the cost-effectiveness study. Exclusion Criteria: * Currently enrolled in another ART adherence intervention * Patients on ART regimen that does not include Tenofovir * HIV care providers from non-study sites Failure to provide written consent Healthy Volunteers: True Minimum Age: 16 Years Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Monica Gandhi Phone: 415 476 4082 Phone Ext: 127 Role: CONTACT Contact 2: Email: [email protected] Name: Purba Chatterjee Role: CONTACT #### Locations Location 1: City: East London Contacts: *Contact 1:* - Email: [email protected] - Name: Sammy Nena - Phone: +27715153785 - Role: CONTACT *Contact 2:* - Name: Andrew Marino, PhD - Role: PRINCIPAL_INVESTIGATOR Country: South Africa Facility: Desmond Tutu HIV Foundation #### Overall Officials Official 1: Affiliation: University of California, San Francisco Name: Monica Gandhi Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: Investigators conducting ART adherence research. Description: We will share de-identified data in publicly accessible databases once study is complete and study findings disseminated. Info Types: - STUDY_PROTOCOL - SAP - ICF - CSR - ANALYTIC_CODE IPD Sharing: YES Time Frame: 48 months from start of study ### References Module #### References Citation: Niu X, Kubiak RW, Siriprakaisil O, Klinbuyaem V, Sukrakanchana PO, Cressey R, Okochi H, Gandhi M, Cressey TR, Drain PK. Tenofovir-Diphosphate in Dried Blood Spots vs Tenofovir in Urine/Plasma for Oral Preexposure Prophylaxis Adherence Monitoring. Open Forum Infect Dis. 2022 Aug 10;9(8):ofac405. doi: 10.1093/ofid/ofac405. eCollection 2022 Aug. PMID: 36004315 Citation: Spinelli MA, Haberer JE, Chai PR, Castillo-Mancilla J, Anderson PL, Gandhi M. Approaches to Objectively Measure Antiretroviral Medication Adherence and Drive Adherence Interventions. Curr HIV/AIDS Rep. 2020 Aug;17(4):301-314. doi: 10.1007/s11904-020-00502-5. PMID: 32424549 Citation: Gandhi M, Wang G, King R, Rodrigues WC, Vincent M, Glidden DV, Cressey TR, Bacchetti P, Spinelli MA, Okochi H, Siriprakaisil O, Klinbuayaem V, Mugo NR, Ngure K, Drain PK, Baeten JM. Development and validation of the first point-of-care assay to objectively monitor adherence to HIV treatment and prevention in real-time in routine settings. AIDS. 2020 Feb 1;34(2):255-260. doi: 10.1097/QAD.0000000000002395. PMID: 31634188 Citation: Cressey TR, Siriprakaisil O, Kubiak RW, Klinbuayaem V, Sukrakanchana PO, Quame-Amaglo J, Okochi H, Tawon Y, Cressey R, Baeten JM, Gandhi M, Drain PK. Plasma pharmacokinetics and urinary excretion of tenofovir following cessation in adults with controlled levels of adherence to tenofovir disoproxil fumarate. Int J Infect Dis. 2020 Aug;97:365-370. doi: 10.1016/j.ijid.2020.06.037. Epub 2020 Jun 14. PMID: 32553717 Citation: Drain PK, Bardon AR, Simoni JM, Cressey TR, Anderson P, Sevenler D, Olanrewaju AO, Gandhi M, Celum C. Point-of-care and Near Real-time Testing for Antiretroviral Adherence Monitoring to HIV Treatment and Prevention. Curr HIV/AIDS Rep. 2020 Oct;17(5):487-498. doi: 10.1007/s11904-020-00512-3. PMID: 32627120 Citation: Drain P, Ngure K, Mugo N, Spinelli M, Chatterjee P, Bacchetti P, Glidden D, Baeten J, Gandhi M. Testing a Real-Time Tenofovir Urine Adherence Assay for Monitoring and Providing Feedback to Preexposure Prophylaxis in Kenya (PUMA): Protocol for a Pilot Randomized Controlled Trial. JMIR Res Protoc. 2020 Apr 2;9(4):e15029. doi: 10.2196/15029. PMID: 32238341 ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423599 Acronym: FIT-HF Brief Title: Effect of Weight Loss on Physical and Cardiac Performance in People With Obesity and Heart Failure Official Title: Effect of Weight Loss on Physical and Cardiac Performance in People With Obesity and Heart Failure #### Organization Study ID Info ID: U1111-1298-6418 #### Organization Class: OTHER Full Name: Hvidovre University Hospital #### Secondary ID Infos ID: 2023-503753-35-01 Type: CTIS ### Status Module #### Completion Date Date: 2026-12-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-24 Type: ACTUAL Last Update Submit Date: 2024-05-23 Overall Status: RECRUITING #### Primary Completion Date Date: 2026-06-30 Type: ESTIMATED #### Start Date Date: 2024-05-17 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Jens D Hove, MD,PHD #### Responsible Party Investigator Affiliation: Hvidovre University Hospital Investigator Full Name: Jens D Hove, MD,PHD Investigator Title: Chief Physician, Research associate Professor, MD, PhD Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: The benefit of weight loss in patients with obesity and heart failure with reduced ejection fraction (HFrEF) is controversial. Semaglutide has shown cardiovascular (CV) risk-reduction and impact on CV risk factors including overweight, dysglycaemia and hypertension in subjects with type 2 diabetes (T2D). The STEP-HFpEF (Semaglutide Treatment Effect in People With Obesity and HFpEF) recently demonstrated, at 1-year, to not only reduce weight considerably, but also significantly improve health-related quality of life, functional status scores and 6-min walk distance in patients with heart failure with preserved ejection fraction (HFpEF). Also, the recently concluded SELECT trial was the first CV outcome trial with semaglutide in patients with overweight or obesity and established CV disease, including heart failure (but no T2D). Semaglutide demonstrated a 20% reduction in MACE, defined as the composite of cardiovascular death, non-fatal myocardial infarction, and non-fatal stroke. These landmark findings have important implications for clinicians -as they mean that weight loss and/or semaglutide as anti-obesity pharmacotherapy could be a treatment strategy for secondary prevention of CV disease in patients with overweight or obesity. It is, however, unknown whether weight loss with either calorie-restricted diet or semaglutide has beneficial effects in obese subjects with heart failure and reduced ejection fraction. Also it is unclear whether semaglutide has cardiovascular benefits irrespective of starting weight and amount of weight loss. Purpose: The study aims to investigate whether weight loss treatment with semaglutide is superior to weight loss with calorie-restricted diet in improving peak oxygen uptake in patients with obesity and heart failure with reduced ejection fraction. Detailed Description: Background: The prevalence of overweight and obesity has reached pandemic proportions. Obesity is known to increase the risk for Type 2 diabetes and hypertension, as well as the risk for overt cardiovascular (CV) disease, including myocardial infarction, heart failure, and stroke. The rising prevalence of obesity may counteract the recent advances in primary and secondary prevention of CV disease. Overweight and obesity are common in patients with CV disease; however, cardiologists face several challenges in managing body weight in this population. Many may not consider obesity as a therapeutic target probably because there were no previous highly effective and safe pharmacologic interventions to consider. In addition, they may not have the expertise or resources to implement lifestyle interventions and may have limited familiarity with obesity pharmacotherapy. Moreover, the long-term CV effects of obesity pharmacotherapy remain uncertain due to limited CV outcome data with weight loss as the primary intervention. Although current CV guidelines recognize the importance of weight loss, they primarily focus on lifestyle modifications, with fewer details on strategies to utilize obesity pharmacotherapy and surgery. However, the recent 2022 American Diabetes Association/European Association for the Study of Diabetes consensus on the management of Type 2 diabetes has moved up weight management to the front of the treatment algorithm, by prioritizing the use of pharmacologic interventions such as glucagon-like peptide-1 receptor agonists and dual glucose-dependent insulinotropic polypeptide/glucagon-like peptide-1 receptor agonists, which have potent weight-lowering effects, in addition to glucose-lowering effects. Hypothesis: The investigators hypothesise that weight loss treatment with semaglutide is superior to weight loss with state-of-the-art calorie-restricted diet in improving the peak oxygen uptake (ml/min/kg) after 52 weeks as a marker of physical performance (and with prognostic implications) in patients with obesity and heart failure with reduced ejection fraction. Design: This is a investigator-initiated, parallel-group, 2-arm assessor-blinded, open-label, randomised, controlled trial (RCT) comparing the effect of weight loss using low-calorie replacement diet to weight loss using semaglutide in obese patients with heart failure with reduced ejection fraction. Subjects will be randomised in a 1:1 ratio to receive either low-calorie replacement diet or semaglutide.The subjects wil be followed for 52 weeks during the intervention period. The patients will be examined at 16 weeks (where the weight loss is anticipated to be approximately equal in the two groups) and after 52 weeks. Primary, secondary and exploratory objectives are listed below. The exploratory objectives are mostly embedded mechanistic studies of an exploratory nature and therefore hypothesis-generating in the RCT. Intervention: Subjects will be treated with semaglutide once weekly or a weight loss intervention consisting of a calorie-restricted diet and dietary advice on top of standard of care, which covers management of heart failure medication, CV risk factors and healthy lifestyle counselling. ### Conditions Module Conditions: - Heart Failure With Reduced Ejection Fraction - Obesity - Weight Loss - Chronic Heart Failure ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: This is a investigator-initiated, parallel-group, 2-arm assessor-blinded, open-label, randomised, clinical trial ##### Masking Info Masking: SINGLE Masking Description: Anonymized data will be analyzed Who Masked: - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 100 Type: ESTIMATED Phases: - PHASE2 - PHASE3 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Dose-escalation of semaglutide will take place during the first 16 weeks after randomisation (week 0). Patients will start at the 0.25 mg once-weekly dose and follow dose-escalation schedule (0.25, 0.5, 1.0, 1.7 and 2.4 mg). For all subjects we aim at reaching the recommended target dose of 2.4 mg semaglutide once weekly for the rest of the period of total 52 weeks. Intervention Names: - Drug: Semaglutide Injectable Product Label: Semaglutide intervention group Type: EXPERIMENTAL #### Arm Group 2 Description: In short, the weight loss program in the calorie-restricted diet group consists of 3 phases after randomisation (week 0). An initial weight loss phase of 8 weeks with 800 calories/day, a food re-introduction phase for 8 weeks and a weight loss maintenance phase for the rest of the period of total 52 weeks. Intervention Names: - Dietary Supplement: Calorie-restricted diet Label: Calorie-restricted diet intervention group Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Semaglutide intervention group Description: Weight loss using Semaglutide Name: Semaglutide Injectable Product Type: DRUG #### Intervention 2 Arm Group Labels: - Calorie-restricted diet intervention group Description: Weight loss by calorie-restricted diet program followed by a weight loss maintenance follow-up program Name: Calorie-restricted diet Type: DIETARY_SUPPLEMENT ### Outcomes Module #### Other Outcomes Measure: Composite endpoint consisting of all-cause death, non-fatal myocardial infarction, non-fatal stroke, heart failure hospitalisation or urgent heart failure visit Time Frame: Follow-up at 52 weeks Measure: First occurrence of a composite heart failure endpoint consisting of: heart failure hospitalisation, urgent heart failure visit, ischemic events or CV death Time Frame: Follow-up at 52 weeks Measure: All-cause death Time Frame: Follow-up at 52 weeks Measure: Total number of hospitalised days Time Frame: Follow-up at 52 weeks Measure: Total number of hospitalisations Time Frame: Follow-up at 52 weeks Measure: Total number of Serious Adverse Events (SAEs) Time Frame: Follow-up at 52 weeks Measure: Change in heart failure medication Time Frame: Follow-up at 52 weeks Description: To examine the effect of a weight loss with either calorie-restricted diet or semaglutide on quality of life in patients with obesity and heart failure with reduced EF Measure: EuroQol five dimensions five level (EQ-5D-5L) questionnaire Time Frame: The patients will answer a questionnaire after 0, 16 and 52 weeks Measure: Effects of weight loss with either treatment on cardiac metabolism, fibrosis, inflammation, and diastolic function by Cardiac MRI and Cardiac Rubidium-PET Time Frame: The patients will be examined after 0, 16 and 52 weeks Description: Analysis of: Blood samples, pulmonary function test and body composition scan (DEXA) Measure: Potentially favorable changes in other organ systems caused by weight loss in this patient group Time Frame: The patients will be examined after 0, 16 and 52 weeks Measure: Feasibility and safety of two modern weight loss programs for aggressive weight lowering in patients with heart failure with reduced ejection fraction. Time Frame: Follow-up at 52 weeks Measure: Changes in systolic and diastolic function and cardiac morphology assessed by echocardiography Time Frame: The patients will be examined after 0, 16 and 52 weeks #### Primary Outcomes Description: To examine the effect of weight loss on mean change in peak oxygen uptake at 52 weeks between semaglutide and calorie-restricted group compared to baseline (Measured in ml O2/(kg x min)) Measure: Peak oxygen uptake Time Frame: The patients will be examined after 0, 16 and 52 weeks #### Secondary Outcomes Description: To compare the effect of weight loss on the mean change Measure: The Clinical Summary Score of the Kansas City Cardiomyopathy Questionnaire (KCCQ-CSS) Time Frame: The patients will be examined after 0, 16 and 52 weeks. Description: To compare the effect of weight loss on the mean change Measure: 6-min walk distance (6MWD) Time Frame: The patients will be examined after 0, 16 and 52 weeks Description: To compare the effect of weight loss on the mean change Measure: End-systolic volume of the left ventricle assessed by Cardiac MRI Time Frame: The patients will be examined after 0, 16 and 52 weeks Description: To compare the effect of weight loss on the mean change Measure: N-terminal pro-B-type natriuretic peptide (NT-proBNP) and C-reactive protein (CRP) change Time Frame: The patients will be examined after 0, 16 and 52 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Male or female, age ≥ 18 years at the time of signing informed consent * Body mass index (BMI) ≥ 30 kg/m2 * Heart failure with New York Heart Association (NYHA)-class 1-3 and reduced ejection fraction (EF≤40%) established by either: 1. echocardiography AND/OR 2. cardiac magnetic resonance * On stable optimal medical heart failure therapy for at least 4 weeks Exclusion Criteria: 1. Cardiovascular-related: * Any of the following: myocardial infarction, stroke, hospitalisation for unstable angina pectoris or transient ischaemic attack within the past 6 months prior to the day of screening * Planned coronary, carotid or peripheral artery revascularisation known on the day of screening * Transient heart failure related to reversible mechanisms like tachycardia, sepsis, etc. 2. Glycaemia-related: * Type 1 diabetes * Treatment with any Glucagon-Like Peptide-1 (GLP-1) agonists within 90 days prior to the day of screening * Type 2 diabetes requiring other pharmacotherapy than metformin and Sodium-glucose Cotransporter-2 (SGLT2) Inhibitors 3. General safety: * Pregnancy or planned pregnancy * History or presence of chronic pancreatitis * Presence of acute pancreatitis within the past 180 days prior to the day of screening * Kidney disease with eGFR \< 35ml/min * Presence or history of malignant neoplasms within the past 5 years prior to the day of screening (Basal and squamous cell skin cancer and any carcinoma in-situ are allowed) * Known or suspected hypersensitivity to trial product(s) or related products Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Jens D Hove, MD, PhD Phone: +4538623218 Role: CONTACT Contact 2: Email: [email protected] Name: Mohammed El-Sheikh, MD Phone: +4552309685 Role: CONTACT #### Locations Location 1: City: Copenhagen Contacts: *Contact 1:* - Email: [email protected] - Name: Jens D Hove, MD, PhD - Phone: +4538623218 - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Mohammed El-Sheikh, MD - Phone: +4552309685 - Role: CONTACT Country: Denmark Facility: Amager and Hvidovre Hospital University of Copenhagen Status: RECRUITING Zip: DK-2650 #### Overall Officials Official 1: Affiliation: Amager-Hvidovre Universitetshospital Name: Jens D Hove Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000050177 - Term: Overweight - ID: D000044343 - Term: Overnutrition - ID: D000009748 - Term: Nutrition Disorders - ID: D000006331 - Term: Heart Diseases - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000001836 - Term: Body Weight Changes ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M12701 - Name: Obesity - Relevance: HIGH - As Found: Obesity - ID: M9421 - Name: Heart Failure - Relevance: HIGH - As Found: Heart Failure - ID: M18102 - Name: Weight Loss - Relevance: HIGH - As Found: Weight Loss - ID: M5114 - Name: Body Weight - Relevance: HIGH - As Found: Weight - ID: M26186 - Name: Overweight - Relevance: LOW - As Found: Unknown - ID: M25307 - Name: Overnutrition - Relevance: LOW - As Found: Unknown - ID: M12684 - Name: Nutrition Disorders - Relevance: LOW - As Found: Unknown - ID: M9419 - Name: Heart Diseases - Relevance: LOW - As Found: Unknown - ID: M5115 - Name: Body Weight Changes - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000006333 - Term: Heart Failure - ID: D000009765 - Term: Obesity - ID: D000001835 - Term: Body Weight - ID: D000015431 - Term: Weight Loss ### Intervention Browse Module - Ancestors - ID: D000097789 - Term: Glucagon-Like Peptide-1 Receptor Agonists - ID: D000007004 - Term: Hypoglycemic Agents - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: Hypo - Name: Hypoglycemic Agents - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Gast - Name: Gastrointestinal Agents ### Intervention Browse Module - Browse Leaves - ID: M353561 - Name: Semaglutide - Relevance: HIGH - As Found: Consent - ID: M9043 - Name: Glucagon - Relevance: LOW - As Found: Unknown - ID: M3401 - Name: Glucagon-Like Peptide-1 Receptor Agonists - Relevance: LOW - As Found: Unknown - ID: M26997 - Name: Glucagon-Like Peptide 1 - Relevance: LOW - As Found: Unknown - ID: M10054 - Name: Hypoglycemic Agents - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: C000591245 - Term: Semaglutide ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423586 Brief Title: Effect of Lecithin-based Curcuma and Boswellia on Post-acute COVID-19 IBS Official Title: Positive Effect of Lecithin-based Delivery Form of Curcuma and Boswellia Extracts on Post-acute COVID-19 Irritable Bowel Syndrome. Two Cohorts of an Open-label Study. #### Organization Study ID Info ID: 0912/09052020 #### Organization Class: OTHER Full Name: Azienda di Servizi alla Persona di Pavia ### Status Module #### Completion Date Date: 2022-06-10 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-22 Overall Status: COMPLETED #### Primary Completion Date Date: 2021-10-01 Type: ACTUAL #### Start Date Date: 2021-09-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Azienda di Servizi alla Persona di Pavia #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: This open-label study investigates the effects of lecithin-based formulations of Curcuma longa (Meriva™) and Boswellia serrata (Casperome™) extracts on post-acute COVID-19 irritable bowel syndrome (PCIBS) and irritable bowel syndrome (IBS) without prior COVID-19 infection. A total of 44 participants, 16 with PCIBS and 28 controls with IBS, were supplemented for 30 days. Outcomes measured included abdominal bloating, abdominal pain, enteral dysbiosis, and global assessment of efficacy. The study found significant reductions in bloating and pain in both groups, with a notable decrease in dysbiosis only in the IBS group. This suggests potential benefits of the supplementation in managing gastrointestinal symptoms associated with PCIBS and IBS. Detailed Description: This study aims to evaluate the efficacy and safety of lecithin-based formulations of Curcuma longa (Meriva™) and Boswellia serrata (Casperome™) extracts in treating gastrointestinal symptoms in patients with post-acute COVID-19 irritable bowel syndrome (PCIBS) and irritable bowel syndrome (IBS) without prior COVID-19 infection. The study was conducted at the Department of Public Health of the University of Pavia, Italy. Participants included 16 PCIBS patients and 28 IBS controls, aged 18-75 years. They were administered 500 mg of Curcuma longa and 150 mg of Boswellia serrata extracts twice daily for 30 days, in conjunction with a low FODMAP diet. Key outcomes measured were reductions in abdominal bloating and pain, changes in enteral dysbiosis as indicated by urinary indican levels, and overall treatment efficacy as assessed by participants. The study found that both groups experienced significant reductions in abdominal bloating and pain. However, a notable decrease in enteral dysbiosis was observed only in the IBS control group. The treatment was well tolerated with no reported adverse effects. These findings suggest that the combination of Curcuma longa and Boswellia serrata extracts may provide significant benefits in managing gastrointestinal symptoms associated with PCIBS and IBS. ### Conditions Module Conditions: - Post-Acute COVID-19 Syndrome - Irritable Bowel Syndrome - Abdominal Pain - Dysbiosis Keywords: - abdominal pain - Bloating - Boswellia serrata - Covid-19 infection - Curcuma longa - Dysbiosis - IBS (irritable bowel syndrome) - Long Covid ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 44 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants with post-acute COVID-19 irritable bowel syndrome (PCIBS) supplemented with lecithin-based formulations of Curcuma longa (Meriva™) and Boswellia serrata (Casperome™) extracts. Intervention Names: - Dietary Supplement: Curcuma longa and Boswellia serrata extracts Label: PCIBS Group Type: EXPERIMENTAL #### Arm Group 2 Description: Participants with irritable bowel syndrome (IBS) without prior COVID-19 infection supplemented with lecithin-based formulations of Curcuma longa (Meriva™) and Boswellia serrata (Casperome™) extracts. Intervention Names: - Dietary Supplement: Curcuma longa and Boswellia serrata extracts Label: IBS Control Group Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - IBS Control Group - PCIBS Group Description: Participants received 500 mg of Curcuma longa and 150 mg of Boswellia serrata extracts (Meriva™ and Casperome™) twice daily for 30 days. Name: Curcuma longa and Boswellia serrata extracts Type: DIETARY_SUPPLEMENT ### Outcomes Module #### Other Outcomes Description: Assess the overall efficacy of the treatment using a 4-point scale (ineffective, moderately effective, effective, very effective). Measure: Global Assessment of Efficacy (GAE) Time Frame: 30 days #### Primary Outcomes Description: Measure the change in abdominal bloating severity from baseline to the end of the study using a validated questionnaire. Measure: Reduction in Abdominal Bloating Time Frame: 30 days #### Secondary Outcomes Description: Evaluate the change in urinary indican levels from baseline to the end of the study to assess enteral dysbiosis Measure: Change in Urinary Indican Levels Time Frame: 30 days ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age: 18-75 years, male or female. * Diagnosis of post-acute COVID-19 irritable bowel syndrome (PCIBS) 60-120 days after the end of infection. * Diagnosis of irritable bowel syndrome (IBS) without prior COVID-19 infection. * Evidence of functional abdominal bloating/distention (FAB/D) type of IBS according to Mearin et al. * Presence of enteral dysbiosis defined by increased urinary indican values with normal skatole urinary concentration. Exclusion Criteria: * Normal urinary indican values or increased urinary skatole values. * Subjects already on a low FODMAP diet or other dietary restrictions such as gluten-free diet or lactose-free diet within the past 6 months. * Allergies to soy, nuts, or seafood, or insulin-dependent diabetes. * Known history of celiac disease, symptomatic diverticular disease, inflammatory bowel disease, or microscopic colitis. * Prior small bowel or colonic surgery or cholecystectomy. * Presence of bloody diarrhea or severe vomiting. * Severe renal disease (serum creatinine \>1.5 mg/dL) or liver disease (altered liver function tests). Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Pavia Country: Italy Facility: Mariangela Rondanelli State: PV Zip: 27100 #### Overall Officials Official 1: Affiliation: Italian Diagnostic Center (CDI) Name: Giacosa Attilio Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000004194 - Term: Disease - ID: D000010335 - Term: Pathologic Processes - ID: D000011024 - Term: Pneumonia, Viral - ID: D000011014 - Term: Pneumonia - ID: D000012141 - Term: Respiratory Tract Infections - ID: D000007239 - Term: Infections - ID: D000014777 - Term: Virus Diseases - ID: D000018352 - Term: Coronavirus Infections - ID: D000003333 - Term: Coronaviridae Infections - ID: D000030341 - Term: Nidovirales Infections - ID: D000012327 - Term: RNA Virus Infections - ID: D000008171 - Term: Lung Diseases - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000003109 - Term: Colonic Diseases, Functional - ID: D000003108 - Term: Colonic Diseases - ID: D000007410 - Term: Intestinal Diseases - ID: D000005767 - Term: Gastrointestinal Diseases - ID: D000004066 - Term: Digestive System Diseases - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations - ID: D000012817 - Term: Signs and Symptoms, Digestive - ID: D000094025 - Term: Post-Infectious Disorders - ID: D000002908 - Term: Chronic Disease - ID: D000020969 - Term: Disease Attributes ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC01 - Name: Infections - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M16355 - Name: Syndrome - Relevance: HIGH - As Found: Syndrome - ID: M10283 - Name: Infections - Relevance: LOW - As Found: Unknown - ID: M3013 - Name: Post-Acute COVID-19 Syndrome - Relevance: HIGH - As Found: Post-Acute COVID-19 Syndrome - ID: M2561 - Name: COVID-19 - Relevance: HIGH - As Found: COVID-19 - ID: M25118 - Name: Irritable Bowel Syndrome - Relevance: HIGH - As Found: Irritable Bowel Syndrome - ID: M6368 - Name: Communicable Diseases - Relevance: LOW - As Found: Unknown - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M18311 - Name: Abdominal Pain - Relevance: HIGH - As Found: Abdominal Pain - ID: M30405 - Name: Dysbiosis - Relevance: HIGH - As Found: Dysbiosis - ID: M13904 - Name: Pneumonia - Relevance: LOW - As Found: Unknown - ID: M13914 - Name: Pneumonia, Viral - Relevance: LOW - As Found: Unknown - ID: M14978 - Name: Respiratory Tract Infections - Relevance: LOW - As Found: Unknown - ID: M17522 - Name: Virus Diseases - Relevance: LOW - As Found: Unknown - ID: M20490 - Name: Coronavirus Infections - Relevance: LOW - As Found: Unknown - ID: M6555 - Name: Coronaviridae Infections - Relevance: LOW - As Found: Unknown - ID: M23685 - Name: Nidovirales Infections - Relevance: LOW - As Found: Unknown - ID: M15149 - Name: RNA Virus Infections - Relevance: LOW - As Found: Unknown - ID: M11168 - Name: Lung Diseases - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: M6336 - Name: Colonic Diseases - Relevance: LOW - As Found: Unknown - ID: M6337 - Name: Colonic Diseases, Functional - Relevance: LOW - As Found: Unknown - ID: M10444 - Name: Intestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: M15622 - Name: Signs and Symptoms, Digestive - Relevance: LOW - As Found: Unknown - ID: M3014 - Name: Post-Infectious Disorders - Relevance: LOW - As Found: Unknown - ID: M6147 - Name: Chronic Disease - Relevance: LOW - As Found: Unknown - ID: M22700 - Name: Disease Attributes - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000086382 - Term: COVID-19 - ID: D000094024 - Term: Post-Acute COVID-19 Syndrome - ID: D000043183 - Term: Irritable Bowel Syndrome - ID: D000013577 - Term: Syndrome - ID: D000015746 - Term: Abdominal Pain - ID: D000064806 - Term: Dysbiosis ### Intervention Browse Module - Ancestors - ID: D000000975 - Term: Antioxidants - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000020011 - Term: Protective Agents - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: HB - Name: Herbal and Botanical - Abbrev: Ot - Name: Other Dietary Supplements ### Intervention Browse Module - Browse Leaves - ID: M342247 - Name: Turmeric extract - Relevance: HIGH - As Found: Urodynamic study - ID: M4292 - Name: Antioxidants - Relevance: LOW - As Found: Unknown - ID: M21869 - Name: Protective Agents - Relevance: LOW - As Found: Unknown - ID: T319 - Name: Turmeric - Relevance: HIGH - As Found: Urodynamic study - ID: T198 - Name: Indian Frankincense - Relevance: HIGH - As Found: Coxsackievirus - ID: T404 - Name: Lecithin - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: C000012596 - Term: Turmeric extract ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423573 Acronym: FOSteR Brief Title: A Study to Assess the Incidence of Skin Cancers in Patients With Epidermolysis Bullosa Receiving Filsuvez Official Title: A Long-term Non-interventional Study to Assess the Incidence of Skin Malignancies in Patients With Dystrophic and Junctional Epidermolysis Bullosa Receiving Treatment With Filsuvez #### Organization Study ID Info ID: AEB-21 #### Organization Class: INDUSTRY Full Name: Amryt Pharma ### Status Module #### Completion Date Date: 2032-08-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2031-11-30 Type: ESTIMATED #### Start Date Date: 2024-11-30 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: INDUSTRY Name: Chiesi Farmaceutici S.p.A. #### Lead Sponsor Class: INDUSTRY Name: Amryt Pharma #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: In patients with epidermolysis bullosa (EB), collagen does not form properly, so their skin is very fragile and blisters easily. Such patients are also at greatly increased risk of developing skin cancers. Filsuvez is a topical gel used to promote healing of skin lesions in patients with certain types of EB. In this observational study, patients with either dystrophic EB (DEB) or junctional EB (JEB) will receive standard of care treatment, whether Filsuvez or something else, and will be followed for up to 5 years. The main purpose is to see if the use of Filsuvez affects the likelihood of developing skin malignancies in these patient populations. Detailed Description: Some forms of EB are associated with a greatly increased incidence of aggressive skin and mucosal squamous cell carcinoma (SCC), as well as increased incidence of other skin malignancies including basal cell carcinoma (BCC) and malignant melanoma (MM). This long-term non-interventional study will assess all types of skin malignancies (SCC, BCC, and MM) in DEB and JEB patients. It is an observational study of real-world treatment practices, in which patients will receive standard of care therapy whatever that may entail. Data will be obtained from two sources: clinical study centers in the European Union (EU) and the United Kingdom (UK), and pre-existing EB registries in the EU. Participants will be followed for up to 5 years, and information about the development and nature of skin malignancies will be collected over this time period both from patients who are taking and those who are not taking Filsuvez. ### Conditions Module Conditions: - Epidermolysis Bullosa, Dystrophic - Epidermolysis Bullosa, Junctional Keywords: - Filsuvez - Birch bark extract ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 580 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients in this cohort will be receiving treatment with Filsuvez for their EB. Intervention Names: - Drug: Filsuvez Label: Patients with dystrophic or junctional EB being treated with Filsuvez #### Arm Group 2 Description: Patients in this cohort will be receiving treatment other than Filsuvez or no treatment at all for their EB. Label: Patients with dystrophic or junctional EB not being treated with Filsuvez ### Interventions #### Intervention 1 Arm Group Labels: - Patients with dystrophic or junctional EB being treated with Filsuvez Description: Topical gel Name: Filsuvez Other Names: - Birch bark extract Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Patients being treated with Filsuvez will be followed for occurrence of skin malignancies from the date of study enrolment until either the date of discontinuation (withdrawal of consent, withdrawal from the site or registry, physician decision, death, or lost to follow-up) or termination of the study Measure: Incidence of first skin malignancy during follow-up in EB patients receiving Filsuvez Time Frame: Up to 5 years #### Secondary Outcomes Description: Patients with EB who are not being treated with Filsuvez will be followed for occurrence of skin malignancies from the date of study enrolment until either the date of discontinuation (withdrawal of consent, withdrawal from the site or registry, physician decision, death, or lost to follow-up) or termination of the study Measure: Incidence of first skin malignancy during follow-up in EB patients not receiving Filsuvez Time Frame: Up to 5 years ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Patients with a confirmed diagnosis of dystrophic EB or junctional EB Exclusion Criteria: * None Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT Study Population: Patients with dystrophic EB or junctional EB, whether they are receiving Filsuvez, receiving another treatment for EB, or not receiving any treatment. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Chiesi Clinical Trials Phone: +3905212791 Role: CONTACT ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012868 - Term: Skin Abnormalities - ID: D000000013 - Term: Congenital Abnormalities - ID: D000012873 - Term: Skin Diseases, Genetic - ID: D000030342 - Term: Genetic Diseases, Inborn - ID: D000012871 - Term: Skin Diseases - ID: D000012872 - Term: Skin Diseases, Vesiculobullous - ID: D000003095 - Term: Collagen Diseases - ID: D000003240 - Term: Connective Tissue Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC16 - Name: Diseases and Abnormalities at or Before Birth - Abbrev: BC17 - Name: Skin and Connective Tissue Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC05 - Name: Musculoskeletal Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M7976 - Name: Epidermolysis Bullosa - Relevance: HIGH - As Found: Epidermolysis Bullosa - ID: M18587 - Name: Epidermolysis Bullosa, Junctional - Relevance: HIGH - As Found: Epidermolysis Bullosa, Junctional - ID: M15681 - Name: Skin Neoplasms - Relevance: LOW - As Found: Unknown - ID: M18586 - Name: Epidermolysis Bullosa Dystrophica - Relevance: HIGH - As Found: Epidermolysis Bullosa, Dystrophic - ID: M12 - Name: Congenital Abnormalities - Relevance: LOW - As Found: Unknown - ID: M15672 - Name: Skin Abnormalities - Relevance: LOW - As Found: Unknown - ID: M15674 - Name: Skin Diseases - Relevance: LOW - As Found: Unknown - ID: M15676 - Name: Skin Diseases, Genetic - Relevance: LOW - As Found: Unknown - ID: M23686 - Name: Genetic Diseases, Inborn - Relevance: LOW - As Found: Unknown - ID: M15675 - Name: Skin Diseases, Vesiculobullous - Relevance: LOW - As Found: Unknown - ID: M15045 - Name: Rheumatic Diseases - Relevance: LOW - As Found: Unknown - ID: M6323 - Name: Collagen Diseases - Relevance: LOW - As Found: Unknown - ID: M6464 - Name: Connective Tissue Diseases - Relevance: LOW - As Found: Unknown - ID: T2098 - Name: Epidermolysis Bullosa - Relevance: HIGH - As Found: Epidermolysis Bullosa - ID: T3164 - Name: Junctional Epidermolysis Bullosa - Relevance: HIGH - As Found: Epidermolysis Bullosa, Junctional - ID: T1991 - Name: Dystrophic Epidermolysis Bullosa - Relevance: HIGH - As Found: Epidermolysis Bullosa, Dystrophic ### Condition Browse Module - Meshes - ID: D000004820 - Term: Epidermolysis Bullosa - ID: D000016109 - Term: Epidermolysis Bullosa, Junctional - ID: D000016108 - Term: Epidermolysis Bullosa Dystrophica ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423560 Acronym: SPIFFERO Brief Title: Pulmonary Fibrosis After Severe COVID-19 Pneumonia Official Title: Evaluation of Pulmonary Fibrosis After Severe Interstitial Pneumonia Due to COVID-19 (SARS-CoV-2) #### Organization Study ID Info ID: CET 145-2024 #### Organization Class: OTHER Full Name: IRCCS San Raffaele ### Status Module #### Completion Date Date: 2024-05-16 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: COMPLETED #### Primary Completion Date Date: 2022-03-01 Type: ACTUAL #### Start Date Date: 2020-03-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: IRCCS San Raffaele #### Responsible Party Investigator Affiliation: IRCCS San Raffaele Investigator Full Name: Gabriele Fragasso Investigator Title: Principal Investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: Patients discharged after hospitalization for COVID-19 pneumonia were retrospectively selected by radiologically established criteria that at admission presented at chest computed tomography (CT) (i) normal lung parenchyma \<50% of total lung volume; and/or (ii) area of lung consolidation \> 10%. All At discharge and after 9 months, all subjects underwent cardiological evaluation, echocardiogram, pulmonary function tests (PFT) both atby 3 and by 12 months after discharge. Chest CT was performed by 12 months after discharge and chest CT. Specifically, the magnitude of pulmonary involvement between baseline and follow-up was considered the primary endpoint of this study. Secondary endpoints of the study were results of respiratory function testing, echocardiographic parametersparameters, and persistence of symptoms. ### Conditions Module Conditions: - Pulmonary Fibrosis - COVID-19 Keywords: - COVID-19 - Pulmonary fibrosis - ARDS - Computed tomography - pulmonary function test ### Design Module #### Design Info Observational Model: CASE_CONTROL Time Perspective: RETROSPECTIVE #### Enrollment Info Count: 61 Type: ACTUAL Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Radiation: Computed tomography Label: Residual disease > 20% of the total lung volume was considered pathological at follow-up CT #### Arm Group 2 Intervention Names: - Radiation: Computed tomography Label: Residual disease < 20% of the total lung volume was considered pathological at follow-up CT ### Interventions #### Intervention 1 Arm Group Labels: - Residual disease < 20% of the total lung volume was considered pathological at follow-up CT - Residual disease > 20% of the total lung volume was considered pathological at follow-up CT Description: Follow-up computed tomography at 3-6 months and 12 months Name: Computed tomography Other Names: - Pulmonary function test - Echocardiography Type: RADIATION ### Outcomes Module #### Primary Outcomes Measure: The magnitude of pulmonary involvement Time Frame: 12 months #### Secondary Outcomes Measure: results of respiratory function testing Time Frame: 12 months Measure: echocardiographic parameters Time Frame: 12 months Measure: persistence of symptoms Time Frame: 12 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age ≥ 18 * Hospitalization for severe COVID-19 pneumonia * Computed tomography during index hospitalization that showed: (i) normale lung parenchyma \< 50% of total lung volume and/or (ii) parenchymal consolidation \> 10% * Cardiological and pneumological visit, echocardiography and pulmonary function test at 3 and 12 months from hospital discharge * Computed tomography by 12 months from hospital discharge Exclusion Criteria: * Age \< 18 * Absence of previously cited test. Minimum Age: 18 Years Sampling Method: PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Patients hospitalized for sever COVID-19 pneumonia and successively discharge and with a 1-year follow-up ### Contacts Locations Module #### Locations Location 1: City: Milano Country: Italy Facility: IRCCS San Raffaele State: Lombardia Zip: 20132 #### Overall Officials Official 1: Affiliation: IRCCS San Raffaele Name: Gabriele Fragasso, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011024 - Term: Pneumonia, Viral - ID: D000012141 - Term: Respiratory Tract Infections - ID: D000007239 - Term: Infections - ID: D000014777 - Term: Virus Diseases - ID: D000018352 - Term: Coronavirus Infections - ID: D000003333 - Term: Coronaviridae Infections - ID: D000030341 - Term: Nidovirales Infections - ID: D000012327 - Term: RNA Virus Infections - ID: D000008171 - Term: Lung Diseases - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000010335 - Term: Pathologic Processes - ID: D000017563 - Term: Lung Diseases, Interstitial ### Condition Browse Module - Browse Branches - Abbrev: BC01 - Name: Infections - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M2561 - Name: COVID-19 - Relevance: HIGH - As Found: COVID-19 - ID: M8485 - Name: Fibrosis - Relevance: HIGH - As Found: Fibrosis - ID: M14512 - Name: Pulmonary Fibrosis - Relevance: HIGH - As Found: Pulmonary Fibrosis - ID: M13904 - Name: Pneumonia - Relevance: HIGH - As Found: Pneumonia - ID: M13914 - Name: Pneumonia, Viral - Relevance: LOW - As Found: Unknown - ID: M10283 - Name: Infections - Relevance: LOW - As Found: Unknown - ID: M6368 - Name: Communicable Diseases - Relevance: LOW - As Found: Unknown - ID: M14978 - Name: Respiratory Tract Infections - Relevance: LOW - As Found: Unknown - ID: M17522 - Name: Virus Diseases - Relevance: LOW - As Found: Unknown - ID: M20490 - Name: Coronavirus Infections - Relevance: LOW - As Found: Unknown - ID: M6555 - Name: Coronaviridae Infections - Relevance: LOW - As Found: Unknown - ID: M23685 - Name: Nidovirales Infections - Relevance: LOW - As Found: Unknown - ID: M15149 - Name: RNA Virus Infections - Relevance: LOW - As Found: Unknown - ID: M11168 - Name: Lung Diseases - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: M19813 - Name: Lung Diseases, Interstitial - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000086382 - Term: COVID-19 - ID: D000011014 - Term: Pneumonia - ID: D000011658 - Term: Pulmonary Fibrosis - ID: D000005355 - Term: Fibrosis ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423547 Brief Title: Risk Warning Model of Postoperative Delirium and Long-term Cognitive Dysfunction in Elderly Patients Official Title: Risk Warning Model of Postoperative Delirium and Long-term Cognitive Dysfunction in Elderly Patients Based on Autonomous Evolutionary Neural Network Algorithm #### Organization Study ID Info ID: 62376168 #### Organization Class: OTHER Full Name: Xuanwu Hospital, Beijing ### Status Module #### Completion Date Date: 2027-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-30 Type: ACTUAL Last Update Submit Date: 2024-05-29 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2027-12-31 Type: ESTIMATED #### Start Date Date: 2024-06-15 Type: ESTIMATED Status Verified Date: 2024-03 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: UNKNOWN Name: Chongqing Institute of Green and Intelligent Technology, Chinese Academy of Sciences #### Lead Sponsor Class: OTHER Name: Xuanwu Hospital, Beijing #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: The incidence of postoperative delirium in elderly patients is high, which can lead to long-term postoperative neurocognitive disorders. Its high risk factors are not yet clear. At present, there is a lack of early diagnosis and alarm technology for perioperative neurocognitive disorders, which can not achieve early intervention and effective treatment. By artificial intelligence and autonomously evolutionary neural network algorithm, relying on multi-source clinical big data, we explored the use of Bayesian network to optimize the anesthesia decision-making system in enhanced recovery after surgery, and established risk prediction model for perioperative critical events. It is expected that this method will also help to establish a risk prediction model for postoperative delirium and long-term postoperative neurocognitive disorders. This project plans to collect the perioperative sensitive parameters of anesthesia machine, multi-parameter monitor, EEG monitor,fMRI and HIS system, to explore the evolution process of data characteristics by feature fusion.We also plan to quickly screen key perioperative risk characteristics of postoperative delirium from massive clinical data through feature selection, to explore the high risk factors of long-term postoperative neurocognitive disorders developing from postoperative delirium. Finally, with multi-center intelligent analysis，the risk prediction model of postoperative delirium and long-term postoperative neurocognitive disorders will be constructed. Detailed Description: This project intends to collect and identify clinical monitoring data of anesthesia machine, multi-parameter monitor and brain function monitor on the basis of the team's previous series of studies on cognitive function protection of elderly patients in perioperative period and the research on tracking and warning of critical illness events and decision support services based on artificial intelligence. HIS clinical data and classified and tracked fMRI imaging data were integrated to form a large data set related to perioperative cognitive function of elderly patients. Based on pNCD clinical diagnostic information and fMRI imaging diagnostic information, a brain adverse event prediction system capable of intelligent extraction of clinical key information and real-time early warning was established by using key technologies such as data quality control, real-time collection and identification of multi-source clinical monitoring data, and artificial intelligence adverse event prediction. ### Conditions Module Conditions: - Postoperative Delirium - Postoperative Neurocognitive Disorder - Surgery Keywords: - postoperative delirium; - postoperative neurocognitive disorder; - risk prediction model; - artificial intelligence; - evolutionary neural network ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 10000 Type: ESTIMATED Patient Registry: True Study Type: OBSERVATIONAL Target Duration: 1 Year ### Arms Interventions Module #### Arm Group 1 Description: Delirium (CAM scale ) was assessed 7 days after surgery and divided into POD and non-POD groups; one of the above scenarios indicated postoperative delirium;The patients in the POD group were evaluated for cognitive function at 1 month and 12 months after surgery to determine whether pNCD occurred. The patients in the POD group were further divided into pNCD subgroup and non-PNCD subgroup, and EEG data collection and fMRI scanning were performed Intervention Names: - Other: no intervention Label: postoperative delirium(POD) and postoperative neurocognitive disorder(pNCD) ### Interventions #### Intervention 1 Arm Group Labels: - postoperative delirium(POD) and postoperative neurocognitive disorder(pNCD) Description: this is an observation study,no intervention Name: no intervention Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The feature selection technique in artificial intelligence was used to screen and analyze data from a large dataset of clinical care after fusion The risk factors with the highest probability of PND occurrence can be screened from a large number of characteristics,By screening the risk factors that have the highest correlation with the probability of POD occurrence, combined with the comparison of fMRI imaging data of different groups of large sample size POD patients with long-term conversion to pNCD group and non-PNCD group, the brain network mechanism and perioperative high risk factors of POD conversion to long-term cognitive dysfunction were further explored. Measure: Screening for risk factors of perioperative cognitive dysfunction Time Frame: 2024.4.1-2027.12.31 Description: The monitoring data of surgical patients contains a large amount of medical information, and the analysis and modeling of the data can provide effective early warning and intervention. The project intends to adopt EEG time-frequency feature extraction and analysis, EEG micro-state analysis, and brain network analysis, and adopt feature fusion technology to fuse various features into unified features of patients. On this basis, a prediction model of adverse brain function events based on domain adaptation algorithm was constructed to realize real-time tracking, early diagnosis and early warning of postoperative delirium and long-term cognitive dysfunction in elderly patients Measure: Establish a prediction system for adverse brain function events Time Frame: 2025.1.1-2027.12.31 ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Patients ≥65 years of age who have undergone surgical anesthesia; Sign informed consent Exclusion Criteria: * Inability to complete cognitive function assessment; Illiteracy, hearing impairment or visual impairment; He has a history of epilepsy, depression, schizophrenia, Alzheimer's disease and other psychiatric and neurological diseases Maximum Age: 100 Years Minimum Age: 65 Years Sampling Method: PROBABILITY_SAMPLE Sex: ALL Standard Ages: - OLDER_ADULT Study Population: Patients 65\~100 years of age who have undergone surgical anesthesia ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: lei zhao Phone: +8613811035886 Role: CONTACT Contact 2: Email: [email protected] Name: xia li li Phone: +86818810616341 Role: CONTACT #### Overall Officials Official 1: Affiliation: xuanwu hospital of capital medical university,Beijing Name: lei zhao Role: STUDY_CHAIR Official 2: Affiliation: Chongqing Institute of Green and Intelligent Technology, Chinese Academy of Sciences Name: yong yang Role: PRINCIPAL_INVESTIGATOR Official 3: Affiliation: xuanwu hospital of capital medical university,Beijing Name: yi an Role: PRINCIPAL_INVESTIGATOR Official 4: Affiliation: xuanwu hospital of capital medical university,Beijing Name: xia li li Role: PRINCIPAL_INVESTIGATOR Official 5: Affiliation: xuanwu hospital of capital medical university,Beijing Name: yang liu Role: PRINCIPAL_INVESTIGATOR Official 6: Affiliation: xuanwu hospital of capital medical university,Beijing Name: yi shu yang Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ### References Module #### References Citation: Patel A, Zhang M, Liao G, Karkache W, Montroy J, Fergusson DA, Khadaroo RG, Tran DTT, McIsaac DI, Lalu MM. A Systematic Review and Meta-analysis Examining the Impact of Age on Perioperative Inflammatory Biomarkers. Anesth Analg. 2022 Apr 1;134(4):751-764. doi: 10.1213/ANE.0000000000005832. PMID: 34962902 Citation: An Y, Zhao L, Wang T, Huang J, Xiao W, Wang P, Li L, Li Z, Chen X. Preemptive oxycodone is superior to equal dose of sufentanil to reduce visceral pain and inflammatory markers after surgery: a randomized controlled trail. BMC Anesthesiol. 2019 Jun 11;19(1):96. doi: 10.1186/s12871-019-0775-x. PMID: 31185942 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000003221 - Term: Confusion - ID: D000019954 - Term: Neurobehavioral Manifestations - ID: D000009461 - Term: Neurologic Manifestations - ID: D000009422 - Term: Nervous System Diseases - ID: D000001523 - Term: Mental Disorders - ID: D000003072 - Term: Cognition Disorders - ID: D000011183 - Term: Postoperative Complications - ID: D000010335 - Term: Pathologic Processes ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M29705 - Name: Cognitive Dysfunction - Relevance: HIGH - As Found: Cognitive Dysfunction - ID: M6894 - Name: Delirium - Relevance: HIGH - As Found: Delirium - ID: M21836 - Name: Neurocognitive Disorders - Relevance: HIGH - As Found: Neurocognitive Disorders - ID: M772 - Name: Emergence Delirium - Relevance: HIGH - As Found: Postoperative Delirium - ID: M6446 - Name: Confusion - Relevance: LOW - As Found: Unknown - ID: M21826 - Name: Neurobehavioral Manifestations - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: M4815 - Name: Mental Disorders - Relevance: LOW - As Found: Unknown - ID: M14473 - Name: Psychotic Disorders - Relevance: LOW - As Found: Unknown - ID: M6301 - Name: Cognition Disorders - Relevance: LOW - As Found: Unknown - ID: M14065 - Name: Postoperative Complications - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003693 - Term: Delirium - ID: D000071257 - Term: Emergence Delirium - ID: D000060825 - Term: Cognitive Dysfunction - ID: D000019965 - Term: Neurocognitive Disorders ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423534 Brief Title: Empowering New Mothers: Exploring the Effect of Breastfeeding Health Educational Program on Practices and Feeding Self-Efficacy of Primigravida in Saudi Arabia Official Title: Empowering New Mothers: Exploring the Effect of Breastfeeding Health Educational Program on Practices and Feeding Self-Efficacy of Primigravida in Saudi Arabia #### Organization Study ID Info ID: H-2024-126 #### Organization Class: OTHER Full Name: Alexandria University ### Status Module #### Completion Date Date: 2024-08-10 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-07-15 Type: ESTIMATED #### Start Date Date: 2024-03-20 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Alexandria University #### Responsible Party Investigator Affiliation: Alexandria University Investigator Full Name: Mahmoud Khedr Investigator Title: Lecturer Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: Being pregnant causes a mother and her child to form a maternal tie, and the birth of the child fills the mother with an immense amount of love and happiness. Breastfeeding is how a mother and infant make their initial touch. Breastfeeding is a mother's priceless gift to her infant and nature's own method of nurturing a baby. Detailed Description: This study will be done to evaluate the primigravida mother's breastfeeding's knowledge, attitude and corrective technique through the implementation of an educational program and to ascertain the efficacy of such a program. ### Conditions Module Conditions: - Primigravida Women ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: SUPPORTIVE_CARE #### Enrollment Info Count: 70 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Each primigravida in the study group during the last three trimesters will receive three sessions of knowledge, breast care, and breastfeeding technique after filling out a questionnaire (pretest). During 1 month from delivery, we will conduct a post-test with them (after 2 weeks and after 4 weeks) to explore the effect of breastfeeding health educational programs on practices and breastfeeding self-efficacy Intervention Names: - Behavioral: Breastfeeding Health Educational Program Label: Study GROUP Type: EXPERIMENTAL #### Arm Group 2 Description: The control group was selected first and received a brochure leaflet delivered by the researcher. They didn't receive the health educational program Intervention Names: - Behavioral: Breastfeeding Health Educational Program Label: Control group Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Control group - Study GROUP Description: Breastfeeding is a mother's priceless gift to her infant and nature's own method of nurturing a baby. Therefore, this study will be conducted to evaluate the primigravida mother's breastfeeding's knowledge, attitude and corrective technique through the implementation of an educational program and to ascertain the efficacy of such a program. Name: Breastfeeding Health Educational Program Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: It was developed by Tella et al. (2016) and comprised 12 questions that were assessed in various areas under various breastfeeding techniques practice. Measure: A preformatted structured questionnaire Time Frame: 3 months Description: It was adopted (Dennis, 2003) that assess maternal self-efficacy for breastfeeding throughout all stages of the study. The BSES-SF is a Likert scale with 14 items organized into two domains, namely: technical and intrapersonal thoughts. Measure: Self-Efficacy Scale - Short-Form (BSES-SF) Time Frame: 3 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Primigravida mothers who regularly visit maternity hospitals at Hail and Bisha City. * Primigravida mothers during last three trimester and 1 month after delivery * No problems during pregnant and have a healthy baby * Primigravida mothers who are not contraindicated to breastfeeding Exclusion Criteria: * Multigravida mothers and pregnant women during first and second trimester Maximum Age: 45 Years Minimum Age: 17 Years Sex: FEMALE Standard Ages: - CHILD - ADULT ### Contacts Locations Module #### Locations Location 1: City: Hail Contacts: *Contact 1:* - Email: [email protected] - Name: Asmaa Ali - Phone: 543132470 - Role: CONTACT Country: Saudi Arabia Facility: Faculty of Nursing, Hail university Status: RECRUITING ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423521 Acronym: VAPUST Brief Title: Value Analysis in Patients Undergoing Self-Management Training Using a Coagulometer Official Title: Value Analysis in Patients Undergoing Anticoagulant Therapy: Impact of Self-management Training Using a Coagulometer #### Organization Study ID Info ID: 1057/2021 #### Organization Class: OTHER Full Name: Value for Health CoLAB ### Status Module #### Completion Date Date: 2024-04-01 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: COMPLETED #### Primary Completion Date Date: 2024-04-01 Type: ACTUAL #### Start Date Date: 2021-10-10 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: NOVA Medical School Class: INDUSTRY Name: Roche Diagnostics GmbH #### Lead Sponsor Class: OTHER Name: Ana Rita Londral, PhD #### Responsible Party Investigator Affiliation: Value for Health CoLAB Investigator Full Name: Ana Rita Londral, PhD Investigator Title: MSc Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: Prior research has not assessed the value of remote patient monitoring (RPM) systems for patients undergoing anticoagulation therapy after cardiac surgery. This study aims to assess whether the clinical follow-up through RPM yields comparable outcomes with the standard protocol. A crossover trial assigned participants to SOC-RPM or RPM-SOC, starting with the standard of care (SOC) for the first 6 months after surgery and using RPM for the following 6 months, or vice-versa, respectively. During RPM, patients used the Coaguchek© to accurately measure International Normalized Ratio values and a mobile text-based chatbot to report PROs and adjust the therapeutic dosage. The study assessed patients' and clinicians' experience with RPM and compared direct costs. Detailed Description: The main objective of this pilot study was to evaluate the outcomes and costs of a digital clinical service to support patients with anticoagulant therapy after cardiac surgery. This study used an RPM-based system with a portable coagulometer for clinical follow-up and self-management of INR control and compared with the standard of care (SOC). In addition, this study seeks to assess patients' and clinical teams' satisfaction and experience. Patients were recruited in sequential order based on their availability in the cardiothoracic surgery department. The participants were assigned into two arms: one would follow the SOC for the first six months and then receive the RPM intervention for the following six months (SOC-RPM); the other group would receive the intervention (RPM) for the first six months and then follow the SOC for the remaining six months (RPM-SOC). Blinding was not feasible due to the nature of the trial, and both patients and the clinical team were aware of the follow-up being conducted. In this study, it was decided that a washout period was not required. This was because withdrawing effective follow-up care for a washout period is not possible, as patients need to be constantly monitored to ensure effective treatment, thus preventing thromboembolic events. The study was conducted for twelve months, as follows: 1. Patients received a kit with a Coagulometer-CoaguChek® (Roche Diagnostics, Switzerland) and the necessary test strips for use during the period established, as well as written instructions on how to take the measurements, and were registered on the monitoring platform. 2. Patients received periodic text messages on their smartphones to report the INR value, and they responded to messages regarding their symptoms related to anticoagulant therapy and the INR value. 3. The clinical team received notifications if patients' reports had been assessed outside therapeutic standards and then sent a text message back with the medication adjustment. ### Conditions Module Conditions: - Post-Cardiac Surgery Patients Keywords: - Digital healthcare - Telemedice - Remote Patient Monitoring - Antocoagulation Therapy ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: CROSSOVER ##### Masking Info Masking: NONE Primary Purpose: HEALTH_SERVICES_RESEARCH #### Enrollment Info Count: 28 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: SOC-RPM arm, would follow the Standard of Care (SOC) for the first six months and then receive the Remote Patient Monitoring (RPM). Intervention Names: - Other: Standard of Care (SOC) Label: SOC-RPM Type: EXPERIMENTAL #### Arm Group 2 Description: RPM-SOC arm: would receive the intervention (RPM) for the first six months and then follow the SOC for the remaining six months. Intervention Names: - Other: Remote Patient Monitoring (RPM) Label: RPM-SOC Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - SOC-RPM Description: The SOC intervention constitutes the common clinical practice of care that is habitually performed after cardiac surgery to manage anticoagulation therapies. Name: Standard of Care (SOC) Type: OTHER #### Intervention 2 Arm Group Labels: - RPM-SOC Description: The RPM intervention involves the use of a remote patient monitoring (RPM) system with a portable coagulometer for the clinical follow-up and self-management of International Normalized Ratio (INR) control in patients undergoing anticoagulant therapy post-cardiac surgery. Patients were provided with a Coagulometer-CoaguChek® (Roche Diagnostics, Switzerland) kit and test strips, along with written instructions for conducting measurements. They were also enrolled in a monitoring platform. Patients received regular text messages on their smartphones to report their INR values and symptoms related to anticoagulant therapy. The clinical team received notifications if patients\&#39; reports fell outside therapeutic standards and then responded with medication adjustments via text message. Name: Remote Patient Monitoring (RPM) Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The primary endpoint was the patient's TTR for INR values among the programs, i.e., a comparison between SOC and RPM over time. The TTR for INR value was self-measured by the portable monitor and calculated by the Rosendaal method of lineal interpolation Measure: Time in Therapeutic Range (TTR) for International Normalized Ratio (INR) Time Frame: From enrollment to the end of treatment at 12 months #### Secondary Outcomes Description: Zero is equivalent to no hypoagulation symptoms and more than one indicates a symptom Measure: Number of events of hypocoagulation symptoms Time Frame: From enrollment to the end of treatment at 12 months Description: . A questionnaire with 13 self-reported questions was used to evaluate patient experience and satisfaction. The first four questions measured experience, while the following nine focused on satisfaction. The responses were rated on a scale of disagree to agree, with 1-4 points assigned to each response. To prevent ceiling and floor effects in our tool, the questions numbered '2', '11', and '12' were calculated as "inverted," and an optional open question was included. The questionnaire used to assess experience and satisfaction is not validated, precluding external validity. Still, it was used due to the lack of instruments in Portuguese language to assess the experience and satisfaction of digital health RPM-based systems. Measure: Patient Experience and Satisfaction Time Frame: From enrollment to the end of treatment at 12 months Description: The method used in the trial compared the average cost per patient in standard of care (SOC) versus remote patient monitoring (RPM) using the Time-Driven Activity-Based Costing (TDABC) method from the perspective of the Public National Healthcare Service (NHS). The method involved mapping patient pathway activities and identifying direct costs such as healthcare professionals, facilities, equipment and technology, and consumables. Costs for healthcare professionals, equipment and technology, and facilities were determined based on market value, depreciation rate, and public salary scale. Travel costs for patients undergoing SOC were considered, and all monetary values are in Euros as of 2023. Measure: Costs Time Frame: From enrollment to the end of treatment at 12 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * equal or more than 18 years old and with a smartphone Exclusion Criteria: * analphabetism, poor health, low digital literacy level and inability to use the RPM alone or with caregiver support Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Lisboa Country: Portugal Facility: Hospital de Santa Marta Zip: 1169-024 #### Overall Officials Official 1: Affiliation: Value for Health CoLAB Name: Ana Rita Londral, PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ### References Module #### References Citation: Sharma P, Scotland G, Cruickshank M, Tassie E, Fraser C, Burton C, Croal B, Ramsay CR, Brazzelli M. Is self-monitoring an effective option for people receiving long-term vitamin K antagonist therapy? A systematic review and economic evaluation. BMJ Open. 2015 Jun 25;5(6):e007758. doi: 10.1136/bmjopen-2015-007758. PMID: 26112222 Citation: Menendez-Jandula B, Garcia-Erce JA, Zazo C, Larrad-Mur L. Long-term effectiveness and safety of self-management of oral anticoagulants in real-world settings. BMC Cardiovasc Disord. 2019 Aug 2;19(1):186. doi: 10.1186/s12872-019-1168-2. Erratum In: BMC Cardiovasc Disord. 2019 Nov 26;19(1):263. PMID: 31375070 Citation: Azevedo S, Guede-Fernandez F, von Hafe F, Dias P, Lopes I, Cardoso N, Coelho P, Santos J, Fragata J, Vital C, Semedo H, Gualdino A, Londral A. Scaling-up digital follow-up care services: collaborative development and implementation of Remote Patient Monitoring pilot initiatives to increase access to follow-up care. Front Digit Health. 2022 Dec 7;4:1006447. doi: 10.3389/fdgth.2022.1006447. eCollection 2022. PMID: 36569802 Citation: Wu Y, Wang X, Zhou M, Huang Z, Liu L, Cong L. Application of eHealth Tools in Anticoagulation Management After Cardiac Valve Replacement: Scoping Review Coupled With Bibliometric Analysis. JMIR Mhealth Uhealth. 2024 Jan 5;12:e48716. doi: 10.2196/48716. PMID: 38180783 Citation: Huang Y, Xie Y, Huang L, Han Z. The Value of Anticoagulation Management Combining Telemedicine and Self-Testing in Cardiovascular Diseases: A Meta-Analysis of Randomized Controlled Trials. Ther Clin Risk Manag. 2023 Mar 14;19:279-290. doi: 10.2147/TCRM.S395578. eCollection 2023. PMID: 36941980 ## Derived Section ### Intervention Browse Module - Browse Branches - Abbrev: AnCoag - Name: Anticoagulants - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M4244 - Name: Anticoagulants - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423508 Acronym: PROTEGI Brief Title: PRObing The Efficacy of Commercial Stage Storage Buffers and Evaluating Gut Metaproteome Variability Between Individuals Official Title: PRObing The Efficacy of Commercial Stage Storage Buffers and Evaluating Gut Metaproteome Variability Between Individuals #### Organization Study ID Info ID: EK_01149_3/05/2024 #### Organization Class: OTHER Full Name: University of Vienna ### Status Module #### Completion Date Date: 2025-09-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-12-30 Type: ESTIMATED #### Start Date Date: 2024-06-03 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: University of Vienna #### Responsible Party Investigator Affiliation: University of Vienna Investigator Full Name: Giacomo Carta Investigator Title: Postdoc Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The study aims to assess the effectiveness of various commercial and non-hazardous buffers for the storage of human gut fecal samples over time. This evaluation will be conducted by comparing the performance of these buffers against directly frozen samples using metaproteomic analysis. The study is motivated by the need for standardized protocols for sample preservation in metaproteomic research, particularly focusing on protein preservation in fecal samples. By investigating proteomic, taxonomic, and functional identifications, the research seeks to provide insights into the reliability of these buffers as storage solutions. Additionally, the study plans to explore inter- and intra-individual variabilities at the proteome level by periodically collecting fecal samples from volunteers, complementing existing knowledge in metaproteomics. Overall, the study addresses a critical gap in the field and has the potential to enhance reproducibility and comparability across metaproteomic studies Detailed Description: A. Introduction: Metaproteomics studies the entire protein complement of a microbial community and offers insight into intricate ecosystems like the gut microbiome. Metaproteomics allows researchers to delve deep into gut microbiomes, providing insights into these microbial inhabitants, abundance and functional activities. This knowledge has been instrumental in elucidating the mechanisms underlying various diseases, such as inflammatory bowel disease, and obesity. Researchers can develop targeted strategies for personalized medicine and precision healthcare based on the underlying biology by identifying key protein signatures. In gut microbiome studies, standardized sample collection and preservation are particularly crucial to preserve the integrity of the microbial community and its proteome. Indeed, to obtain reliable results it must be considered the susceptibility to environmental influences like temperature and oxygen amount. For gut microbiome metaproteomic studies, non-invasive or minimally invasive methods are preferred to minimize disruption, or contamination, and preserve the native microbial composition and protein profiles. Also, the sample handling and storage strategies affect the degradation of proteins and the microbial population stability. For this reason, immediate freezing, or preservation at low temperatures (e.g., -80°C) is often recommended to maintain sample integrity until analysis. However, using a cold chain for storage and transportation is not compatible with an on-site sampling strategy that is necessary for large-scale and delocalized studies. Moreover, it is less ideal, more expensive, and logistically tedious than potential room temperature options. Furthermore, present knowledge of the fecal sample collection/preservation methods is based on preserving nucleic acids or metabolites during the transportation to the laboratory for analysis. However, protein preservation requires different strategies and studies are scarce and rely on adopting the devices or reagents used in the case of nucleic acids or metabolites analysis. Thus, tailored, and standardized protocols together with metadata collection are essential for ensuring reproducibility and comparability across metaproteomic studies. The present study aims to evaluate the fitness of several commercial and non-hazardous buffers for the storage of human gut fecal samples over time. Fecal samples will be stored in five different buffers and will be benchmarked with directly frozen samples. Using metaproteomics the investigators will compare the proteomic, taxonomic, and functional identifications to understand the potential of these buffers as a reliable storage solution for human feces. This research is unique and to the best of our knowledge, no similar study has addressed this demanding question. Preliminary evidence in humans has shown inter- and intra-individual variability of the proteomes of the host and microbiomes. In particular, the intra-individual taxonomic and functional variation in the gut microbiome seems to be lower than inter-individual variation over time. However, metatranscriptomics profiles exhibited comparable variability within and between subjects. Therefore, using metaproteomics, investigators aim to assess the inter- and intra-individual variabilities at the proteome level by studying fecal samples periodically collected from participants. B. The academic and social relevance: The first part of the study aims to define the most effective storage buffer for preserving protein integrity during sample transportation from the site of collection to the site of processing - a key factor in the future of metaproteomics applied to health and disease. Despite its importance, a similar evaluation has not been performed for proteomic applications. This knowledge will be critical for academic purposes to be used for large-scale human fecal proteomic studies. For people to have their gut health examined through metaproteomics and unlock the potential of microbial communities-based personalized medicine and therapeutic interventions there will be a requirement for consistent sample collection and this study will provide it. The second part of the study is designed to understand the variability that can be observed in the gut microbiome composition and functions from the proteomics perspective. The gut microbiome is dynamic and is known to be altered by multiple factors such as diet, age, genetics, environment, etc. These variations can be broadly classified into inter- and intra-individual. Inter-individual variability refers to the differences observed between individuals within a population or group, and they can encompass a wide range of characteristics, including genetic makeup, physiological parameters, lifestyle factors, and environmental exposures. Understanding inter-individual variability from people of the same "community" is essential in fields such as personalized medicine, where tailored interventions account for individual differences to optimize treatment outcomes. Intra-individual variability, on the other hand, refers to variations observed within the same individual over time or under different conditions and can arise from biological fluctuations, such as circadian rhythms, hormonal fluctuations, or physiological responses to stimuli. Recognizing and characterizing intra-individual variability is crucial for accurately interpreting research findings and assessing the reliability of biological measurements, particularly in longitudinal studies or clinical monitoring scenarios. This study aims to understand these variabilities through the proteomics data collected from participants' fecal samples and define the variables detected in the gut microbiome. C. Objectives: 1. To identify the effect of five different buffers used for the storage and transportation of collected human fecal material, by metaproteomic profiles. 2. To determine the variability in microbiota and host proteomes at the inter- and intra-individual levels. D. Study Design: For the first phase, the investigators will deploy the following protocol for on-site fecal sampling and transport preservation: The participants (recruited among the members of our laboratory/Division) will be provided with 18 tubes (numbered 1-18; 15 ml conical centrifuge tubes; Ref# 339650, Thermo Scientific and 18 easy-to-use commercial swabs (C1052-50, Zymo Research) or spatulas (DNAGenotek). The 18 tubes correspond to three storage time points of 6 different experimental conditions: an empty tube (without preservation liquid) as a control sample and 5 different non-hazardous fecal preservation liquids: (a) In-house buffer (called LB) with SDS and Urea, commercially obtained (b) Zymo DNA/RNA Shield (R1100, Zymo Research), (c) Copan Amies buffer (480CE, Copan Italia SpA), (d) OMNIgene•GUT (OM200, DNAGenotek), (e) OMNImet•GUT (ME200, DNAGenotek). Briefly, LB, Zymo Shield, and OM200 are known to contain detergents that help to preserve the biomolecules, Copan Amies buffer is a nutrient-free media known to keep the cells viable and shown to have applications in culturomics, and ME200 is solvent based useful in metabolomic applications. In addition, the participants will receive a commercial stool catcher that is displayed over the toilet for facilitating fecal sampling (Servoprax Stuhlfaenger, Reference number H7 61000-50 from www.medundorg.de) and a little box with ice packs in which the three Control samples will be stored and transported to the lab. These ice-stored Control samples are key to evaluating the performance of the different storage buffers. The participants will bring the samples to our laboratory in the following 24 hours. Upon reception in the lab, the Control samples will be stored at -80°C until further biochemical processing using established protocols. The rest of the samples will be stored at +20°C inside an orbital shaker incubator for a total of 2, 5, and 10 days (simulating different storage/transport times, thereof). At the end of these time points, the samples will be stored at -80°C until further biochemical processing using established protocols. The metaproteomic profiles (indicating the taxonomical and functional changes in the gut microbiome and the host physiology; as in the previous experiment from these samples will inform us about the best preservation liquid (defined as the one where the microbiome composition and function are more like the Control sample). This experiment is necessary for initiating Phase II of the study, and it is novel in the field as no guidelines are established for best in-house fecal sampling practices in metaproteomics. Six healthy participants (among the members of the Systems Biology of Pain laboratory, Division of Pharmacology \& Toxicology, Department of Pharmaceutical Sciences) will be recruited. This is a randomized study with no participant groups. Samples will be collected once and distributed to 18 tubes representing different conditions. A sample size of 6 subjects will be enough to find the best preservation solution and the sampling will be performed one time under normal bowel movement by the participants. In addition, the participants will fill out a questionnaire (attached) that includes information like age, sex, Body Mass Index, the gastrointestinal symptoms rating scale (GSRS), administration of antibiotics in the last 30 days before sample collection, the Bristol stool form scale (BSFS), and the approximate time needed for sample collection in the 18 tubes (to account for potential effects due to oxidation processes). For the second phase, the participants will be expected to collect fecal samples for 4 weeks during their regular defecation (ten different times maximum). They will be provided with an adequate number of 15ml conical centrifuge tubes (339650, Thermo Scientific) containing the best-performing preservation buffer (as defined in the first phase of the study, see above), and a commercial collection device with a stool catcher. Upon reception in the lab, the samples will be stored at -80°C until further biochemical processing using established protocols. In addition, the participants will fill out a questionnaire (see above). Participants will take part voluntarily in the experiment after receiving an explanation of all the risks and benefits of participating in the present study, and after signing the written informed consent form according to the Declaration of Helsinki (see the consent form, attached). The participants will be instructed and provided with necessary sampling devices to collect stool samples (see above) and submit the samples to the Department of Pharmacology and Toxicology at the earliest opportunity. Participants will be expected to complete self-administered questionnaires that include information like the one described above. For the second phase, 46 healthy participants (among the members of our laboratory/Division) will be recruited from both sexes (23 males and females) considering a possible dropout rate of 20%. This is a randomized study with no participant groups. The sample size was calculated based on the threshold of Eggerthella estimates with time. The statistics procedure used is F tests - two-way ANOVA with repeated measures with the following values Cohens'd = 0.75, 1-β= 0.80, and α= 0.05. A total of 400 - 460 samples are expected to be collected. ### Conditions Module Conditions: - Gut Microbiome - Buffer - Methodology Study - Fecal Microbiota - Variability Keywords: - storage buffer - fecal samples - human gut microbiome - metaproteomics - intra-individual variability - inter-individual variability ### Design Module #### Bio Spec Description: human fecal samples Retention: SAMPLES_WITH_DNA #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 52 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Identifying the most effective storage buffer for preserving protein integrity during the transportation of fecal samples from collection to processing sites, is essential for establishing consistent sample collection protocols, particularly for large-scale human fecal proteomic studies. Achieving consistency in sample collection is crucial for enabling individuals to have their gut health assessed via metaproteomics, unlocking the potential for personalized medicine and therapeutic interventions based on microbial communities. Label: storage buffer standardisation #### Arm Group 2 Description: the aim is to explore the inter- and intra-individual variability observed in gut microbiome composition and functions from a proteomic perspective. Understanding inter-individual variability differences is crucial for personalized medicine. Recognizing and characterizing intra-individual variability is essential for accurately interpreting research findings, particularly in longitudinal studies or clinical monitoring scenarios. This study aims to elucidate these variabilities using proteomic data from volunteers' fecal samples, shedding light on the variables detected in the gut microbiome and providing insights into its dynamic nature Label: inter- and intra-individual variability ### Outcomes Module #### Primary Outcomes Description: Eggerthella abundance will be checked in to the Metaproteomic profile of each fecal samples and inter/intra-individual variability will be assessed Measure: Eggerthella abundance Time Frame: From enrollment to the end of treatment at 4 weeks #### Secondary Outcomes Description: Age will be collected from each participant during the first interview Measure: Age Time Frame: From enrollment to the end of treatment at 4 weeks Description: Sex will be collected from each participant during the first interview Measure: Sex Time Frame: From enrollment to the end of treatment at 4 weeks Description: BMI will be collected from each participant during the first interview Measure: Body Mass Index (BMI) Time Frame: From enrollment to the end of treatment at 4 weeks Description: Antibiotic use in the previous 1 month before the study enrollment, will be collected from each participant during the first interview Measure: Antibiotic use Time Frame: From enrollment to the end of treatment at 4 weeks Description: The Bristol Stool Form Scale (BSFS), or Bristol stool scale, is a chart that can help classify stools into seven groups. Characterizing the stool based on its consistency can help identify if it is a healthy bowel movement. It will be administerd refearring to the the day(s) of the fecal sample collection(s) Measure: Bristrol Stool Form Scale (BSFS) Time Frame: From enrollment to the end of treatment at 4 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * agreeing to participate after signing the informed consent form and * being 18-70 years old. Exclusion Criteria: * take antibiotics during the previous 1 month * had undergone gastrointestinal surgery Healthy Volunteers: True Maximum Age: 70 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: healthy volunteers (among the members of our laboratory/Division) will be recruited ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: David Gomez Varela PhD. Senior Scientist, PhD Phone: 1427755361 Role: CONTACT Contact 2: Email: [email protected] Name: Ranjith Kumar Ravi Kumar PhD- postdoc, PhD Phone: 1427755318 Role: CONTACT #### Locations Location 1: City: Vienna Contacts: *Contact 1:* - Email: [email protected] - Name: David Gomez Varela, PhD - Phone: 1427755361 - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Ranjith Kumar Ravi Kumar, PhD - Phone: +43142-775-5318 - Role: CONTACT Country: Austria Facility: UVienna State: Wien Zip: 1090 #### Overall Officials Official 1: Affiliation: University of Vienna Name: Giacomo Carta, PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Description: anonymized data will be provided under scientific plausible request sent by email to the principal investigator IPD Sharing: NO ### References Module #### References Citation: Gomez-Varela D, Xian F, Grundtner S, Sondermann JR, Carta G, Schmidt M. Increasing taxonomic and functional characterization of host-microbiome interactions by DIA-PASEF metaproteomics. Front Microbiol. 2023 Oct 16;14:1258703. doi: 10.3389/fmicb.2023.1258703. eCollection 2023. PMID: 37908546 ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423495 Brief Title: Efficacy of Photobiomodulation in the Rehabilitation of Olfactory Dysfunctions Induced by Long COVID-19 Official Title: Efficacy of Photobiomodulation in the Rehabilitation of Olfactory Dysfunctions Induced by Long COVID-19 #### Organization Study ID Info ID: GaffreeGuinleUH #### Organization Class: OTHER Full Name: Gaffree & Guinle Universitary Hospital ### Status Module #### Completion Date Date: 2024-12-22 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-17 Overall Status: RECRUITING #### Primary Completion Date Date: 2023-12-22 Type: ACTUAL #### Start Date Date: 2022-06-05 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-02-22 Study First Submit QC Date: 2024-05-17 ### Sponsor Collaborators Module #### Collaborators Class: OTHER_GOV Name: Rio de Janeiro State Research Supporting Foundation (FAPERJ) #### Lead Sponsor Class: OTHER Name: Gaffree & Guinle Universitary Hospital #### Responsible Party Investigator Affiliation: Gaffree & Guinle Universitary Hospital Investigator Full Name: Deborah Santos Sales Investigator Title: Deborah Santos Sales Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: On January 30, 2020, the WHO (World Health Organization) declared the new coronavirus pandemic as the sixth public health emergency of international concern. In February 2020, the virus was designated by the Coronavirus Study Group of the International Committee on Virus Taxonomy as severe acute respiratory syndrome coronavirus 2. Many reports have described the appearance of olfactory or gustatory dysfunction simultaneously with other pre-established symptoms of COVID-19. Symptoms such as loss of taste or smell may appear 2 to 14 days after being infected with COVID-19. Worldwide, evidence regarding anosmia (loss of smell) and dysgeusia (change in taste) has been associated with COVID-19 infection. OBJECTIVES: To evaluate the effectiveness of low-intensity laser in treating changes in smell and taste after COVID-19 infection and map which changes obtained the best results. MATERIAL AND METHODS: This is an intervention study whose sample will consist of 30 individuals with loss of smell and taste for more than 6 months after COVID-19 infection, aged 18 years or older. Detailed Description: objective: To evaluate the effectiveness of low-intensity laser in resolving chemosensory symptoms caused by COVID-19. This is an intervention study. The sample will consist of 30 individuals who will be allocated to the low-intensity laser treatment group. The patients will come from research at the COVID-19 outpatient clinic at the Gafree Guinle University Hospital - UNIRIO. Patients who agree to participate in the study will be informed about the objective of the research and will sign an informed consent form. ### Conditions Module Conditions: - Anosmia - Ageusia - COVID-19 - Rehabilitation - Laser Therapy Keywords: - Anosmia - ageusia - COVID-19 - Rehabilitation - Photobiomodulation ### Design Module #### Design Info Allocation: NA Intervention Model: SEQUENTIAL Intervention Model Description: The sample will consist of 30 individuals who will be allocated to the low-intensity laser treatment group. ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 30 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: This is an intervention study. The sample will consist of 30 individuals who will be allocated to the low-intensity laser treatment group. Intervention Names: - Device: low-intensity laser treatment Label: low-intensity laser treatment group Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - low-intensity laser treatment group Description: The experimental group will be subjected to a total of up to 24 sessions (2x a week for up to 12 weeks) of irradiation with red and infrared laser pulsed radiation, with 820mm wavelength, 60w power and 6 energy cages, applied in both nostrils and in 10 points under the tongue. Name: low-intensity laser treatment Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: evaluate the effectiveness of low-intensity laser Measure: effectiveness of low-intensity laser in the treatment of olfactory dysfunction in long term covid-19 Time Frame: 20 minutes session with photobiomodulation therapy twice a week, for a total of 16 sessions ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Patients who complained of loss of smell and taste more than 6 months after COVID-19 infection, aged 18 years or older, with proof of infection by PCR, will be included in the study. Exclusion Criteria: * Patients with comorbidities prior to COVID-19 infection that could interfere with the functions of smell and taste will be excluded from the study; patients with a history of head and neck cancer, epileptic patients; mouth breathing patients; and pregnant women. Healthy Volunteers: True Maximum Age: 70 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: DEBORAH S SALES, phd Phone: +5521982161520 Role: CONTACT #### Locations Location 1: City: Rio de Janeiro Contacts: *Contact 1:* - Email: [email protected] - Name: DEBORAH S SALES, PHD - Phone: +5521982161520 - Role: CONTACT Country: Brazil Facility: university hospital Gafree Guinle Status: RECRUITING Zip: 20270004 #### Overall Officials Official 1: Affiliation: federal university of the state of rio de janeiro - UNIRIO Name: Claudia CF Vasconcelos, PHD Role: STUDY_DIRECTOR Official 2: Affiliation: University hospital Gafree Guinle - UNIRIO Name: Mariana B Hammerle, MD Role: STUDY_CHAIR Official 3: Affiliation: University hospital Gafree Guinle - UNIRIO Name: DEBORAH SANTOS SALES, PHD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ### References Module #### References Citation: Hammerle MB, Sales DS, Pinheiro PG, Gouvea EG, de Almeida PIFM, de Araujo Davico C, Souza RS, Spedo CT, Nicaretta DH, Alvarenga RMP, Pires KL, Thuler LCS, Vasconcelos CCF. Cognitive Complaints Assessment and Neuropsychiatric Disorders After Mild COVID-19 Infection. Arch Clin Neuropsychol. 2023 Feb 18;38(2):196-204. doi: 10.1093/arclin/acac093. PMID: 36464245 Citation: Vasconcelos CCF, Hammerle MB, Sales DS, Rueda Lopes FC, Pinheiro PG, Gouvea EG, Alves MCDF, Pereira TV, Schmidt SL, Alvarenga RMP, Pires KL. Post-COVID-19 olfactory dysfunction: carbamazepine as a treatment option in a series of cases. J Neurovirol. 2022 Apr;28(2):312-318. doi: 10.1007/s13365-022-01066-3. Epub 2022 Apr 2. PMID: 35366736 #### See Also Links Label: Post-COVID-19 Olfactory and Gustatory Dysfunction: Photobiomodulation Therapy as a Treatment Option in a Series of Cases URL: https://openneurologyjournal.com/VOLUME/17/ELOCATOR/e1874205X2309190/FULLTEXT/ ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011024 - Term: Pneumonia, Viral - ID: D000011014 - Term: Pneumonia - ID: D000012141 - Term: Respiratory Tract Infections - ID: D000007239 - Term: Infections - ID: D000014777 - Term: Virus Diseases - ID: D000018352 - Term: Coronavirus Infections - ID: D000003333 - Term: Coronaviridae Infections - ID: D000030341 - Term: Nidovirales Infections - ID: D000012327 - Term: RNA Virus Infections - ID: D000008171 - Term: Lung Diseases - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000094025 - Term: Post-Infectious Disorders - ID: D000002908 - Term: Chronic Disease - ID: D000020969 - Term: Disease Attributes - ID: D000010335 - Term: Pathologic Processes - ID: D000000857 - Term: Olfaction Disorders - ID: D000012678 - Term: Sensation Disorders - ID: D000009461 - Term: Neurologic Manifestations - ID: D000009422 - Term: Nervous System Diseases - ID: D000013651 - Term: Taste Disorders ### Condition Browse Module - Browse Branches - Abbrev: BC01 - Name: Infections - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M3013 - Name: Post-Acute COVID-19 Syndrome - Relevance: HIGH - As Found: Long COVID - ID: M2561 - Name: COVID-19 - Relevance: HIGH - As Found: COVID-19 - ID: M2570 - Name: Anosmia - Relevance: HIGH - As Found: Anosmia - ID: M3720 - Name: Ageusia - Relevance: HIGH - As Found: Ageusia - ID: M16355 - Name: Syndrome - Relevance: LOW - As Found: Unknown - ID: M13904 - Name: Pneumonia - Relevance: LOW - As Found: Unknown - ID: M13914 - Name: Pneumonia, Viral - Relevance: LOW - As Found: Unknown - ID: M10283 - Name: Infections - Relevance: LOW - As Found: Unknown - ID: M6368 - Name: Communicable Diseases - Relevance: LOW - As Found: Unknown - ID: M14978 - Name: Respiratory Tract Infections - Relevance: LOW - As Found: Unknown - ID: M17522 - Name: Virus Diseases - Relevance: LOW - As Found: Unknown - ID: M20490 - Name: Coronavirus Infections - Relevance: LOW - As Found: Unknown - ID: M6555 - Name: Coronaviridae Infections - Relevance: LOW - As Found: Unknown - ID: M23685 - Name: Nidovirales Infections - Relevance: LOW - As Found: Unknown - ID: M15149 - Name: RNA Virus Infections - Relevance: LOW - As Found: Unknown - ID: M11168 - Name: Lung Diseases - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: M3014 - Name: Post-Infectious Disorders - Relevance: LOW - As Found: Unknown - ID: M6147 - Name: Chronic Disease - Relevance: LOW - As Found: Unknown - ID: M22700 - Name: Disease Attributes - Relevance: LOW - As Found: Unknown - ID: M4183 - Name: Olfaction Disorders - Relevance: LOW - As Found: Unknown - ID: M15490 - Name: Sensation Disorders - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: M16423 - Name: Taste Disorders - Relevance: LOW - As Found: Unknown - ID: T170 - Name: Acute Graft Versus Host Disease - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000086382 - Term: COVID-19 - ID: D000094024 - Term: Post-Acute COVID-19 Syndrome - ID: D000086582 - Term: Anosmia - ID: D000000370 - Term: Ageusia ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423482 Brief Title: Digitization Accuracy and Scannability of Two Different Implant-Supported Prosthodontic Framework Materials Official Title: Digitization Accuracy and Scannability of Two Different Implant-Supported Prosthodontic Framework Materials #### Organization Study ID Info ID: 0796-11/2023 #### Organization Class: OTHER Full Name: Alexandria University ### Status Module #### Completion Date Date: 2025-05-14 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-05-14 Type: ESTIMATED #### Start Date Date: 2024-05-14 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Nourhan Samy #### Responsible Party Investigator Affiliation: Alexandria University Investigator Full Name: Nourhan Samy Investigator Title: Ph.D student Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: The present study aims to clinically evaluate and compare the scanning accuracy and the scannability of 2 different materials used in constructing frameworks for implant-supported prosthesis (titanium and PEEK). The objective of the present study is to evaluate the digitization accuracy and scannability of milled titanium and PEEK implant-supported frameworks in intra-oral conditions and to evaluate the accuracy of the superstructures designed and constructed over the intraorally scanned framework. Detailed Description: Background: For implementing a fully digital workflow, intraoral scanning of prosthetic frameworks may be required for editing purposes in some clinical scenarios. Different materials can be used in constructing implant-supported prosthetic frameworks. However, the scannability and the influence of the material used on the accuracy of the intraoral scan are still unclear. Aim of the study: The purpose of this in vivo study is to evaluate the scanning accuracy and the scannability of different framework materials and to assess the marginal adaptation and accuracy of the superstructures designed and constructed over different scanned framework materials. Materials and methods: Two milled maxillary implant-supported frameworks constructed from 2 different materials will be used in this study. Group I will be constructed from titanium and group II from Poly-Ether-Ether-Ketone (PEEK). The frameworks will be digitized by using a desktop scanner (Tabletop Scanner, Medit T-310; Medit Corp). The STL file produced will be considered as a reference file. Each framework will be scanned intraorally (n=10) by using an intraoral scanner (IOS) (Medit i700; Medit Corp). The STL files obtained from the intraoral scanner will be compared to the reference STL file to assess the scannability. The unscanned surface area in a preset time limit will be used to determine the scannability of each framework. To evaluate the scanning accuracy, all STL files will be imported into a surface-matching software program (Medit Design v3.0.6 Build 286; Medit Corp) where deviation measurements in (μm) will be calculated. A total of 20 superstructures made of nano-ceramic hybrid resin (Flexcera™ Smile Ultra) will be 3D-printed from each STL file obtained from intraoral scanning of the frameworks and then the marginal adaptation will be evaluated by using a stereomicroscope (SZ1145TR; Olympus, Japan). The accuracy will also be assessed by using a surface-matching software program (Geomagic Control X v.2018.1.1; 3D Systems). Analysis: Data will be collected, tabulated, and statistically analyzed by using the appropriate statistical tests. Keywords: Digitization, accuracy, trueness, precision, scannability, implant-supported frameworks, superstructures, marginal adaptation, titanium, PEEK, digital workflow, editing, nano-ceramic hybrid resin. ### Conditions Module Conditions: - Digitalization Accuracy Keywords: - Digitization, accuracy, trueness, precision, scannability, implant-supported frameworks, superstructures, marginal adaptation, titanium, PEEK ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: OTHER #### Enrollment Info Count: 1 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Other: PEEK bar Label: PEEK bar Type: EXPERIMENTAL #### Arm Group 2 Intervention Names: - Other: Titanium bar Label: Titanium bar Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - PEEK bar Description: The framework will be constructed from Poly-Ether-Ether-Ketone (PEEK). The framework will be digitized by using a desktop scanner (Tabletop Scanner, Medit T-310; Medit Corp). The STL file produced will be considered as a reference file. Each framework will be scanned intraorally (n=10) by using an intraoral scanner (IOS) (Medit i700; Medit Corp). Name: PEEK bar Type: OTHER #### Intervention 2 Arm Group Labels: - Titanium bar Description: The framework will be constructed from titanium. The framework will be digitized by using a desktop scanner (Tabletop Scanner, Medit T-310; Medit Corp). The STL file produced will be considered as a reference file. Each framework will be scanned intraorally (n=10) by using an intraoral scanner (IOS) (Medit i700; Medit Corp). Name: Titanium bar Type: OTHER ### Outcomes Module #### Primary Outcomes Description: All scans obtained will be cropped eliminating soft tissue areas guided by the bar's finish line. The STL(D) file obtained from scanning the frameworks by using the desktop scanner will be used as reference scan for the assessment of trueness in the study, to measure the discrepancy with the corresponding 10 STLI files in each group. In each reference STL(D) file, the framework will be selected and used for alignment with their corresponding STL(I) with the best fit alignment algorithm to assess trueness, and then all the STL(I) in each material group will be superimposed to assess precision by using a specialized software program (Medit link). For the quantitative evaluation of 3D deviations between the reference STL(D) and the target data STL(I), the software program deviation display mode will be used to produce color-difference maps from which RMS (root mean square) will be calculated for statistical analysis. Measure: Digitization accuracy of the two different framework materials. Time Frame: one year ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Maxillary edentulous adult patient with a good health status classified as ASA I or II physical status and having maxillary osseointegrated dental implants. 2. Adequate maxillary restorative space (6-8 mm). 3. Adequate zone of keratinized tissue (at least 2 mm). 4. Presence of an antagonistic dentate or rehabilitated arch. Exclusion Criteria: 1. A systemic disease that compromises osseointegration such as uncontrolled diabetes mellitus or metabolic bone diseases. 2. Improper implant position. 3. Heavy smoking. 4. Inability to obtain written informed consent. - Healthy Volunteers: True Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: nourhan Samy Emam, BDS, Msc, Ph.D student Phone: 01099671431 Role: CONTACT #### Locations Location 1: City: Alexandria Contacts: *Contact 1:* - Email: [email protected] - Name: nourhan Samy Emam, BDS,Msc, Ph.D - Phone: 01099671431 - Role: CONTACT Country: Egypt Facility: Alexandria University State: Stanly Status: RECRUITING Zip: 21500 ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ## Derived Section ### Intervention Browse Module - Browse Branches - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M8134 - Name: Ether - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423469 Brief Title: Noninvasive Intracranial Pressure Waveforms Assessment in Traumatic Brain Injury Official Title: A Multicenter Observational Cohort for the Determination of Noninvasive Intracranial Pressure Waveforms Role in Traumatic Brain Injury #### Organization Study ID Info ID: 39348920.1.1001.0068 #### Organization Class: OTHER Full Name: University of Sao Paulo ### Status Module #### Completion Date Date: 2024-04-30 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: COMPLETED #### Primary Completion Date Date: 2024-03-30 Type: ACTUAL #### Start Date Date: 2020-02-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Sergio Brasil, MD #### Responsible Party Investigator Affiliation: University of Sao Paulo Investigator Full Name: Sergio Brasil, MD Investigator Title: MD. PhD Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: In clinical practice, hospital admission of patients with altered level of consciousness ranging from drowsiness to decreasing response states or coma is extremely common. This clinical condition demands effective investigation and early treatment. Imaging and laboratory tests have played increasingly relevant roles in supporting clinical research. One of the main causes of coma is intracranial hypertension (IH), with traumatic brain injuries (TBI) and cerebral hemorrhages being the major contributors to its development. IH increases the risk of secondary damage in these populations, and consequently, morbidity and mortality. Clinical studies show that adequate intracranial pressure (ICP) control in TBI patients reduces mortality and increases functionality. Unfortunately, the most accurate way to measure and evaluate the ICP is through a catheter located inside the skull, and its perforation is required for this purpose. Several studies have attempted to identify noninvasive solutions for ICP monitoring; however, to date, none of the techniques gathered sufficient evidence to replace invasive monitors. Recently, an extensometer device has been developed, which only maintains contact with the skull's skin and therefore eliminates the need for its perforation, being able to obtain recordings of cranial dilatation at each heartbeat and consequently reflecting brain compliance. In vivo studies have identified excellent qualitative correlation with catheter ICP recordings. However, this device was evaluated only in a limited number of clinical cohorts and the correlations between the information provided by this device with patients outcomes is still poor. Therefore, this project aims primarily to evaluate the use of this noninvasive brain compliance monitoring system in a cohort of TBI patients. ### Conditions Module Conditions: - Traumatic Brain Injury Keywords: - traumatic brain injury - intracranial pressure - intracranial compliance - intracranial pressure waveforms - neurological noninvasive monitoring ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 345 Type: ACTUAL Patient Registry: True Study Type: OBSERVATIONAL Target Duration: 6 Months ### Outcomes Module #### Other Outcomes Description: Are brain4care biometrics correlated with invasive intracranial pressure provided by ventricular catheters or parenchymal probes? Measure: Correlation with invasive information Time Frame: Fifteen days #### Primary Outcomes Description: Is in-hospital mortality correlated with poorer brain4care biometrics? Measure: In-hospital mortality Time Frame: One month #### Secondary Outcomes Description: Is morbidity correlated with poorer brain4care biometrics? Measure: Morbidity Time Frame: Six months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Moderate to severe traumatic brain injury with less than 24 hours. Exclusion Criteria: * Primary decompressive craniectomy * Brain death signs at admission * Severe hemodynamic instability Minimum Age: 18 Years Sampling Method: PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Patients of any gender, older than 18 years, with very acute moderate or severe TBI will be included just after stabilization and any surgical evacuation procedure performed. ### IPD Sharing Statement Module Description: Possibly some anonymous data can be shared with other researchers upon reasonable request. IPD Sharing: UNDECIDED ### References Module #### References Citation: Gulamali F, Jayaraman P, Sawant AS, Desman J, Fox B, Chang A, Soong BY, Arivazaghan N, Reynolds AS, Duong SQ, Vaid A, Kovatch P, Freeman R, Hofer IS, Sakhuja A, Dangayach NS, Reich DS, Charney AW, Nadkarni GN. Derivation, External Validation and Clinical Implications of a deep learning approach for intracranial pressure estimation using non-cranial waveform measurements. medRxiv [Preprint]. 2024 Jan 30:2024.01.30.24301974. doi: 10.1101/2024.01.30.24301974. PMID: 38352556 Citation: Kawoos U, McCarron RM, Auker CR, Chavko M. Advances in Intracranial Pressure Monitoring and Its Significance in Managing Traumatic Brain Injury. Int J Mol Sci. 2015 Dec 4;16(12):28979-97. doi: 10.3390/ijms161226146. PMID: 26690122 Citation: de Moraes FM, Rocha E, Barros FCD, Freitas FGR, Miranda M, Valiente RA, de Andrade JBC, Neto FEAC, Silva GS. Waveform Morphology as a Surrogate for ICP Monitoring: A Comparison Between an Invasive and a Noninvasive Method. Neurocrit Care. 2022 Aug;37(1):219-227. doi: 10.1007/s12028-022-01477-4. Epub 2022 Mar 24. PMID: 35332426 Citation: de Moraes FM, Brasil S, Frigieri G, Robba C, Paiva W, Silva GS. ICP wave morphology as a screening test to exclude intracranial hypertension in brain-injured patients: a non-invasive perspective. J Clin Monit Comput. 2024 Feb 14. doi: 10.1007/s10877-023-01120-3. Online ahead of print. PMID: 38355918 Citation: Brasil S, Solla DJF, Nogueira RC, Teixeira MJ, Malbouisson LMS, Paiva WDS. A Novel Noninvasive Technique for Intracranial Pressure Waveform Monitoring in Critical Care. J Pers Med. 2021 Dec 5;11(12):1302. doi: 10.3390/jpm11121302. PMID: 34945774 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001927 - Term: Brain Diseases - ID: D000002493 - Term: Central Nervous System Diseases - ID: D000009422 - Term: Nervous System Diseases - ID: D000006259 - Term: Craniocerebral Trauma - ID: D000020196 - Term: Trauma, Nervous System ### Condition Browse Module - Browse Branches - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC26 - Name: Wounds and Injuries - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M5207 - Name: Brain Injuries - Relevance: HIGH - As Found: Brain Injury - ID: M628 - Name: Brain Injuries, Traumatic - Relevance: HIGH - As Found: Traumatic Brain Injury - ID: M17685 - Name: Wounds and Injuries - Relevance: HIGH - As Found: Injury - ID: M5204 - Name: Brain Diseases - Relevance: LOW - As Found: Unknown - ID: M5742 - Name: Central Nervous System Diseases - Relevance: LOW - As Found: Unknown - ID: M9349 - Name: Craniocerebral Trauma - Relevance: LOW - As Found: Unknown - ID: M22023 - Name: Trauma, Nervous System - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000001930 - Term: Brain Injuries - ID: D000070642 - Term: Brain Injuries, Traumatic - ID: D000014947 - Term: Wounds and Injuries ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423456 Brief Title: Postoperative Pain Control Following Hysteroscopy Official Title: A New Alternative for Postoperative Pain Control Following Hysteroscopy;Preoperative Intravenous Lidocaine #### Organization Study ID Info ID: AFSU-OBGYN-BA-01 #### Organization Class: OTHER Full Name: Afyonkarahisar Health Sciences University ### Status Module #### Completion Date Date: 2024-09-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-22 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-09-30 Type: ESTIMATED #### Start Date Date: 2024-03-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Afyonkarahisar Health Sciences University #### Responsible Party Investigator Affiliation: Afyonkarahisar Health Sciences University Investigator Full Name: Betül Ahat Investigator Title: Assistant Doctor Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Is US Export: False ### Description Module Brief Summary: Intraoperative lidocaine infusion is a frequently preferred method in surgical procedures due to its reducing the need for opioids, providing better postoperative pain control, reducing postoperative nausea and vomiting and increasing rapid recovery. Our aim in this study is to show the effect of intraoperative lidocaine infusion on reducing complications such as pain, nausea, vomiting, and the need for opioid analgesia that occur after hysteroscopy operations, which are often performed in gynecology clinics. Detailed Description: Hysteroscopy abnormal uterine bleeding, infertility, endometrial pathologies, uterine fibroids,it is a method that is often used in the diagnosis and treatment of pathologies such as intrauterine synechia. Hysteroscopy; observation of the inner layer of the uterus with a special optical instrument with a cold light source and it is the process of making intrauterine interventions using small hand tools. General anesthesia or with intrauterine fluid after dilating the cervix under regional (epidural/peridural) anesthesia it is filled and a thin telescope-like optical device (hysteroscope) is transmitted into the uterus. This way the uterine cavity is observed. Hysteroscopy is used for diagnostic purposes as well as for therapeutic purposes it can be applied. General Anesthesia (GA) is often the preferred method for operative hysteroscopy.Intraoperative lidocaine infusion reduces the need for opioids, postoperative pain control is better due to the fact that it reduces postoperative nausea, vomiting and increases rapid recovery, which is often preferred in surgical procedures. 150 patients who are scheduled to undergo hysteroscopy will be included in the study. Hysteroscopy the patients to be applied will be divided into two groups as research and control groups. To both groups 75 patients will be included each. General anesthesia during the procedure for patients in the research arm intravenous lidocaine of 0.15 ml/kg 1% will be administered intraoperatively before and during the procedure a 1% lidocaine infusion(at a dose of 0.2 ml/kg/hour) will be performed. In the control group, if 0.9% saline solution will be used instead of lidocaine. Pain measurement using visual analog scale (VAS) for postoperative pain after surgery will be done. At the same time, intraoperative analgesic use of patients, postoperative nausea-vomiting and antiemetic uses will be recorded. ### Conditions Module Conditions: - Postoperative Pain - Postoperative Nausea - Analgesia Keywords: - hysteroscopy - intraoperative lidocaine - postoperative pain - postoperative nausea ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Intraoperative lidocaine infusion is a frequently preferred method in surgical procedures due to its reducing the need for opioids, providing better postoperative pain control, reducing postoperative nausea and vomiting and increasing rapid recovery. Our aim in this study is to show the effect of intraoperative lidocaine infusion on reducing complications such as pain, nausea, vomiting, and the need for opioid analgesia that occur after hysteroscopy operations, which are often performed in gynecology clinics. ##### Masking Info Masking: TRIPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 160 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: During the procedure, intravenous lidocaine of 0.15 ml/kg 1% will be administered intraoperatively before general anesthesia and infusion of lidocaine of 1%(at a dose of 0.2 ml/kg/hour) will be performed during the procedure. Intervention Names: - Drug: Lidocaine IV Label: Research group Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: In the control group, 0.9% saline solution will be used instead of lidocaine. Intervention Names: - Drug: Saline Label: Control group Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Research group Description: Pain measurement will be performed using a visual analog scale (VAS) for postoperative pain after the operation. At the same time, patients' intraoperative analgesic use, postoperative nausea-vomiting and antiemetic use will be recorded. Name: Lidocaine IV Other Names: - lidocaine HCl 2% Type: DRUG #### Intervention 2 Arm Group Labels: - Control group Description: Pain measurement will be performed using a visual analog scale (VAS) for postoperative pain after the operation. At the same time, patients' intraoperative analgesic use, postoperative nausea-vomiting and antiemetic use will be recorded. Name: Saline Other Names: - 0.09% Saline Type: DRUG ### Outcomes Module #### Primary Outcomes Description: After the hysteroscopy procedure is completed, in the postoperative anesthesia care room, postoperative, 30. and 60. in minutes, 4. per hour and 24. pain measurement will be performed for patients per hour using a visual analog scale (VAS) for postoperative pain. In this scale, patients' pain between 0-10 (0=no pain, 10=very severe pain) will be questioned. Dec. The doctor who performed the measurement will not know which drug infusion was made. NSAIDs will be administered to patients with a VAS score \> 4. Opioid analgesics will be administered to patients whose pain does not go away. At the same time, patients' intraoperative analgesic use, postoperative nausea-vomiting and antiemetic use will be recorded. Measure: Visual analog scale (VAS) Time Frame: 24 hours ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Female patients with ASA I-II according to the American Society of Anesthesiologists (ASA) classification who are scheduled for elective hysteroscopy with indications such as * abnormal uterine bleeding * endometrial polyp * submucosal myoma * foreign body in the endometrial cavity * infertility * intrauterine synechia Exclusion Criteria: * Patients under the age of 18 * Who are allergic to lidocaine addicted to opioids or NSAIDs * Patients with chronic pain * Patients with severe systemic disease * Patients who do not approve Gender Based: True Healthy Volunteers: True Maximum Age: 65 Years Minimum Age: 19 Years Sex: FEMALE Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Betul Ahat Phone: +905467240341 Role: CONTACT #### Locations Location 1: City: Merkez Contacts: *Contact 1:* - Email: [email protected] - Name: Rıza Dur - Phone: +905326919591 - Role: CONTACT Country: Turkey Facility: Afyonkarahisar University of Health Science, school of medicine, hospital State: Afyonkarahi̇sar Status: RECRUITING Zip: 06330 #### Overall Officials Official 1: Affiliation: Afyonkarahisar University of Health Science, school of medicine Name: Betul Ahat Role: PRINCIPAL_INVESTIGATOR Official 2: Affiliation: Afyonkarahisar University of Health Science, school of medicine Name: Tuba Berra Sarıtaş Role: STUDY_CHAIR Official 3: Affiliation: Afyonkarahisar University of Health Science, school of medicine Name: Rıza Dur Role: STUDY_DIRECTOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011183 - Term: Postoperative Complications - ID: D000010335 - Term: Pathologic Processes - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations - ID: D000012817 - Term: Signs and Symptoms, Digestive - ID: D000014839 - Term: Vomiting ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases ### Condition Browse Module - Browse Leaves - ID: M13069 - Name: Pain, Postoperative - Relevance: HIGH - As Found: Postoperative Pain - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M12273 - Name: Nausea - Relevance: HIGH - As Found: Nausea - ID: M17582 - Name: Vomiting - Relevance: LOW - As Found: Unknown - ID: M22074 - Name: Postoperative Nausea and Vomiting - Relevance: HIGH - As Found: Postoperative Nausea - ID: M14065 - Name: Postoperative Complications - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: M15622 - Name: Signs and Symptoms, Digestive - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000010149 - Term: Pain, Postoperative - ID: D000009325 - Term: Nausea - ID: D000020250 - Term: Postoperative Nausea and Vomiting ### Intervention Browse Module - Ancestors - ID: D000000779 - Term: Anesthetics, Local - ID: D000000777 - Term: Anesthetics - ID: D000002492 - Term: Central Nervous System Depressants - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000018689 - Term: Sensory System Agents - ID: D000018373 - Term: Peripheral Nervous System Agents - ID: D000000889 - Term: Anti-Arrhythmia Agents - ID: D000061567 - Term: Voltage-Gated Sodium Channel Blockers - ID: D000026941 - Term: Sodium Channel Blockers - ID: D000049990 - Term: Membrane Transport Modulators - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action ### Intervention Browse Module - Browse Branches - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: AnArAg - Name: Anti-Arrhythmia Agents - Abbrev: ChanBlk - Name: Channel Blockers - Abbrev: Analg - Name: Analgesics - Abbrev: PhSol - Name: Pharmaceutical Solutions - Abbrev: AnEm - Name: Antiemetics - Abbrev: Gast - Name: Gastrointestinal Agents ### Intervention Browse Module - Browse Leaves - ID: M4107 - Name: Anesthetics - Relevance: LOW - As Found: Unknown - ID: M11014 - Name: Lidocaine - Relevance: HIGH - As Found: Solution - ID: M4032 - Name: Analgesics - Relevance: LOW - As Found: Unknown - ID: M21860 - Name: Pharmaceutical Solutions - Relevance: LOW - As Found: Unknown - ID: M4251 - Name: Antiemetics - Relevance: LOW - As Found: Unknown - ID: M4109 - Name: Anesthetics, Local - Relevance: LOW - As Found: Unknown - ID: M4213 - Name: Anti-Arrhythmia Agents - Relevance: LOW - As Found: Unknown - ID: M23177 - Name: Sodium Channel Blockers - Relevance: LOW - As Found: Unknown - ID: M30025 - Name: Diuretics, Potassium Sparing - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000008012 - Term: Lidocaine ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423443 Brief Title: Digital Cognitive Behavioral Therapy for Depressive Disorders Official Title: Digital Cognitive Behavioral Therapy for Depressive Disorders: A Randomized Controlled Trial #### Organization Study ID Info ID: ICBT2301 #### Organization Class: OTHER Full Name: Adai Technology (Beijing) Co., Ltd. ### Status Module #### Completion Date Date: 2025-12-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-24 Type: ACTUAL Last Update Submit Date: 2024-05-22 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-06-30 Type: ESTIMATED #### Start Date Date: 2023-12-20 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Adai Technology (Beijing) Co., Ltd. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: This study aims to explore the effectiveness of digital interventions combined with medication in the treatment of patients with depressive disorders. Its main aim is to answer: Can digital interventions combined with medication effectively alleviate symptoms of depression? The experiment will compare the effects of medication combined with digital interventions to those combined with online mental health education to evaluate their relative effectiveness. Participants will be required to engage with the medication plus digital therapy for a duration of two months, and follow-up assessments will be conducted to evaluate the long-term effects of the treatments and monitor any changes in depressive symptoms. ### Conditions Module Conditions: - Depression - Anxiety ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: DOUBLE Who Masked: - PARTICIPANT - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 146 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Behavioral: Digital Cognitive Behavioral Therapy - Drug: TAU Label: Digital Cognitive Behavioral Therapy Type: EXPERIMENTAL #### Arm Group 2 Intervention Names: - Behavioral: Health Education - Drug: TAU Label: Health Education Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Digital Cognitive Behavioral Therapy Description: digital cognitive behavioral therapy app Name: Digital Cognitive Behavioral Therapy Type: BEHAVIORAL #### Intervention 2 Arm Group Labels: - Health Education Description: traditional on-line health education app Name: Health Education Type: BEHAVIORAL #### Intervention 3 Arm Group Labels: - Digital Cognitive Behavioral Therapy - Health Education Description: treatment as usual Name: TAU Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Score Range: 0 (best outcome) to 60 (worst outcome) Higher scores indicate worse depression symptoms. Measure: Montgomery-Asberg Depression Rating Scale (MADRS) Time Frame: baseline and immediately after 8-week intervention, and follow-ups at 4 weeks, 12 weeks, and 6 months #### Secondary Outcomes Description: PHQ-9 Score Range: 0 (best outcome) to 27 (worst outcome); higher scores indicate more severe depression symptoms. Measure: PHQ-9 (Patient Health Questionnaire-9) Time Frame: baseline and weekly assessments during the treatment period, assessed up to 8 weeks, and follow-ups at 4 weeks, 12 weeks, and 6 months Description: GAD-7 Score Range: 0 (best outcome) to 21 (worst outcome); higher scores indicate more severe generalized anxiety symptoms. Measure: GAD-7 (Generalized Anxiety Disorder-7) Time Frame: baseline and weekly assessments during the treatment period, assessed up to 8 weeks, and follow-ups at 4 weeks, 12 weeks, and 6 months Description: Score Range: 14 (best outcome) to 56 (worst outcome) Higher scores indicate greater levels of anhedonia (reduced ability to experience pleasure). Measure: Snaith-Hamilton Pleasure Scale (SHAPS) Time Frame: baseline, immediately after 8-week intervention, and follow-ups at 4 weeks, 12 weeks, and 6 months Description: Score Range: 22 (best outcome) to 88 (worst outcome) Higher scores indicate higher levels of rumination. Measure: Rumination Response Scale (RRS) Time Frame: baseline, immediately after 8-week intervention, and follow-ups at 4 weeks, 12 weeks, and 6 months Description: Score Range: 0 (best outcome) to 21 (worst outcome) Higher scores indicate poorer sleep quality. Measure: Pittsburgh Sleep Quality Index (PSQI) Time Frame: baseline, immediately after 8-week intervention, and follow-ups at 4 weeks, 12 weeks, and 6 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Meets the diagnostic criteria for depression according to the DSM-5 (Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition), without psychotic symptoms, as recurrent outpatient or inpatient. 2. Patients with a Montgomery-Asberg Depression Rating Scale (MADRS) score ≥ 22 before randomization. 3. Age ≥ 18 and ≤ 65 years, regardless of gender. 4. Understands the trial and signs the informed consent form. Exclusion Criteria: 1. Meets criteria for other psychiatric disorders according to the DSM-5, including schizophrenia spectrum disorders, bipolar and related disorders, neurodevelopmental disorders, neurocognitive disorders, or depression due to substance and/or medication or other medical conditions. 2. History of substance and/or alcohol abuse within the past year. 3. Significant risk of suicide (MADRS item 10 score = 4). 4. Difficulty or inability to communicate verbally, understand or follow instructions, or cooperate with treatment and assessment. 5. Inability to use a smartphone. 6. Deemed unsuitable for participation by the researcher. Maximum Age: 65 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Liqun Zhang Phone: 010-85795371 Role: CONTACT #### Locations Location 1: City: Chengdu Contacts: *Contact 1:* - Name: Liqun Zhang - Role: CONTACT Country: China Facility: West China Hospital State: Sichuang Status: RECRUITING ## Derived Section ### Condition Browse Module - Ancestors - ID: D000019964 - Term: Mood Disorders - ID: D000001523 - Term: Mental Disorders ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M7058 - Name: Depression - Relevance: LOW - As Found: Unknown - ID: M4324 - Name: Anxiety Disorders - Relevance: LOW - As Found: Unknown - ID: M7061 - Name: Depressive Disorder - Relevance: HIGH - As Found: Depressive Disorder - ID: M21835 - Name: Mood Disorders - Relevance: LOW - As Found: Unknown - ID: M4815 - Name: Mental Disorders - Relevance: LOW - As Found: Unknown - ID: M14473 - Name: Psychotic Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003866 - Term: Depressive Disorder ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423430 Brief Title: [Trial of device that is not approved or cleared by the U.S. FDA] Official Title: [Trial of device that is not approved or cleared by the U.S. FDA] #### Organization Study ID Info ID: ABT-CIP-10494 #### Organization Full Name: [Redacted] ### Status Module Delayed Posting: True #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: WITHHELD #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-16 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Name: [Redacted] #### Responsible Party Old Name Title: [Redacted] Old Organization: [Redacted] ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423417 Brief Title: RCT: the Effectiveness of LifeHack in Improving Mental Wellbeing in University Students. Official Title: LifeHack: RCT Evaluating the Effectiveness of a Guided E-health Programme in Improving Mental Wellbeing in University Students. #### Organization Study ID Info ID: 2023-10-30-S.vanLuenen-V1-506 #### Organization Class: OTHER Full Name: Universiteit Leiden ### Status Module #### Completion Date Date: 2025-07 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-12 Type: ESTIMATED #### Start Date Date: 2023-11-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-08 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Maastricht University Class: OTHER Name: VU University of Amsterdam Class: OTHER Name: Utrecht University Class: OTHER Name: University of Amsterdam Class: OTHER Name: Rotterdam University of Applied Sciences Class: OTHER Name: Erasmus University Rotterdam Class: UNKNOWN Name: Avans University of applied sciences Class: UNKNOWN Name: InHolland University of Applied Sciences #### Lead Sponsor Class: OTHER Name: Universiteit Leiden #### Responsible Party Investigator Affiliation: Universiteit Leiden Investigator Full Name: Sanne van Luenen Investigator Title: assistant professor in the Clinical Psychology unit at the Institute of Psychology Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Psychological issues are common among university students and affect mental wellbeing. The Caring Universities (CU) project, involving nine Dutch universities, aims to enhance students' mental health through an annual online questionnaire and a platform offering guided eHealth interventions. One intervention, LifeHack, utilizes cognitive behavioral therapy-based modules to improve mental wellbeing by enhancing resilience and life skills. The effects of LifeHack with pre-post measurements (total n = 216 at post-test) found found that LifeHack led to improvements in mental wellbeing, but dropout rates were influenced by lack of motivation and module relevance. A personalized version of LifeHack is being developed to address these issues and will be evaluated in an RCT to assess its effectiveness in improving mental wellbeing and related outcomes among university students. Detailed Description: Psychological problems are prevalent among university students and are associated with lower mental wellbeing and resilience. Universities provide an excellent environment for students to enhance mental wellbeing, resilience, and acquire life skills. Caring Universities (CU) is an internationally embedded consortium of nine Dutch universities aimed at improving students' mental wellbeing. The CU project consists of two components: 1) an annual online questionnaire assessing students' mental health; and 2) a platform offering free, guided eHealth interventions to enhance mental well-being. One of the interventions on the CU platform - called LifeHack - seeks to enhance mental wellbeing by increasing resilience, teaching life skills, and strengthening mental wellbeing. LifeHack is a guided eHealth intervention based on cognitive behavioural therapy, comprising 13 modules of approximately 30 minutes each focusing on four themes (mood management, productivity, self-worth, and relationships). We investigated the effects of LifeHack with pre-post measurements (total n = 216 at post-test) and found that after following LifeHack, mental wellbeing improved with small to moderate effect sizes. Additionally, students reported satisfaction with the programme and the eCoach. However, participants indicated lack of motivation and early symptom reduction as important reasons for drop-out. Furthermore, the diverse topics covered in LifeHack may not be relevant to all students, leading to more dropouts. Currently, there are two versions of LifeHack: one 'structured', where modules must be completed in order, and one 'free choice', where all modules are available from the start and none are mandatory. For the proposed study, the free choice version of LifeHack will be used and adapted in co-creation with students as follows: participants will be asked which topics they find most important and want to work on. Based on their answers, a personalized selection of modules will be presented, and students can choose which module to start with. Each module is standalone, allowing students to proceed to another module or stop after completing one or more. Each module has a clear structure, beginning with goal formulation and concluding with an action plan. The new adapted version of LifeHack will be personalized and tailored for each student, aiming to improve motivation and reduce dropout rates. With the current study, we aim to examine the effectiveness of the adapted version of LifeHack in an RCT to enhance mental wellbeing in university students. Secondary objectives include investigating differences between the intervention and control groups on students' self-report questionnaire resilience scores, depression scores, anxiety scores, stress-related scores, and mental health quality of life scores (pretest vs post-test). Additional outcomes include satisfaction with the programme and the eCoach, as well as adherence to the intervention. ### Conditions Module Conditions: - Internet-based Intervention - Waiting List Control Group - Depression - Anxiety - Stress - Quality of Life - Mental Wellbeing - Resilience ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: The present study is a two-arm randomized controlled superiority trial. This trial will be conducted in a university setting. A guided web-based resilience and mental wellbeing programme (LifeHack) will be compared to a waiting list condition. Participants in the waiting list condition will start with the programme 4 weeks after randomization. ##### Masking Info Masking: NONE Primary Purpose: HEALTH_SERVICES_RESEARCH #### Enrollment Info Count: 217 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: LifeHack is a guided (weekly feedback by a coach is provided) e-heath self-help application, which is based on cognitive behavioral techniques. The goal of LifeHack is to improve mental wellbeing. The guided internet-based self-help programme LifeHack was developed based on existing literature and adapted in collaboration with university students. The programme comprises twelve modules that are delivered via computer, laptop, tablet, or mobile phone. The modules take approximately 30 minutes on 4 themes (mood management, productivity, self-worth and relationships). Guidance: E-coaches will be trained clinical psychology master students. E-coaches will provide asynchronous written personalized feedback to each participant through the program platform within 48 hours (counting workdays only) after session completion. The aim of the written feedback is to increase motivation and adherence of the participants. Intervention Names: - Behavioral: LifeHack Label: LifeHack Type: EXPERIMENTAL #### Arm Group 2 Description: Participants in the waiting list control condition will start with the programme 4 weeks after randomization. Label: Control group Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - LifeHack Description: See arm description Name: LifeHack Type: BEHAVIORAL ### Outcomes Module #### Other Outcomes Description: Patient Health Questionnaire - 4 (Kroenke et al., 2009). After each module, the PHQ-4 will be assessed in both groups. Measure: Depression and anxiety (PHQ-4) after each module. Time Frame: After each module (approximately once per week) Description: The Client Satisfaction Questionnaire, CSQ-8 (Larsen et al., 1979) Measure: Client satisfaction (CSQ-8) Time Frame: 4 weeks post-baseline active group and 4 weeks post-T2 wait list group. Description: We will also ask participants to evaluate the e-coach at the post-test. The questions about e-coach evaluation will be based on the Working Alliance Inventory for Guided Internet Interventions (WAI-I) (Gómez Penedo et al., 2020) Measure: E-coach evaluation (WAI-I) Time Frame: 4 weeks post-baseline active group and 4 weeks post-T2 wait list group. Description: Adherence will be measured by the total number of completed sessions, time spent on the platform, and the number of logins. Measure: Adherence (Log info) Time Frame: T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) #### Primary Outcomes Description: Mental Health Continuum-Short Form, MHC-SF (Lamers et al., 2011). Measure: Mental wellbeing (MHC-SF) Time Frame: T0 (baseline), T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) #### Secondary Outcomes Description: Brief Resilience Scale (Smith et al., 2008). Measure: Resilience (BRS) Time Frame: T0 (baseline), T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) Description: Patient Health Questionnaire - 9, PHQ-9 (Kroenke et al., 2001). Measure: Depressive symptoms (PHQ-9) Time Frame: T0 (baseline), T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) Description: Perceived Stress Scale-10, PSS-10 (Cohen, 1988). Measure: Stress related symptoms (PSS-10) Time Frame: T0 (baseline), T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) Description: Generalized Anxiety Disorder-7 scale, GAD-7 (Spitzer et al., 2006). Measure: Symptoms of anxiety (GAD-7) Time Frame: T0 (baseline), T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) Description: Mental Health Quality of Life questionnaire, MHQoL (Krugten et al., 2022). Measure: Quality of life (MHQoL) Time Frame: T0 (baseline), T1 (4 weeks post-baseline active group), T2 (4 weeks post-baseline wait list group), T3 (4 weeks post-T2 wait list group), T4 (6 months post-baseline both groups) Description: E.g. gender, age, nationality Measure: Demographics Time Frame: T0 (baseline) ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Being fluent in Dutch and/or English * Being enrolled as a student at one of the 9 participating universities * Being 16 years of age or older * Having access to a PC or mobile device with internet access * Provide informed consent before participation * Score of 50 or lower on the MHC-SF. This is 1 SD above the mean baseline score of participants of LifeHack. This inclusion criterion ensures no students with optimal mental wellbeing are included because they will not be able to show any change. Healthy Volunteers: True Maximum Age: 99 Years Minimum Age: 16 Years Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Sanne van Luenen, PhD Phone: 0031-715277957 Role: CONTACT #### Locations Location 1: City: Amsterdam Contacts: *Contact 1:* - Name: Sanne van Luenen - Role: CONTACT Country: Netherlands Facility: VU Amsterdam Status: RECRUITING Location 2: City: Leiden Contacts: *Contact 1:* - Name: Sanne van Luenen - Role: CONTACT Country: Netherlands Facility: Leiden University Status: RECRUITING #### Overall Officials Official 1: Affiliation: Leiden University Name: Sanne van Luenen, PhD Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M7058 - Name: Depression - Relevance: LOW - As Found: Unknown - ID: M4324 - Name: Anxiety Disorders - Relevance: LOW - As Found: Unknown - ID: M7061 - Name: Depressive Disorder - Relevance: LOW - As Found: Unknown - ID: T6034 - Name: Quality of Life - Relevance: HIGH - As Found: Quality of Life ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423404 Brief Title: Active Breaks on Mental Health and Classroom Climate in Chilean Schoolchildren Aged 6 to 10 Official Title: Video-Guided Active Breaks With Curricular Content on Mental Health and Classroom Climate in Chilean Schoolchildren Aged 6 to 10: Study Protocol for a Multicentre Randomized Controlled Trial #### Organization Study ID Info ID: Universidad de Concepción #### Organization Class: OTHER Full Name: Universidad de Concepcion ### Status Module #### Completion Date Date: 2024-08-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: ENROLLING_BY_INVITATION #### Primary Completion Date Date: 2024-08-30 Type: ESTIMATED #### Start Date Date: 2024-03-20 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Universidad de Concepcion #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Background: The incidence of mental health issues in children is increasing worldwide. In Chile, a recent surge in reports of deteriorating mental health among school populations and an increase in complaints related to poor school climate have been observed. Physical activity, specifically active breaks in the classroom, has shown positive effects on children's health. However, evidence regarding its impact on mental health and school climate in children is limited. Objective: This article outlines the design, measurements, intervention program, and potential efficacy of the Active Classes + School Climate and Mental Health project. This project will assess a 12-week program of active breaks through guided videos with curricular content in the school classroom, and its effects on mental health and school climate as its primary contributions. Additionally, it will measure physical activity, physical fitness, motor competence, and academic performance in students aged 6 to 10 years in the Biobío province, Chile, as secondary contributions. Methodology: It will be performed a multicenter randomized controlled trial involving students in the 1st to 4th grade (6 to 10 years old), encompassing a total of 48 classes across six schools (three intervention and three control) in the Biobío region, Chile. Video-guided active breaks will be implemented through the Active Classes; web platform, featuring curricular content, lasting 5 to 10 minutes and of moderate to vigorous intensity physical activity, twice a day, Monday to Friday, over a span of 12 weeks. Expected Results/Discussion: To our knowledge, this will be the first study in Chile to evaluate the effects of incorporating video-guided active breaks with curricular content on mental health variables and school climate in schoolchildren. Thus, this study contributes to the scarce evidence on the effects of video-guided active breaks on mental health variables and school climate in schoolchildren worldwide. Additionally, it will provide crucial information about active teaching methodologies that have the potential to positively contribute to the well-being of students, thus addressing the problems of mental health and climate in Chilean schools. ### Conditions Module Conditions: - Mental Health - School-age Children - School Health Keywords: - active break - mental health - school climate - schoolchildren - physical fitness - multicentre randomized controlled trial ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: The project involves public primary schools with similar indices of school vulnerability (SVI) and medium to low socioeconomic status in the Biobío province, Chile. This selection was made because students attending these schools spend approximately eight hours per day (from 8:00 AM to 4:00 PM) with two 30-minute breaks and a longer one-hour lunch break. The intervention will focus on 1st to 4th grade classes. Six schools (three treatments and three controls) were recruited, estimating a sample size of 700 students (six schools × eight classes, with each class having 30 to 40 students). ##### Masking Info Masking: DOUBLE Masking Description: After schools agreed to participate, they were randomly assigned using a sequence generated by the IBM SPSS statistical package, with concealed allocation to one of two groups: 1) the Experimental Group (n=3), receiving a 12-week program of video-guided active breaks with curricular content in the school classroom; and 2) the Control Group (n=3), receiving the same intervention as the experimental group after the final data collection. A simple stratified randomization sequence by sex was used to achieve balance between males and females in both groups. The randomization sequence will be concealed through sequentially numbered, opaque, sealed envelopes, conduct by a project investigator with no contact with schools and participants. Significant differences in the quality of life, motor skills, and academic performance have been found in studies with similar samples. Who Masked: - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 700 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The Experimental Group, receiving a 12-week program of video-guided active breaks with curricular content in the school classroom Intervention Names: - Behavioral: the Experimental Group, receiving a 12-week program of video-guided active breaks with curricular content in the school classroom Label: Experimental Group: Active Break group Type: EXPERIMENTAL #### Arm Group 2 Description: The Control Group, receiving the same intervention as the experimental group after the final data collection. During the time of the intervention, the waiting list group will receive the usual classes. Intervention Names: - Behavioral: the Experimental Group, receiving a 12-week program of video-guided active breaks with curricular content in the school classroom Label: Control group: waiting list group Type: OTHER ### Interventions #### Intervention 1 Arm Group Labels: - Control group: waiting list group - Experimental Group: Active Break group Description: The \"Active Classes + School Climate and Mental Health\" program was crafted following a comprehensive review by the research team on active breaks in the child school population. Based on the findings of this review, the optimal type and duration of intervention, frequency and intensity of the most effective exercises, and video-guided modalities with curricular content for active breaks will be established. Subsequently, a collaborative network was formed, involving researchers from education, sports science, social sciences, medicine, primary school teachers within the Chilean public school system, teams of educational leaders, parents, guardians, pedagogy students, and graduate students. The purpose was to create a team that systematically supports the development of various stages of the project from a multi and interdisciplinary perspective Name: the Experimental Group, receiving a 12-week program of video-guided active breaks with curricular content in the school classroom Other Names: - active break program Type: BEHAVIORAL ### Outcomes Module #### Other Outcomes Description: The sociodemographic instrument includes information related to characteristics of the students and their parents (i.e. economic level, educational level). In addition, physical activity and sedentary behavior, eating habits, sleeping and screen habits, type of transportation to the educational center. Measure: Sociodemographic Time Frame: From enrollment to the end of treatment at five months #### Primary Outcomes Description: School climate scale (ECLIS). 82 items with a four-level Likert-type response format (ranging from all to none). Measure: School climate Time Frame: From enrollment to the end of treatment at five months Description: This outcome will be measurement with School Self-Esteem Test (SSET) and Self-report of socioemotional well-being. The raw score sum is transformed into a T score according to age norms, categorizing students as follows: normal self-esteem, ≥ 40 points; low self-esteem, 30-39 points; and very low self-esteem, ≤ 29 points. Measure: Mental health Time Frame: From enrollment to the end of treatment at five months #### Secondary Outcomes Description: The academic performance of the students will be measured using Integral Learning Diagnosis. For this study, only the reading test (2nd, 3rd, and 4th grades) and mathematics test (3rd and 4th grades) were used, measured at the beginning and end of the school year. The grading scale is from 1 as a minimum value to 7 as a maximum value. Measure: Academic performance Time Frame: From enrollment to the end of treatment at five months Description: This outcome will be measurement using the Alpha Fitness Test battery protocol, which includes measurements of cardiorespiratory, musculoskeletal, and motor condition. Measure: Physical health Time Frame: From enrollment to the end of treatment at five months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: - a) Regular male or female students in primary education, from first to fourth grade, at a public school in one of the three provinces of the Biobío region, willing to participate and with parental consent. b) Students spend at least 38 hours per week in classes (6.5 hours daily) and have at least two short breaks (10-15 minutes) per day. Exclusion Criteria: * a) Students with a medical diagnosis of spinal pathologies, vertigo, or uncontrolled hypertension. b) Students with severe intellectual disabilities prevented them from following the program instructions. c) Students participating simultaneously in another project with similar objectives. Healthy Volunteers: True Maximum Age: 10 Years Minimum Age: 6 Years Sex: ALL Standard Ages: - CHILD ### Contacts Locations Module #### Locations Location 1: City: Concepción Country: Chile Facility: Universidad de Concepción State: Biobio Zip: 4030000 Location 2: City: Concepción Country: Chile Facility: Universidad de Concepción State: Biobio Zip: 4070371 ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ### References Module #### References Citation: Reyes-Amigo T, Ibarra-Mora J, Aguilar-Farias N, Gomez-Alvarez N, Carrasco-Beltran H, Zapata-Lamana R, Hurtado-Almonacid J, Paez-Herrera J, Yanez-Sepulveda R, Cortes G, Rolle-Caceres G, Bezerra A. An active break program (ACTIVA-MENTE) at elementary schools in Chile: study protocol for a pilot cluster randomized controlled trial. Front Public Health. 2024 Jan 8;11:1243592. doi: 10.3389/fpubh.2023.1243592. eCollection 2023. PMID: 38259740 ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423391 Acronym: NeuOst Brief Title: Multimodal Intervention for Painful Diabetic Neuropathy: NeuOst Feasibility Trial Official Title: A Multimodal Manual Therapy-Based Intervention for People With Painful Diabetic Neuropathy: Feasibility of a Randomised Controlled Efficacy Trial #### Organization Study ID Info ID: NeuOst feasib V 1.0 March 2024 #### Organization Class: OTHER Full Name: University College of Osteopathy ### Status Module #### Completion Date Date: 2024-11-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-10-01 Type: ESTIMATED #### Start Date Date: 2024-04-30 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-09 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Imperial College London Class: OTHER Name: King's College London Class: OTHER Name: University of Oxford Class: OTHER Name: Universität Münster #### Lead Sponsor Class: OTHER Name: University College of Osteopathy #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: This is the feasibility study of a single-site parallel three-armed participant-blinded controlled randomised efficacy trial of a 5-week course of the 'NeuOst treatment', compared to a designated control intervention, and to usual care only, for adults with pDPN. Detailed Description: Eligible participants are adults diagnosed with diabetes and pDPN, as evaluated with clinical questionnaires during an initial telephone screening. Participants with foot ulcerations, amputations, and advanced organ failure are excluded. Twelve participants per arm (36 in total) will be recruited via social media, local print media, and a poster and leaflet campaign in relevant clinics. Blocked randomisation will allocate participants in a 1:1:1 ratio, using permuted block sizes. The test intervention consists of five weekly 1-hour sessions of semi-standardised augmented manual therapy with a specifically trained provider (NeuOst), in addition to participants' continued usual care. The control intervention will be specifically matched following current guidance, replicating the NeuOst intervention in all aspects except selected components which the study aims to investigate. Providers will be UK-registered osteopaths. Both test and control intervention were developed with extensive involvement of people with pDPN and practitioners. The third study arm will be a Usual Care (UC) group, consisting of baseline and follow-up assessments only. All trial participants can continue their usual care outside the trial, although participants will be asked to not alter their medication regimens or nonpharmacological management if possible. An independent combined steering \& data-monitoring committee (TSC/DMC) will monitor the trial throughout and include a stakeholder representative. Participants will be reimbursed for their travel expenses but not time. Screening and follow-up data collection will be conducted electronically or via the phone to minimise trial burden. The timepoints of follow-up are immediately after treatment completion, and at 8 and 16 weeks from randomisation. Key methodological and reporting guidance for feasibility trials will be followed, and a protocol pre-registered. Ethical approval was obtained from the institutional Research Ethics Committee. Feasibility of a definite trial will be judged according to pre-specified criteria regarding the primary feasibility outcomes following pre-specified progression rules: Recruitment, consent rates, treatment completion, retention rates, interventionist fidelity in treatment delivery, data completeness, treatment acceptability, blinding success, and adverse events. Secondary outcomes include measures of pain intensity, interference, and quality, sleep, quality of life, and fear of falling. The sample size of 36 was a pragmatic decision based on available funding and the trial is not powered to detect meaningful differences in clinical outcomes. Analysis of feasibility outcomes will be largely descriptive. For clinical outcomes, a pre-specified blinded analysis will provide estimates of changes in clinical outcome measures and their variance, modelling differently sized confidence intervals and presenting them as forest plot with the MCID indicated. This information can then be used for sample size calculations for a potential full-scale trial. Qualitative data from interviews with volunteering participants and trial interventionists will provide further nuance for progression decisions or intervention refinement. ### Conditions Module Conditions: - Painful Diabetic Neuropathy ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: feasibility study of a single-site parallel three-armed participant-blinded controlled randomised trial ##### Masking Info Masking: TRIPLE Masking Description: The following stakeholders will be blinded to participants' group allocation in the test intervention and control intervention groups. Allocation to the Usual Care group will not be concealed from staff or participants, except for the trial statistician: * Trial participants (except in usual care arm) * Clinical support and administration staff * Outcome assessors (collecting data at end-of-treatment and follow-up) * Trial statistician * Provider blinding will not be possible as providers will have to actively deliver both the test and the control intervention. However, extensive pre-trial training and supervision during the trial will ensure that providers understand the purpose of the control intervention and are supported to deliver it with high fidelity. Who Masked: - PARTICIPANT - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 36 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The tested treatment is a manual therapy-based intervention, drawing on core manual therapy components and integrating psychologically informed approaches to pain management and elements from diabetes education, foot care, and exercise rehabilitation. This intervention is called 'Augmented manual therapy for people with painful diabetic neuropathy', or NeuOst. NeuOst components will be taught to fully qualified UK-registered osteopaths who then deliver the intervention according to a treatment manual in 1:1 appointments, lasting 45-60 minutes each (90 mins first appointment). Up to 5 treatment sessions will be provided per patient, at weekly intervals and at maximum over 10n weeks. The treatment manual specifies obligatory and optional elements for each of the 5 study treatment sessions. Exercise components will be rehearsed in the clinic with providers. Participants will then be encouraged to complete a progressive home-exercise programme according to the manual. Intervention Names: - Other: NeuOst Label: Tested intervention (NeuOst treatment) Type: EXPERIMENTAL #### Arm Group 2 Description: The objectives of the control intervention are to replicate the contextual elements of the test intervention (to test efficacy), and to blind participants to group allocation. Trial providers will be trained in its delivery. As per CoPPS guidance, the control intervention will resemble the tested intervention in all aspects but for the components whose effect the trial is designed to study. These excluded components of interest, and their respective adaptations in the control intervention, are specified in the detailed pre-registered protocol. Control intervention components will be taught to fully qualified UK-registered osteopaths who then deliver the intervention according to a treatment manual in 1:1 appointments, lasting 45-60 minutes each (90 mins first appointment). Up to 5 treatment sessions will be provided per patient, at weekly intervals and at maximum over 10 weeks. Intervention Names: - Other: Control Intervention Label: Control intervention Type: SHAM_COMPARATOR #### Arm Group 3 Description: Participants randomized to this study arm will only undergo baseline and follow-up assessments but will receive no further attention as part of this trial. As in all other trial arms, they are free to continue their usual medical care but will be encouraged to not change their analgesic regime or nonpharmacological management as far as possible. Intervention Names: - Other: Usual Care Label: Usual care comparator Type: OTHER ### Interventions #### Intervention 1 Arm Group Labels: - Tested intervention (NeuOst treatment) Description: As above Name: NeuOst Type: OTHER #### Intervention 2 Arm Group Labels: - Control intervention Description: As above Name: Control Intervention Type: OTHER #### Intervention 3 Arm Group Labels: - Usual care comparator Description: As above Name: Usual Care Other Names: - Treatment as Usual Type: OTHER ### Outcomes Module #### Other Outcomes Description: Patient's Global Impression of Change scale Measure: Global Impression of Change Time Frame: 5, 8, 16 weeks Description: Concomitant medication and intervention use via self-reported questionnaire Measure: Concomitant medication and intervention use Time Frame: 5, 8, 16 weeks Description: measured as number of days with 'bothersome' and 'intolerable' pain in past week Measure: Pain Bothersomeness Time Frame: 1, 2, 3, 4, 5, 8, 16 weeks Description: measured as number of days with 'intolerable' pain in past week Measure: Pain Intolerability Time Frame: 1, 2, 3, 4, 5, 8, 16 weeks Description: Participant feedback form and semi-structured interviews on NeuOst and trial-related aspects Measure: Participant experiences Time Frame: 16 weeks #### Primary Outcomes Description: Using pre-defined set of feasibility criteria, measuring recruitment, consent rates, treatment completion, retention rates, interventionist fidelity in treatment delivery, treatment acceptability, blinding success, data completeness, adverse events, and participant acceptability. Measure: Study Feasibility Time Frame: 12 months from recruitment start #### Secondary Outcomes Description: measured on the Brief Pain Inventory (Short Form) Measure: Pain intensity (average in past week) Time Frame: 1, 2, 3, 4, 5, 8, 16 weeks Description: measured on the Diabetic Peripheral Neuropathic Pain Impact (DPNPI) measure Measure: Impact of Diabetic Neuropathic Pain Time Frame: 5, 8, 16 weeks Description: Neuropathy- and foot ulcer-specific quality of life instrument (NeuroQoL) Measure: Neuropathy- and Foot Ulcer-Specific Quality of Life Time Frame: 5, 8, 16 weeks Description: Falls Efficacy Scale (FES-I, short form) Measure: Fear of Falling Time Frame: 5, 8, 16 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Medical diagnosis of diabetes mellitus (type 1 or type 2) as per patient self-report. * Distal symmetrical peripheral neuropathy (defined as a score of ≥4 on the Michigan Neuropathy Screening Instrument (questionnaire part) (Herman et al., 2012)). * Neuropathic pain as assessed by DN4 questionnaire (defined as a score of ≥3 of 7 self-reported items) (Spallone et al., 2012). * Stable analgesic medication regimen for at least 3 weeks prior to anticipated study enrolment and no revision of regimen planned within the next 3 months. * Stable attendance of out-of-study nonpharmacological therapies for neuropathic pain or professional exercise programmes (including gym classes and manual therapy) for at least 3 weeks prior to anticipated study enrolment and no revision of routine planned within the next 3 months. * Participants capable of giving informed consent themselves. * Participants able to speak, understand, and read English at conversational levels. * Age: 18 and older. Exclusion Criteria: * Contraindications to manual therapy and conservative pain management (as determined by recruiting staff during screening calls or the trial provider at the initial or any other appointment; May include medical emergencies and suspected severe pathology, advanced osteoporosis, and active foot ulcerations) * Past or scheduled amputations * Advanced renal failure * Recent physical trauma and suspected fracture * Currently experiencing severe depressive or other current and severe psychopathology such as bipolar/psychosis, and/or presenting with active suicidal risk * Carpal Tunnel Syndrome diagnosis or symptoms as the only source of neuropathic pain * Unable or unwilling to provide consent for study participation * Unable to attend in-person appointments at treatment site (for health reasons) * Unable to attend in-person appointments at treatment site (for organisational reasons) * Knowing other participants signed up to the study (to avoid group contamination) * Concomitant participation in another clinical intervention study * Changes in medication or physical activity programmes in the past 1 month or planned for the next 3 months. Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: David Hohenschurz-Schmidt, PhD Phone: +44 (0)20 7089 5330 Role: CONTACT Contact 2: Email: [email protected] Name: Steven Vogel, DO Phone: +44 (0)20 7089 5330 Role: CONTACT #### Locations Location 1: City: London Contacts: *Contact 1:* - Email: [email protected] - Name: David Hohenschurz-Schmidt, PhD - Role: CONTACT Country: United Kingdom Facility: University College of Osteopathy Status: RECRUITING Zip: SE1 1HX #### Overall Officials Official 1: Affiliation: University College of Osteopathy / Imperial College London Name: David Hohenschurz-Schmidt, PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: Anyone can access Description: The sharing of trial data, specifically anonymised individual patient data and summary data, is permissible once the final report of all analyses specified in this report has been published in a scientific journal. External parties can request access to this dataset or the dataset may be shared on an online repository (OSF.io). Info Types: - STUDY_PROTOCOL - SAP - ICF - CSR - ANALYTIC_CODE IPD Sharing: YES Time Frame: Once the final report of all analyses specified in this report has been published in a scientific journal. URL: https://osf.io/sbqce/ ### References Module #### See Also Links Label: Full protocol (embargoed until Nov 2024) URL: https://osf.io/sbqce/ Label: Study website URL: https://www.uco.ac.uk/NeuOst ## Document Section ### Large Document Module #### Large Docs - Date: 2024-03-20 - Filename: ICF_000.pdf - Has ICF: True - Has Protocol: False - Has SAP: False - Label: Informed Consent Form - Size: 120443 - Type Abbrev: ICF - Upload Date: 2024-05-08T16:00 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000010523 - Term: Peripheral Nervous System Diseases - ID: D000009468 - Term: Neuromuscular Diseases - ID: D000009422 - Term: Nervous System Diseases - ID: D000009461 - Term: Neurologic Manifestations - ID: D000048909 - Term: Diabetes Complications - ID: D000003920 - Term: Diabetes Mellitus - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases ### Condition Browse Module - Browse Leaves - ID: M7124 - Name: Diabetic Neuropathies - Relevance: HIGH - As Found: Diabetic Neuropathy - ID: M13066 - Name: Pain - Relevance: HIGH - As Found: Painful - ID: M13432 - Name: Peripheral Nervous System Diseases - Relevance: LOW - As Found: Unknown - ID: M12411 - Name: Neuromuscular Diseases - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M26004 - Name: Diabetes Complications - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003929 - Term: Diabetic Neuropathies - ID: D000010146 - Term: Pain ### Intervention Browse Module - Browse Branches - Abbrev: Analg - Name: Analgesics - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M4032 - Name: Analgesics - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423378 Brief Title: Bio-Integrative, Fiber-Reinforced Kneebar for Treating Subchondral Insufficiency of the Knee Official Title: Bio-Integrative, Fiber-Reinforced Kneebar for Treating Subchondral Insufficiency of the Knee #### Organization Study ID Info ID: OSSIOfiber Kneebar #### Organization Class: OTHER Full Name: Vanderbilt University Medical Center ### Status Module #### Completion Date Date: 2025-12-03 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-12-03 Type: ESTIMATED #### Start Date Date: 2024-06-03 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-07 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Vanderbilt University Medical Center #### Responsible Party Investigator Affiliation: Vanderbilt University Medical Center Investigator Full Name: Lance LeClere Investigator Title: Dr. Lance LeClere, MD; Principal Investigator, Associate Professor Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: True Is FDA Regulated Drug: False Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: The OSSIOfiber® Trimmable Fixation Nails are indicated for maintenance of alignment and fixation of bone fractures, osteotomies, arthrodesis and bone grafts in the presence of appropriate additional immobilization (e.g., rigid fixation implants, cast, brace). Our hypothesis is that the use of OSSIOfiber® Trimmable Fixation Nails for treating subchondral insufficiency of the knee will result in improvement of patient-reported outcomes and imaging findings. The primary objective of this study is to evaluate the effectiveness of implanting bio-integrative OSSIOfiber® Trimmable Fixation Nails, organized in a bi-cortical rafter formation within the tibia or femur for the management of subchondral insufficiency. The OSSIOfiber® Trimmable Fixation Nails used in this study will be considered on-label. ### Conditions Module Conditions: - Subchondral Insufficiency Fracture ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 10 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module ### Interventions #### Intervention 1 Description: Subjects will be treated with cannulated nails before or after arthroscopic management of their concomitant pathology at the discretion of the investigator. Technique described below. Following nail placement, tissue layers will be closed in standard fashion. 1. Preop MRI views used to estimate the proper depth \& location of nail placement on the femur and/or tibia 2. Exposure is gained to medial tibia 3. 1.4 mm K-Wire is placed through medial tibia parallel to the articular joint surface \~ 1 cm distal to the articular joint line 4. A depth gauge is placed over K-Wire to determine required length of cannulated nail 5. A 4.0 mm cannulated drill bit used over K-Wire to prepare the pilot hole 6. Tamp is used to insert pre-trimmed 4.0 mm cannulated nail into the pilot hole and K-Wire is subsequently removed 7. Intraop fluoroscopy can confirm adequate nail placement prior to removing K-wire 8. Repeat steps for additional nails Name: OSSIOfiber® Trimmable Fixation Nails Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: The overall KOOS score combines pain and function domains. KOOS is out 100, where 0 equates to extreme pain and 100 equates to no pain. Measure: Knee injury and Osteoarthritis Outcome Score (KOOS) Time Frame: 3 months post-operatively Description: The overall KOOS score combines pain and function domains. KOOS is out 100, where 0 equates to extreme pain and 100 equates to no pain. Measure: Knee injury and Osteoarthritis Outcome Scale Score (KOOS) Time Frame: 6 months post-operatively #### Secondary Outcomes Description: Measures the knee health of individuals following surgery Measure: Knee injury and Osteoarthritis Outcome Score for Joint Replacement (KOOS, JR.) Time Frame: 6 months post-operatively Description: IKDC measures: symptoms, athletic activity, and knee function. Measure: International Knee Documentation Committee (IKDC) Subjective Knee Evaluation Form Time Frame: 6 months post-operatively Description: VR-12 combines measures of general health perceptions, physical functioning, role limitations due to physical and emotional problems, bodily pain, fatigue , social functioning, and mental health Measure: Veterans Rand-12 (VR-12) Health Survey Scale Score Time Frame: 6 months post-operatively Description: Measures a subject's perceived pain level. This score is usually on a scale of 0-10 with 0 equating to no pain and 10 equating to the worst pain imaginable. Measure: Numeric Pain Reported Scale Score Time Frame: 6 months post-operatively Description: Measures what level pain hinders a patient's engagement in several activities including social, cognitive, physical, and recreational activities. There are 7 sub items and each are rated from a scale of 0-10 where 0 means it does not interfere and 10 means it completely interferes. These contribute to a final score ranging anywhere from 0-70. Measure: PROMIS Pain Interference Score Time Frame: 6 months post-operatively Description: Measures self-reported negative mood (sadness, guilt), views of self (self- criticism, worthlessness), and social cognition (loneliness, interpersonal alienation), as well as decreased positive affect and engagement (loss of interest, meaning, and purpose). Each item on the measure is rated on a 5-point scale (1=never; 2=rarely; 3=sometimes; 4=often; and 5=always) with a range in score from 8 to 40. Higher scores indicate greater severity of depression. Measure: PROMIS Depression Score Time Frame: 6 months post-operatively Description: Measures the level of physical function for patients with a wide variety of impairments that may limit the patient's physical capability. This score is on a scale from 0-100 with 0 equating to no physical function and 100 equating to optimal physical function. Measure: PROMIS Physical Function Score Time Frame: 6 months post-operatively Description: Assessment of the incidence of re-operations, revision surgeries, or additional management of the study knee outside of postoperative rehabilitation. Measure: Incidence Assessments Time Frame: Up to 6 month post-operatively Description: To see how the knee ligament is healing by MRI assessment. Measure: Degree of knee ligament healing Time Frame: Baseline and 6 months post-operatively Description: Rate of postoperative adverse events and complications Measure: Adverse Events Time Frame: Up to 6 month post-operatively ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Agree to study participation and consent obtained. * Able to attend all postoperative clinical visits, undergo imaging procedures, and complete relevant questionnaires. * Subjects between the ages of 18 to 75 years. * Body Mass Index \< 40. * Has knee pain in the study knee lasting at least 3 months and has had at least moderate pain recorded on a standard of care (SOC) preoperative Knee Injury and Osteoarthritis Outcome Score (KOOS) and/or Numeric Pain Reported Scale (0-10) questionnaire. The study team may utilize these verbal pain scores collected during the clinic intake process for screening purposes. If the patient was not administered the verbal pain score, the patient will be consented, administered the pain survey, and withdrawn if moderate pain score was not recorded. * At least 3-months without steroid injection or any other non-surgical intervention administered to study knee. * Candidate for knee arthroscopy due to meniscal tear, loose body, unstable articular cartilage or mechanical symptoms. * Uni-compartmental Kellgren-Lawrence grade 2-3 osteoarthritis in the study tibia or femur. * Bone Marrow Lesion (BML) confirmed on magnetic resonance imaging in the femur, tibia or both. * Cartilage lesion on the tibial or femoral condyle(s) of a grading ≤4 by either the International Cartilage Repair Society or Outerbridge classifications verified at the time of arthroscopy. Exclusion Criteria: * Imaging evidence of the study knee that includes any of the following: 1. Kellgren-Lawrence grade 4 osteoarthritis. 2. Collapse of subchondral bone. 3. Avascular Necrosis (AVN). 4. Osteochondral defect overlying the BML 5. BML located at ACL or PCL insertions * Clinical evidence of the study knee that includes any of the following: 1. History of rheumatoid arthritis, septic arthritis, reactive arthritis, gout or pseudogout, secondary arthropathy (e.g., hemochromatosis, hemophilia, or psoriasis). 2. Osteochondritis dissecans. 3. Frank ligamentous instability. 4. Neuromuscular deficiency or other that would limit the ability to do a functional assessment. * Bi-cortical nail implantation cannot be achieved, including where the required nail length is not yet available. * Current tobacco use or has quit within 3 months of study enrolment. * Substance abuse history. * Diabetes mellitus, HbA1c\>8 * High surgical risk due to pre-existing conditions. * Currently pregnant or has plans to become pregnant prior to surgery. * Active infection or history of chronic infection in study knee. * Will require concomitant procedures within study knee, including but not limited to ligament reconstruction, tendon repair, meniscus repair, microfracture, osteotomy, or osteochondral transplantation (Meniscal tears, including chronic, are acceptable if no repair is required) * Significant malalignment (varus or valgus) of the knee (\>8°) * Use of augmentation or concomitant biologic therapy during surgery. * Contraindications to magnetic resonance imaging. * Any condition which in the view of the treating physician makes it inadvisable for the subject to participate in the study. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Lindsey Agnew, MS Phone: 6158751996 Role: CONTACT ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000050723 - Term: Fractures, Bone - ID: D000014947 - Term: Wounds and Injuries ### Condition Browse Module - Browse Branches - Abbrev: BC26 - Name: Wounds and Injuries - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M26370 - Name: Fractures, Bone - Relevance: LOW - As Found: Unknown - ID: M18332 - Name: Fractures, Stress - Relevance: HIGH - As Found: Insufficiency Fractures - ID: M17685 - Name: Wounds and Injuries - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000015775 - Term: Fractures, Stress ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423365 Brief Title: A Tool to Help Patients With Muscle Symptoms After Taking a Statin Medication. Official Title: Development, Testing, and Implementation of Virtual Statin Associated Muscle Symptom Management #### Organization Study ID Info ID: R01HL157439 Link: https://reporter.nih.gov/quickSearch/R01HL157439 Type: NIH #### Organization Class: OTHER Full Name: University of Utah ### Status Module #### Completion Date Date: 2026-07-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-22 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-07-01 Type: ESTIMATED #### Start Date Date: 2024-07-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-20 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Kaiser Permanente #### Lead Sponsor Class: OTHER Name: University of Utah #### Responsible Party Investigator Affiliation: University of Utah Investigator Full Name: Jordan King Investigator Title: Assistant Professor Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The goal of this clinical trial is to learn if an educational website can help patients make an informed decision and engage in shared decision-making with their healthcare provider regarding cholesterol lowering medication use after they have stopped statin therapy due to self-reported muscle symptoms from taking a statin medication. The main questions the trial aims to answer are: 1. Compared to usual care, are patients who engage with the website after experiencing statin-associated muscle symptoms (SAMS) more likely to retry statin therapy? 2. Compared to usual care, are patients who retry statin therapy after engaging with the website more likely to persist on statin therapy? Researchers will compare people randomized to use the website to those who are receiving usual care to see if statin re-start and persistence rates change. All participants will take baseline questionnaires and receive usual care as they would if they were not in the study (e.g., visit their doctor, get labs drawn, take medication as prescribed). Patients randomized to the website arm will be asked to engage with content in a website which is anticipated to take most patients approximately 30-minutes. Their clinician will then contact them for a follow-up visit as needed. ### Conditions Module Conditions: - Hydroxymethylglutaryl-CoA Reductase Inhibitors - Hypercholesterolemia - Cardiovascular Diseases - Pharmacists - Placebo Effect ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: HEALTH_SERVICES_RESEARCH #### Enrollment Info Count: 816 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants randomized to usual care will continue to receive usual care at Kaiser Permanente Colorado as they would under normal, non-study conditions. Label: Usual care Type: NO_INTERVENTION #### Arm Group 2 Description: Participants randomized to usual care + virtual statin management (VSM) will continue to receive usual care at Kaiser Permanente Colorado as they would under normal, non-study conditions, and they will also be given a link to engage with the VSM website. The VSM website is an educational tool which has four principal components: 1) learning how to distinguish if and when muscle symptoms are caused by the statin; 2) learning the essentials about heart disease, focusing on causes, risk factors, and the crucial role of cholesterol management in prevention; exploring various cholesterol lowering options, including when it makes sense to retry a statin and what options exist beyond statins; and 4) learning to engage in productive discussions with healthcare providers and set effective treatment goals together. Intervention Names: - Other: Virtual Statin Management (VSM) Label: Usual Care + Virtual Statin Management (VSM) Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Usual Care + Virtual Statin Management (VSM) Description: VSM is a web-based decision aid to help manage statin therapy after experiencing muscle pain perceived to be caused or worsened by their statin therapy. The introduction will feature a brief explanation of the tool and what they can expect. The modules are: 1. General education (lipids, heart disease, medications) 2. Side effects (causes, diagnosis). 3. Statin modifications. VSM will guide patients to understand their lipid-lowering options, particularly their statin options that may best match patients' stated preferences. 4. ASCVD risk \& statin benefit. Finally, the VSM experience will end by providing the patient with a summary of the results of their use of the tool, which can be used during discussions with their healthcare provider. The information gathered from the VSM will remain confidential and will not be disclosed to anyone other than the patient. Name: Virtual Statin Management (VSM) Type: OTHER ### Outcomes Module #### Other Outcomes Description: Assessed using two questions inspired by the Treatment Satisfaction with Medication Questionnaire. Participants the degree to which they agree or disagree (5-point Likert) regarding their satisfaction with cholesterol-lowering medication. Measure: Proportion of participants satisfied with their treatment Time Frame: 6 months post-enrollment Description: Assessed using the Decisional Conflict Scale, 10-item, 3-response (https://decisionaid.ohri.ca/docs/develop/Tools/DCS_LowLiteracy_English.pdf). Participants indicate "yes", "unsure", or "no" to 10 questions assessing their decisional conflict regarding their decision to use cholesterol-lowering medication. Measure: Participant-reported decisional conflict Time Frame: 1 month post-enrollment Description: Measured using the Decision Self-Efficacy Scale, 11-item, 3-response (https://decisionaid.ohri.ca/docs/develop/User_Manuals/UM_Decision_SelfEfficacy.pdf). Participants indicate their level of confidence from 0 (not at all confident) to 4 (very confident) regarding their decision to use cholesterol-lowering medication. Measure: Participant-reported decision self-efficacy Time Frame: 6 months post-enrollment Description: Adapted from 3 questions used in the Prospective Assessment of Lipid Management (PALM) registry (https://classic.clinicaltrials.gov/ct2/show/NCT02341664). Participants indicate their perceived risk for having a heart disease event. Measure: Participant-reported perception of cardiovascular disease risk Time Frame: 6 months post-enrollment Description: Measured using the Trust in Physician Scale, 11-item (https://pubmed.ncbi.nlm.nih.gov/2084735/). Participants indicate the degree to which they agree or disagree (5-point Likert scale) with statements regarding their trust in healthcare personnel. Measure: Participant-reported degree of trust in healthcare Time Frame: 6 months post-enrollment Description: Participants indicate the degree to which they agree or disagree with 18 statements regarding potential statin-related harms or conspiracies. Answer options of strongly disagree, disagree, neither agree nor disagree, agree, strongly agree, or Not sure. Agreement with the statement indicates a negative belief about statins. Measure: Participant-reported statin conspiracy beliefs Time Frame: 6 months post-enrollment Description: Measured using the Decision Regret Scale, 5-item, 5-response (https://decisionaid.ohri.ca/docs/develop/User_Manuals/UM_Regret_Scale.pdf). Participant indicate the degree to which they agree or disagree (5-point Likert Scale) with 5 statements regarding their choice to use cholesterol-lowering medication. Measure: Participant-reported decision regret Time Frame: 6 months post-enrollment #### Primary Outcomes Description: Measured using pharmacy dispensing records Measure: Number of participants who retry statin therapy Time Frame: 30 days post-enrollment Description: Measured using pharmacy dispensing records Measure: Number of participants who continue to take statin therapy Time Frame: 6 months post-enrollment #### Secondary Outcomes Description: Measured using pharmacy dispensing records, using the proportion of days' covered calculation metric (range: 0-100%, where 100% means perfectly adherent) Measure: How adherent participants are to prescribed statin therapy Time Frame: 6 months post-enrollment ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * KPCO member * Sold a statin from KPCO pharmacy in the previous six months * Have a gap of \>1.0x the days' supply in refilling their statin * Patient who stopped therapy (or delayed filling prescription) due to some perceived side effect * Has email address available in kp.org (and therefore has access to a computer with internet) Exclusion Criteria: * Unable to verbalize comprehension of study or impaired decision-making * Non-English speaking * Limited life expectancy (e.g. hospice or palliative care) * Pregnant or planning to become pregnant * Patients on Kaiser Permanente's "do not call" list for research will also be excluded. Healthy Volunteers: True Maximum Age: 80 Years Minimum Age: 21 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Jordan B King, PharmD, MS Phone: 801-213-8797 Role: CONTACT Contact 2: Email: [email protected] Name: Catherine G Derington, PharmD, MS Phone: 303-550-1980 Role: CONTACT #### Overall Officials Official 1: Affiliation: University of Utah Name: Jordan B King, PharmD, MS Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000006949 - Term: Hyperlipidemias - ID: D000050171 - Term: Dyslipidemias - ID: D000052439 - Term: Lipid Metabolism Disorders - ID: D000008659 - Term: Metabolic Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M9988 - Name: Hypercholesterolemia - Relevance: HIGH - As Found: Hypercholesterolemia - ID: M10000 - Name: Hyperlipidemias - Relevance: LOW - As Found: Unknown - ID: M10002 - Name: Hyperlipoproteinemias - Relevance: LOW - As Found: Unknown - ID: M26181 - Name: Dyslipidemias - Relevance: LOW - As Found: Unknown - ID: M11639 - Name: Metabolic Diseases - Relevance: LOW - As Found: Unknown - ID: M27029 - Name: Lipid Metabolism Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000006937 - Term: Hypercholesterolemia ### Intervention Browse Module - Browse Branches - Abbrev: Lipd - Name: Lipid Regulating Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M21155 - Name: Hydroxymethylglutaryl-CoA Reductase Inhibitors - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423352 Brief Title: A Study to Evaluate Zilebesiran in Japanese Patients With Mild to Moderate Hypertension Official Title: A Phase 1/2, Randomized, Double-blind, Placebo-Controlled, Parallel-Group Study to Evaluate the Safety, Tolerability, Efficacy, Pharmacodynamics, and Pharmacokinetics of Zilebesiran in Japanese Patients With Mild to Moderate Hypertension #### Organization Study ID Info ID: ALN-AGT01-006 #### Organization Class: INDUSTRY Full Name: Alnylam Pharmaceuticals ### Status Module #### Completion Date Date: 2025-09-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-09-30 Type: ESTIMATED #### Start Date Date: 2024-06-07 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-20 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Alnylam Pharmaceuticals #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Is US Export: True ### Description Module Brief Summary: The purpose of this study is to evaluate the safety, tolerability, efficacy, pharmacodynamics (PD) and pharmacokinetics (PK) of zilebesiran in Japanese patients with mild to moderate hypertension. ### Conditions Module Conditions: - Mild to Moderate Hypertension Keywords: - High blood pressure - Hypertension - Hypertensive - siRNA - Angiotensinogen - AGT ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: TRIPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR Primary Purpose: TREATMENT #### Enrollment Info Count: 36 Type: ESTIMATED Phases: - PHASE1 - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants will be administered a single dose of zilebesiran. Intervention Names: - Drug: Zilebesiran Label: Zilebesiran Type: EXPERIMENTAL #### Arm Group 2 Description: Participants will be administered a single dose of placebo. Intervention Names: - Drug: Placebo Label: Placebo Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Zilebesiran Description: Zilebesiran administered by subcutaneous (SC) injection Name: Zilebesiran Other Names: - ALN-AGT01 Type: DRUG #### Intervention 2 Arm Group Labels: - Placebo Description: Placebo administered by SC injection Name: Placebo Type: DRUG ### Outcomes Module #### Primary Outcomes Measure: Frequency of Adverse Events (AEs) Time Frame: Up to 12 months #### Secondary Outcomes Measure: Percent Change from Baseline in Serum Angiotensinogen (AGT) at Month 3 and Month 6 Time Frame: Baseline and Month 3 and Month 6 Measure: Change from Baseline at Month 3 and Month 6 in 24-hour Mean Systolic Blood Pressure (SBP) and Diastolic Blood Pressure (DBP) Assessed by Ambulatory Blood Pressure Monitoring (ABPM) Time Frame: Baseline and Month 3 and Month 6 Measure: Change from Baseline at Month 3 and Month 6 in SBP and DBP Assessed by Office Blood Pressure Time Frame: Baseline and Month 3 and Month 6 Measure: Pharmacokinetics of Zilebesiran and its Metabolite assessed by Plasma Concentration Time Frame: Predose and up to 3 days postdose ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Must have been born in Japan, and their biological parents and grandparents must have been of Japanese origin * Has mean systolic office blood pressure (SBP) of \>130 and \<=165 mmHg by automated office blood pressure measurement, after a minimum of 3 weeks of washout if taking hypertensive medication * Has 24-hour mean SBP ≥130 mmHg by ambulatory blood pressure monitoring (ABPM), without antihypertensive medication Exclusion Criteria: * Has secondary hypertension, symptomatic orthostatic hypotension * Has alanine aminotransferase (ALT) or aspartate aminotransferase (AST) \>2× upper limit of normal (ULN) * Has elevated serum potassium \>5 mmol/L * Has estimated glomerular filtration rate (eGFR) of \<60 mL/min/1.73m\^2 * Has received an investigational agent within the last 30 days * Has Type 1 diabetes mellitus, poorly controlled Type 2 diabetes mellitus or newly diagnosed Type 2 diabetes mellitus * Has history of intolerance to SC injection(s) Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Alnylam Clinical Trial Information Line Phone: 1-877-ALNYLAM Role: CONTACT Contact 2: Email: [email protected] Name: Alnylam Clinical Trial Information Line Phone: 1-877-256-9526 Role: CONTACT #### Overall Officials Official 1: Affiliation: Alnylam Pharmaceuticals Name: Medical Director Role: STUDY_DIRECTOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000014652 - Term: Vascular Diseases - ID: D000002318 - Term: Cardiovascular Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M10024 - Name: Hypertension - Relevance: HIGH - As Found: Hypertension - ID: M17400 - Name: Vascular Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000006973 - Term: Hypertension ### Intervention Browse Module - Browse Branches - Abbrev: VaCoAg - Name: Vasoconstrictor Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M4132 - Name: Angiotensin II - Relevance: LOW - As Found: Unknown - ID: M4135 - Name: Angiotensinogen - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423339 Brief Title: Comparison Between Genicular Nerve Block Combined With (IPACK) Block Versus Adductor Canal Block Official Title: A Comparative Study Between Ultrasound Guided Genicular Nerve Block Combined With Interspace Between the Popliteal Artery and the Capsule of the Posterior Knee Block Versus Adductor Canal Block in Total Knee Replacement #### Organization Study ID Info ID: FAMSU R80/2024 #### Organization Class: OTHER Full Name: Ain Shams University ### Status Module #### Completion Date Date: 2024-11 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-11 Type: ESTIMATED #### Start Date Date: 2024-05-10 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-27 Study First Submit QC Date: 2024-05-20 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Ain Shams University #### Responsible Party Investigator Affiliation: Ain Shams University Investigator Full Name: riham fathy galal Investigator Title: Lecturer Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The patients will be randomized into 2 groups, named group A, B. Group A: The patients will receive Ultrasound guided Genicular nerves block combined with Ultrasound guided IPACK block. Group B: The patients will receive Adductor canal block which will be the control group. The Numerical Rating Scale (NRS) will be used to assess pain intensity. Preoperatively, all study subjects will be trained to use NRS pain scores. The spinal block will be performed. In group A, 15 mL of bupivacaine 0.25% with 2.5 g/mL adrenaline at a concentration 1:4,00,000 will be administered immediately following skin closure. GNB will be performed by using the linear ultrasound probe (10-15 MHz) Sono site M-turbo ultrasonography to scan the long bone shaft with up and down movement to recognize the epicondyle of the tibia and femur. The junctions between the epicondyle and the shafts of the femur and tibia are where the genicular arteries are located; these junctions will be defined as the periosteal areas. The superior lateral, superior medial and inferior medial genicular arteries accompany each genicular nerve. After confirmation of the genicular artery by color Doppler, the needle will be introduced using the in-plane approach and presented in the long axis view. The target point of the needle insertion will be the needle tip beside a genicular artery. Then, a 5 mL volume will be administered after gentle aspiration to prevent a faulty intra-arterial injection at 3 target locations: the superior lateral, superior medial and inferior medial genicular nerves. This will be Followed by the procedure for the IPACK block. In group B, A 22 Gauge 80 mm needle will be guided from lateral to medial to this area called the adductor canal using in-plane technique. 20 mL of 0.5% bupivacaine will be injected with peri-arterial spread after negative aspiration under sterile conditions. TKA will be performed by an orthopedic surgeon by placing three-compartment prostheses with a minimally invasive mini-midvastus approach and using hand-mixed cementing techniques. Detailed Description: The patients will be randomized into 2 equal groups by a computer-generated random numbers table, named group A, B. An independent data manager of computer generated software will be responsible for randomization, assigning the patients to the groups using sequentially numbered, sealed, opaque envelopes containing computer generated random numbers, accessible only to the anesthesiologist performing the block. The subjects will be randomly allocated to one of the two groups. Group A: The patients will receive Ultrasound guided Genicular nerves block combined with Ultrasound guided IPACK block. Group B: The patients will receive Adductor canal block which will be the control group. History taking, clinical examination and routine laboratory investigation will be performed preoperatively, and the patients will be instructed to fast for 8 hours preoperative for solids and 2 hours for clear fluids. On arrival to the operation room, intravenous access will be established and acetated ringer will be infused by rate 10ml/kg. ECG, noninvasive blood pressure and arterial oxygen saturation will be monitored routinely. The Numerical Rating Scale (NRS) will be used to assess pain intensity. Preoperatively, all study subjects will be trained to use NRS pain scores. In the operating room, a peripheral 20 G intravenous (IV) cannula will be inserted. The baseline parameters of five lead electrocardiogram (ECG), non invasive blood pressure and peripheral oxygen saturation will be recorded. IV midazolam 0.02 mg/kg will be administered. The spinal block will be performed using either a 25 or 27 G spinal needle in the sitting position at the L3-L4 or L4-L5 intervertebral space with a 2.5-3 mL hyperbaric bupivacaine 0.5%. The sensory block (to cold and pinprick) to the 10th thoracic dermatome or above will be the target of the spinal block to start the surgery. Hypotension will be defined as ≥20% decrease in blood pressure from baseline measurements and managed by IV Ephedrine6 mg boluses. In group A, 15 mL of bupivacaine 0.25% with 2.5 g/mL adrenaline at a concentration 1:4,00,000 will be administered immediately following skin closure. GNB will be performed by using the linear ultrasound probe (10-15 MHz) Sono site M-turbo ultrasonography to scan the long bone shaft with up and down movement to recognize the epicondyle of the tibia and femur. The junctions between the epicondyle and the shafts of the femur and tibia are where the genicular arteries are located; these junctions will be defined as the periosteal areas. The superior lateral, superior medial and inferior medial genicular arteries accompany each genicular nerve. After confirmation of the genicular artery by color Doppler, the needle will be introduced using the in plane approach and presented in the long axis view. The target point of the needle insertion will be the needle tip beside a genicular artery. Then, a 5 mL volume will be administered after gentle aspiration to prevent a faulty intra arterial injection at 3 target locations: the superior lateral, superior medial and inferior medial genicular nerves. This will be Followed by the procedure for the IPACK block initiated by the visualization of the popliteal artery and posterior surface of the distal femur. Then, the image of the femoral condyles and the popliteal artery will be obtained. A 20G 22G 80 mm needle will be inserted in a medial to the lateral plane, parallel to the femur in the middle area between the popliteal artery and the femur. 20 mL of the local anesthetic solution will be given into this space in increments, ensuring the adequate and equal distribution of the anesthetic agent. In group B, after placing the patients in the supine position, the linear probe of ultrasound (13-6 MHz) will be moved from cephalad to caudal and the superficial femoral artery will be visualized in the short axis, medial to the vastus medialis, lateral to the sartorius muscle, and anterior to the adductor magnus muscle. A 22 Gauge 80 mm needle will be guided from lateral to medial to this area called the adductor canal using in-plane technique. 20 mL of 0.5% bupivacaine will be injected to with peri-arterial spread after negative aspiration under sterile conditions. TKA will be performed by an orthopedic surgeon by placing three-compartment prostheses with a minimally invasive mini-midvastus approach and using hand-mixed cementing techniques. The outcome: The primary outcome will be the total postoperative morphine consumption during the first two postoperative days. NRS will be assessed at 0, 6, 12, 24 and 48 h postoperatively. The period between the end of surgery and the first request for rescue analgesia (NRS \>3) will be considered the time to the first request. Postoperative analgesia, IV paracetamol (1 g/6 h) and IV ketorolac (30 mg/12 h), will be administered to all patients. The pain will be assessed at rest and during movement using NRS (metric score 0-10 for pain severity assessment: mild pain = 1-3, moderate = 4-7 and severe = 8 and above) on the first and second days. When NRS will be \>3, rescue analgesia (morphine 3 mg IV) will be given and repeated whenever required. The secondary outcome will be assessment of Postoperative functional outcomes and knee rehabilitation parameters including quadriceps motor strength score measured by straight leg raising (SLR), knee range of motion (ROM) and time up and go (TUG) test. SLR will be assessed on a scale ranging from 0 to 5 as follows: 0 = unable to contract muscles, 1 = muscles twitch, the limb does not move, 2 = able to move the limb with gravity elimination and passive assistance, 3 = able to move the limb against gravity without resistance (no cuff weights weight wrapped around your thigh just above your kneecap), 4 = move the limb against some resistance (cuff weights weight wrapped around your thigh just above your kneecap) and 5 = normal motor strength against resistance. TUG is a performance test to measure functional mobility. The test requirements will be presented as the subject rises from a chair, walks 3.0 m easily to reach a mark placed on the floor, turns around at the 3.0 m mark, returns to the starting point and sits on the chair. The time the subject takes to complete the test is defined as the TUG score. Patients' movement with aid within 24 h will be encouraged when the motor strength was at least two. The postoperative patient satisfaction and incidence of adverse effects will be recorded. Patient satisfaction will be measured by a self administered satisfaction scale (very satisfied, somewhat satisfied, somewhat dissatisfied, very dissatisfied). ### Conditions Module Conditions: - Post Operative Pain ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: QUADRUPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: PREVENTION #### Enrollment Info Count: 50 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Group A will receive genicular nerve block combined with interspace between the popliteal artery and the capsule of the posterior knee block(IPACK) Intervention Names: - Procedure: Ultrasound guided Genicular nerve block - Procedure: Interspace between the popliteal artery and the capsule of the popliteal artery and the capsule of the posterior knee - Drug: Bupivacaine Hydrochloride Label: Group A Type: EXPERIMENTAL #### Arm Group 2 Description: Group B will receive ultrasound guided sub-sartorial Adductor canal block (ACB) Intervention Names: - Procedure: Adductor canal block - Drug: Bupivacaine Hydrochloride Label: Group B Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Group A Description: Ultrasound guided genicular nerve block Name: Ultrasound guided Genicular nerve block Type: PROCEDURE #### Intervention 2 Arm Group Labels: - Group A Description: Ultrasound guided Interspace between the popliteal artery and the capsule of the popliteal artery and the capsule of the posterior knee Name: Interspace between the popliteal artery and the capsule of the popliteal artery and the capsule of the posterior knee Type: PROCEDURE #### Intervention 3 Arm Group Labels: - Group B Description: Ultrasound guided sub-sartorial Adductor canal block Name: Adductor canal block Type: PROCEDURE #### Intervention 4 Arm Group Labels: - Group A - Group B Description: Pupivacaine 0.5% in 20 ml vial Name: Bupivacaine Hydrochloride Other Names: - Sunnypivacaine Type: DRUG ### Outcomes Module #### Primary Outcomes Description: The primary outcome will be the total postoperative morphine consumption during the first two postoperative days. Measure: The primary outcome will be the total postoperative morphine consumption during the first two postoperative days. Time Frame: 48 hours ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Patients American Society of anesthesiologists' physical status (ASA) I to III. 2. Aged 40 to 70 years. 3. Both sexes. 4. Patients scheduled for unilateral total knee replacement. Exclusion Criteria: 1. Patients with spinal malformation 2. Patients with liver impairment 3. Patients with renal impairment 4. Patients younger than 40 years or older than 70 years 5. Patients with hypersensitivity to one of the used drugs 6. Patients with neuromuscular disorders and 7. Coagulopathy disorders 8. Patients scheduled for revision knee arthroplasty or those who had a past history of previous surgery or trauma to the knee Maximum Age: 70 Years Minimum Age: 40 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Riham F. Galal, MD Phone: 01022739211 Phone Ext: +2 Role: CONTACT Contact 2: Email: [email protected] Name: Ahmad M Ehab, MD Phone: 01111897888 Phone Ext: +2 Role: CONTACT #### Locations Location 1: City: Cairo Contacts: *Contact 1:* - Email: [email protected] - Name: Riham F. Galal, MD - Phone: 01022739211 - Phone Ext: +2 - Role: CONTACT Country: Egypt Facility: Ain shams university hospitals Status: RECRUITING ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000011183 - Term: Postoperative Complications - ID: D000010335 - Term: Pathologic Processes - ID: D000010146 - Term: Pain - ID: D000009461 - Term: Neurologic Manifestations ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases ### Condition Browse Module - Browse Leaves - ID: M13069 - Name: Pain, Postoperative - Relevance: HIGH - As Found: Post Operative Pain - ID: M13066 - Name: Pain - Relevance: LOW - As Found: Unknown - ID: M14065 - Name: Postoperative Complications - Relevance: LOW - As Found: Unknown - ID: M12404 - Name: Neurologic Manifestations - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000010149 - Term: Pain, Postoperative ### Intervention Browse Module - Ancestors - ID: D000000779 - Term: Anesthetics, Local - ID: D000000777 - Term: Anesthetics - ID: D000002492 - Term: Central Nervous System Depressants - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000018689 - Term: Sensory System Agents - ID: D000018373 - Term: Peripheral Nervous System Agents ### Intervention Browse Module - Browse Branches - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M5315 - Name: Bupivacaine - Relevance: HIGH - As Found: IFN - ID: M4107 - Name: Anesthetics - Relevance: LOW - As Found: Unknown - ID: M4109 - Name: Anesthetics, Local - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000002045 - Term: Bupivacaine ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423326 Brief Title: Gemcitabine, Cisplatin and Nab-Paclitaxel as Neoadjuvant Treatment for Patients With Resectable or Borderline Resectable Pancreatic Cancer Official Title: A Single-Arm Phase II Clinical Trial of Gemcitabine, Cisplatin, and Nab-Paclitaxel as Neoadjuvant Therapy for Pancreatic Ductal Adenocarcinoma #### Organization Study ID Info ID: STUDY00006976 #### Organization Class: OTHER Full Name: Emory University #### Secondary ID Infos Domain: CTRP (Clinical Trial Reporting Program) ID: NCI-2024-02082 Type: REGISTRY Domain: Emory University Hospital/Winship Cancer Institute ID: WINSHIP6093-23 Type: OTHER ID: P30CA138292 Link: https://reporter.nih.gov/quickSearch/P30CA138292 Type: NIH Domain: Emory University Hospital/Winship Cancer Institute ID: STUDY00006976 Type: OTHER ### Status Module #### Completion Date Date: 2026-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-16 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-12-31 Type: ESTIMATED #### Start Date Date: 2024-07-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-10 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Collaborators Class: NIH Name: National Cancer Institute (NCI) #### Lead Sponsor Class: OTHER Name: Emory University #### Responsible Party Investigator Affiliation: Emory University Investigator Full Name: Mihir M. Shah, MD, FACS, FSSO Investigator Title: Principal Investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Is US Export: False ### Description Module Brief Summary: This phase II trial tests how well gemcitabine, cisplatin and nab-paclitaxel given before surgery (neoadjuvant) works in treating patients with pancreatic cancer that can be removed by surgery (resectable) or that is borderline resectable. The standard treatment for resectable and borderline resectable pancreatic cancer is a combination of surgery and chemotherapy. Neoadjuvant therapy has been shown to improve overall survival compared to patients receiving surgery first. Gemcitabine is a chemotherapy drug that blocks the cells from making DNA and may kill tumor cells. Cisplatin is in a class of medications known as platinum-containing compounds. It works by killing, stopping or slowing the growth of tumor cells. Nab-paclitaxel is an albumin-stabilized nanoparticle formulation of paclitaxel, an antimicrotubule agent that stops tumor cells from growing and dividing and may kill them. Nab-paclitaxel may have fewer side effects and work better than other forms of paclitaxel. Gemcitabine, cisplatin and nab-paclitaxel may be an effective neoadjuvant treatment option for patients with resectable or borderline resectable pancreatic cancer. Detailed Description: PRIMARY OBJECTIVE: I. Determine the major pathological response rate, feasibility and safety of biweekly gemcitabine, cisplatin and nab-paclitaxel (GCN) in the neoadjuvant setting for patients with resectable and borderline resectable pancreatic ductal adenocarcinoma. SECONDARY OBJECTIVE: I. Determine if neoadjuvant GCN increases tumoral infiltration of lymphocytes with local and systemic phenotypic features that assist in the antitumor immune response. OUTLINE: Patients receive nab-paclitaxel intravenously (IV) over 30 minutes, cisplatin IV over 60 minutes, and gemcitabine IV over 30 minutes on days 1 and 15 of each cycle. Treatment repeats every 28 days for up to 4 cycles in the absence of disease progression or unacceptable toxicity. Patients with stable disease, partial or complete response undergo surgical resection per standard of care. Additionally, patients undergo biopsy on study and undergo blood sample collection and computed tomography (CT) or magnetic resonance imaging (MRI) at pre-study and on study. After completion of study treatment, patients are followed up every 3-4 months for up to 24 months. ### Conditions Module Conditions: - Borderline Resectable Pancreatic Ductal Adenocarcinoma - Resectable Pancreatic Adenocarcinoma - Stage I Pancreatic Cancer AJCC v8 - Stage II Pancreatic Cancer AJCC v8 - Stage III Pancreatic Cancer AJCC v8 ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 44 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients receive nab-paclitaxel IV over 30 minutes, cisplatin IV over 60 minutes, and gemcitabine IV over 30 minutes on days 1 and 15 of each cycle. Treatment repeats every 28 days for up to 4 cycles in the absence of disease progression or unacceptable toxicity. Patients with stable disease, partial or complete response undergo surgical resection per standard of care. Additionally, patients undergo biopsy on study and undergo blood sample collection and CT or MRI at pre-study and on study. Intervention Names: - Procedure: Biopsy - Procedure: Biospecimen Collection - Drug: Cisplatin - Procedure: Computed Tomography - Drug: Gemcitabine - Procedure: Magnetic Resonance Imaging - Drug: Nab-paclitaxel - Procedure: Pancreatic Surgical Procedure Label: Treatment (nab-paclitaxel, cisplatin, gemcitabine) Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Undergo biopsy Name: Biopsy Other Names: - BIOPSY_TYPE - Bx Type: PROCEDURE #### Intervention 2 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Undergo blood sample collection Name: Biospecimen Collection Other Names: - Biological Sample Collection - Biospecimen Collected - Specimen Collection Type: PROCEDURE #### Intervention 3 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Given IV Name: Cisplatin Other Names: - Abiplatin - Blastolem - Briplatin - CDDP - Cis-diammine-dichloroplatinum - Cis-diamminedichloridoplatinum - Cis-diamminedichloro Platinum (II) - Cis-diamminedichloroplatinum - Cis-dichloroammine Platinum (II) - Cis-platinous Diamine Dichloride - Cis-platinum - Cis-platinum II - Cis-platinum II Diamine Dichloride - Cismaplat - Cisplatina - Cisplatinum - Cisplatyl - Citoplatino - Citosin - Cysplatyna - DDP - Lederplatin - Metaplatin - Neoplatin - Peyrone's Chloride - Peyrone's Salt - Placis - Plastistil - Platamine - Platiblastin - Platiblastin-S - Platinex - Platinol - Platinol- AQ - Platinol-AQ - Platinol-AQ VHA Plus - Platinoxan - Platinum - Platinum Diamminodichloride - Platiran - Platistin - Platosin Type: DRUG #### Intervention 4 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Undergo CT Name: Computed Tomography Other Names: - CAT - CAT Scan - Computed Axial Tomography - Computerized Axial Tomography - Computerized axial tomography (procedure) - Computerized Tomography - Computerized Tomography (CT) scan - CT - CT Scan - tomography Type: PROCEDURE #### Intervention 5 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Given IV Name: Gemcitabine Other Names: - dFdC - dFdCyd - Difluorodeoxycytidine Type: DRUG #### Intervention 6 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Undergo MRI Name: Magnetic Resonance Imaging Other Names: - Magnetic Resonance - Magnetic Resonance Imaging (MRI) - Magnetic resonance imaging (procedure) - Magnetic Resonance Imaging Scan - Medical Imaging, Magnetic Resonance / Nuclear Magnetic Resonance - MR - MR Imaging - MRI - MRI Scan - MRIs - NMR Imaging - NMRI - Nuclear Magnetic Resonance Imaging - sMRI - Structural MRI Type: PROCEDURE #### Intervention 7 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Given IV Name: Nab-paclitaxel Other Names: - ABI 007 - ABI-007 - Abraxane - Albumin-bound Paclitaxel - Albumin-Stabilized Nanoparticle Paclitaxel - Nanoparticle Albumin-bound Paclitaxel - Nanoparticle Paclitaxel - Paclitaxel Albumin - paclitaxel albumin-stabilized nanoparticle formulation - Paclitaxel Nanoparticle Albumin-bound - Paclitaxel Protein-Bound - Protein-bound Paclitaxel Type: DRUG #### Intervention 8 Arm Group Labels: - Treatment (nab-paclitaxel, cisplatin, gemcitabine) Description: Undergo surgical resection Name: Pancreatic Surgical Procedure Other Names: - Pancreatic Surgery Type: PROCEDURE ### Outcomes Module #### Primary Outcomes Description: Pathologic response rate will be defined by College of American Pathologists scoring system as 0 (complete response), 1 (near complete response), 2 (partial response) and 3 (poor or no response). Pathologic response rate will be reported as a proportion of 0 and 1, with and exact 90% confidence interval estimated using the Clopper-Pearson method. Measure: Pathologic response rate Time Frame: At time of surgery #### Secondary Outcomes Description: Feasibility will be defined as completion of all preoperative and operative therapy. Treatment completion will reported as a proportion, with an exact 95% confidence interval estimated using the Clopper-Pearson method. Measure: Treatment completion Time Frame: Up to 24 months Description: AEs, with severity will be graded using National Cancer Institute Common Terminology Criteria for Adverse Events version 5.0. Descriptive statistics will be reported, using frequencies and percentages for each toxicity. Measure: Incidence of adverse events (AEs) Time Frame: Up to 28 days after last dose of study treatment Description: Radiological response rate will be defined as complete response, partial response or stable disease after study treatment evaluated using Response Evaluation Criteria in Solid Tumors version 1.1. Radiologic response rate will be reported as a proportion, with an exact 95% confidence interval estimated using the Clopper-Pearson method. Measure: Radiologic response rate Time Frame: Up to 24 months Description: R0 resection indicates a microscopically margin-negative resection. R0 resection rate will reported as a proportion, with an exact 95% confidence interval estimated using the Clopper-Pearson method. Measure: R0 resection rate Time Frame: At time of surgery Description: N0, N1, and N2 will be reported using frequencies and percentages. Measure: Nodal status Time Frame: Up to 24 months Description: RFS will be estimated using the Kaplan-Meier method, and a 95% confidence interval for median RFS will be estimated using the Brookmeyer-Crowley approach. Measure: Recurrence-free survival (RFS) Time Frame: From surgery to recurrence or death, assessed up to 24 months Description: OS will be estimated using the Kaplan-Meier method, and median survival will be calculated. A 95% confidence interval will be estimated using the Brookmeyer-Crowley approach. Measure: Overall survival (OS) rate Time Frame: From study treatment start to date of death, assessed up to 24 months Description: CA19-9 response will be defined as \> 50% decrease from baseline will be correlated with tumor response. CA19-9 will be reported as a proportion, with an exact 95% confidence interval estimated using the Clopper-Pearson method. CA19-9 will be correlated with RFS and OS using log-rank tests and Cox proportional hazards regression. Model assumptions will be checked and verified. Measure: Carbohydrate antigen (CA)19-9 response Time Frame: Up to 24 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Histologically or cytologically confirmed - resectable and borderline resectable pancreatic ductal adenocarcinoma * Resectability will be defined as per National Comprehensive Cancer Network (NCCN) guidelines using cross-sectional imaging (contrast-enhanced computed tomography or magnetic resonance imaging scans of the abdomen, and pelvis) * Decisions about resectability status will be made in consensus at multidisciplinary meetings/discussions Resectable disease will be defined as: * No interface of the tumor with celiac artery, common hepatic artery (CHA), or superior mesenteric arteries (SMA) (and, if present, variants) * Less than 180° interface between tumor and vessel wall of the portal or superior mesenteric veins (SMV) without vein contour irregularity * For tumors of the body and tail of the pancreas, interface with the splenic artery and splenic vein of any degree will be considered resectable disease Borderline resectable disease will be defined as: * To include at least one of the following: * Tumor abutment \< 180° of the superior mesenteric artery or celiac axis * Solid tumor contact with CHA without extension to celiac artery (CA) or hepatic artery bifurcation allowing for safe and complete resection and reconstruction * Solid tumor contact with variant arterial anatomy (ex: accessory right hepatic artery, replaced right hepatic artery, replaced CHA, and the origin of replaced or accessory artery) * Tumor induced narrowing of SMV, portal vein (PV) or SMV-PV of \> 180˚ of the diameter of the vessel * Short segment occlusion of the SMV, PV or SMV-PV with a suitable PV above and SMV below, for reconstruction * Solid tumor contact with inferior vena cava * Biopsy proven N1 disease (regional lymph nodes involved) from pre-referral biopsy or endoscopic ultrasound (EUS)-guided fine needle aspiration (FNA) * No distant extrapancreatic disease (M0) * Adults \> 18 years of age * Able to give informed consent * Able to adhere to study visit schedule and other protocol requirements * Eastern Cooperative Oncology Group (ECOG) performance status of 0 - 1 * Absolute neutrophil count (ANC) ≥ 1,500 cells/ul * Platelet count ≥ 100,000 cells/ul * Hemoglobin ≥ 9 g/dL * Serum total bilirubin ≤ 1.5 x institutional upper limit of normal (ULN) * Aspartate aminotransferase (AST) and alanine aminotransferase (ALT) ≤ 2.5 x ULN * Albumin ≥ 3 g/dl * Creatinine ≤ 1.5 x ULN * Male, or a non-pregnant and non-lactating female * Women of child-bearing potential - defined as a sexually mature woman who has not undergone hysterectomy - the surgical removal of the uterus or bilateral oophorectomy - the surgical removal of both ovaries or has not been naturally postmenopausal for at least 24 consecutive months, i.e., has had menses at any time during the preceding 24 consecutive months, must commit to true abstinence from heterosexual contact, or agree to use, and be able to comply with, effective contraception without interruption for 28 days prior to starting gemcitabine/cisplatin/nab- paclitaxel (including dose interruptions) until treatment with gemcitabine/cisplatin/nab-paclitaxel is complete * Male subjects must practice true abstinence or agree to use a condom during sexual contact with a female of childbearing potential or a pregnant female while on treatment (including during dose interruptions) with gemcitabine/cisplatin/nab-paclitaxel and for 6 months following gemcitabine/cisplatin/nab- paclitaxel discontinuation, even if he has undergone a successful vasectomy Exclusion Criteria: * Peripheral neuropathy of grade 2 or greater by Common Terminology Criteria for Adverse Events (CTCAE) 4.0. In CTCAE version 4.0 grade 2 sensory neuropathy is defined as "moderate symptoms; limiting instrumental activities of daily living (ADLs)" * Concurrent severe and/or uncontrolled medical conditions which could compromise participation in the study such as unstable angina, myocardial infarction within 6 months, unstable symptomatic arrhythmia, symptomatic congestive heart failure, uncontrolled diabetes, serious active, uncontrolled infection after inadequate biliary drainage if tumor obstructing bile duct, or psychiatric illness/social situations * Pregnancy (positive pregnancy test) or lactation * Known central nervous system (CNS) disease, except for treated brain metastasis. Treated brain metastases are defined as having no evidence of progression or hemorrhage after treatment and no ongoing requirement for dexamethasone, as ascertained by clinical examination and brain imaging (MRI or CT) during the screening period. Anticonvulsants (stable dose) are allowed. Treatment for brain metastases may include whole brain radiotherapy (WBRT), radiosurgery (radiosurgery \[RS\]; Gamma Knife, linear accelerator \[LINAC\], or equivalent) or a combination as deemed appropriate by the treating physician. Patients with CNS metastases treated by neurosurgical resection or brain biopsy performed within 3 months prior to day 1 will be excluded * Previous (within the past 5 years) or concurrent presence of other untreated cancer, except nonmelanoma skin cancer and in situ carcinomas * History of allergy or hypersensitivity to any of the study drugs * Current abuse of alcohol or illicit drugs * Inability or unwillingness to sign the informed consent form Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Mihir M. Shah, MD Phone: 404-778-3307 Role: CONTACT #### Locations Location 1: City: Atlanta Contacts: *Contact 1:* - Email: [email protected] - Name: Kathleen M. Coleman - Role: CONTACT *Contact 2:* - Name: Mihir M. Shah, MD - Role: PRINCIPAL_INVESTIGATOR Country: United States Facility: Emory University Hospital/Winship Cancer Institute State: Georgia Zip: 30322 #### Overall Officials Official 1: Affiliation: Emory University Hospital/Winship Cancer Institute Name: Mihir M Shah, MD Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000002277 - Term: Carcinoma - ID: D000009375 - Term: Neoplasms, Glandular and Epithelial - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000004701 - Term: Endocrine Gland Neoplasms - ID: D000004066 - Term: Digestive System Diseases - ID: D000010182 - Term: Pancreatic Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M13110 - Name: Pancreatic Neoplasms - Relevance: HIGH - As Found: Pancreatic Cancer - ID: M3585 - Name: Adenocarcinoma - Relevance: HIGH - As Found: Adenocarcinoma - ID: M5534 - Name: Carcinoma - Relevance: LOW - As Found: Unknown - ID: M12320 - Name: Neoplasms, Glandular and Epithelial - Relevance: LOW - As Found: Unknown - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7863 - Name: Endocrine Gland Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M13102 - Name: Pancreatic Diseases - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown - ID: T4387 - Name: Pancreatic Cancer - Relevance: HIGH - As Found: Pancreatic Cancer ### Condition Browse Module - Meshes - ID: D000000230 - Term: Adenocarcinoma - ID: D000010190 - Term: Pancreatic Neoplasms ### Intervention Browse Module - Ancestors - ID: D000000972 - Term: Antineoplastic Agents, Phytogenic - ID: D000000970 - Term: Antineoplastic Agents - ID: D000050257 - Term: Tubulin Modulators - ID: D000050256 - Term: Antimitotic Agents - ID: D000050258 - Term: Mitosis Modulators - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action - ID: D000000964 - Term: Antimetabolites, Antineoplastic - ID: D000000963 - Term: Antimetabolites ### Intervention Browse Module - Browse Branches - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M19537 - Name: Paclitaxel - Relevance: HIGH - As Found: Surgery - ID: M2985 - Name: Gemcitabine - Relevance: HIGH - As Found: Activity - ID: M231 - Name: Albumin-Bound Paclitaxel - Relevance: HIGH - As Found: Enteral - ID: M6182 - Name: Cisplatin - Relevance: HIGH - As Found: Locally Advanced - ID: M26197 - Name: Tubulin Modulators - Relevance: LOW - As Found: Unknown - ID: M26196 - Name: Antimitotic Agents - Relevance: LOW - As Found: Unknown - ID: M4281 - Name: Antimetabolites - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000017239 - Term: Paclitaxel - ID: D000068196 - Term: Albumin-Bound Paclitaxel - ID: D000002945 - Term: Cisplatin - ID: D000093542 - Term: Gemcitabine ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423313 Brief Title: Effects of Anesthesia Type on QoR-40 Official Title: The Comparison of Total Intravenous Anesthesia and Inhalation Anesthesia Effects on Postoperative Recovery by Quality of Recovery (QoR-40) in Septorhinoplasty #### Organization Study ID Info ID: 2024/07-1 #### Organization Class: OTHER Full Name: Zonguldak Bulent Ecevit University ### Status Module #### Completion Date Date: 2024-10-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: ACTIVE_NOT_RECRUITING #### Primary Completion Date Date: 2024-08-30 Type: ESTIMATED #### Start Date Date: 2024-05-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-03 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Zonguldak Bulent Ecevit University #### Responsible Party Investigator Affiliation: Zonguldak Bulent Ecevit University Investigator Full Name: Çağdaş Baytar Investigator Title: Principal Investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: To compare the effects of total intravenous anesthesia and inhalation anesthesia used for maintenance on postoperative recovery in patients undergoing septorhinoplasty surgery under general anesthesia, using the recovery quality score (QoR-40). ### Conditions Module Conditions: - General Anesthesia - İnhalation Anesthetics - Quality of Recovery Keywords: - total intravenous anesthesia - anesthesia maintenance - inhalation anesthesia - quality of recovery-40 ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 1 Type: ACTUAL Patient Registry: True Study Type: OBSERVATIONAL Target Duration: 1 Day ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Procedure: maintenance of anesthesia Label: Group TIVA #### Arm Group 2 Intervention Names: - Procedure: maintenance of anesthesia Label: Group Inhalation ### Interventions #### Intervention 1 Arm Group Labels: - Group Inhalation - Group TIVA Description: Types used to maintain anesthesia Name: maintenance of anesthesia Type: PROCEDURE ### Outcomes Module #### Primary Outcomes Description: measurement of recovery quality in the first 24 hours after extubation Measure: quality of recovery-40 questionnaire Time Frame: up to 24 hour after surgery #### Secondary Outcomes Description: complications that may occur in the postoperative period Measure: postoperative complications Time Frame: up to 24 hour after surgery Description: time between the last suture and extubation Measure: duration of extubation Time Frame: end of the surgery ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * 18-65 years old * ASA I-II-III risk group * Patients whose consent was obtained with an informed consent form * Patients who will undergo septorhinoplasty surgery Exclusion Criteria: * -ASA \>3 * Psychiatric illness that prevents them from answering the questionnaire * Patients with a history of chronic opioid and benzodiazepine use as it may affect recovery time * Severe renal and hepatic insufficiency * Severe respiratory and cardiovascular disease * Patients with a body mass index \>30 kg m2 * Patients with a known history of allergy or contraindication to any of the drugs to be used in the study Healthy Volunteers: True Maximum Age: 65 Years Minimum Age: 18 Years Sampling Method: PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: The study will include intubated patients who will undergo septorhinoplasty surgery under general anesthesia, aged 18-65 years, in the American Society of Anesthesiology (ASA) I-II-III risk class. ### Contacts Locations Module #### Locations Location 1: City: Zonguldak Country: Turkey Facility: Zonguldak Bülent Ecevit University Medicine Faculty State: Kozlu Zip: 67600 ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012120 - Term: Respiration Disorders - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000010335 - Term: Pathologic Processes ### Condition Browse Module - Browse Branches - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M27137 - Name: Respiratory Aspiration - Relevance: HIGH - As Found: Inhalation - ID: M14957 - Name: Respiration Disorders - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000053120 - Term: Respiratory Aspiration ### Intervention Browse Module - Ancestors - ID: D000002492 - Term: Central Nervous System Depressants - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: CNSDep - Name: Central Nervous System Depressants - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: Ot - Name: Other Dietary Supplements ### Intervention Browse Module - Browse Leaves - ID: M4107 - Name: Anesthetics - Relevance: HIGH - As Found: Imaging - ID: M4854 - Name: Benzocaine - Relevance: LOW - As Found: Unknown - ID: T433 - Name: Tannic Acid - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000000777 - Term: Anesthetics ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423300 Brief Title: [Trial of device that is not approved or cleared by the U.S. FDA] Official Title: [Trial of device that is not approved or cleared by the U.S. FDA] #### Organization Study ID Info ID: CIP0001 #### Organization Full Name: [Redacted] ### Status Module Delayed Posting: True #### Expanded Access Info #### Last Update Post Date Date: 2024-05-31 Type: ESTIMATED Last Update Submit Date: 2024-05-29 Overall Status: WITHHELD #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-24 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Name: [Redacted] #### Responsible Party Old Name Title: [Redacted] Old Organization: [Redacted] ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423287 Acronym: TRELO Brief Title: Effects of TRE With Lactobacillus Plantarum LP-KFY04 Supplementation on Overweight / Obese Individuals Official Title: Effects of Time-Restricted Eating With Lactobacillus Plantarum LP-KFY04 Supplementation on Overweight / Obese Individuals : A Multicenter, Randomized, Double-blind, Placebo-controlled Clinical Trial #### Organization Study ID Info ID: 2024LX0016_GY #### Organization Class: OTHER Full Name: Zhujiang Hospital ### Status Module #### Completion Date Date: 2025-01-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-01-31 Type: ESTIMATED #### Start Date Date: 2024-04-01 Type: ACTUAL Status Verified Date: 2024-03 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Zhujiang Hospital #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: With the improvement of the quality of life, multi-nutritional dietary intake today has provided people with a solid foundation for their health profiles. Time-restricted eating is found to be an effective method to prevent and control obesity, helping obese patients to lose weight in a way of reshaping the gut microbiota. Regulation of gut microbiota, as a valid weight-loss strategy, can be achieved by oral supplementation of probiotics. This study aims to evaluate the effectiveness of time-restricted eating combined with Lactobacillus Plantarum LP-KFY04 on overweight/obese population through a multi-center, randomized and double-blind clinical trial. Detailed Description: With the improvement of the quality of life, multi-nutritional dietary intake today has provided people with a solid foundation for their health profiles. Time-restricted eating is found to be an effective method to prevent and control obesity, helping obese patients to lose weight in a way of reshaping the gut microbiota. Regulation of gut microbiota, as a valid weight-loss strategy, can be achieved by oral supplementation of probiotics. This study aims to evaluate the effectiveness of time-restricted eating combined with Lactobacillus Plantarum LP-KFY04 on overweight/obese population through a multi-center, randomized and double-blind clinical trial.Patients in the treatment group will be instructed to eat in an 8-hour time window (a set period of time decided by the patients) with supplementation of Lactobacillus plantarum LP-KFY04 over 12 weeks'trial.Patients in the control group will be instructed to eat in an 8-hour time window (a set period of time decided by the patients) with supplementation of placebo over 12 weeks' trial. ### Conditions Module Conditions: - Obesity Keywords: - Obesity - Time-restricted Diet - Probiotic Compound LP-KFY04 - Weight Loss ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: DOUBLE Who Masked: - PARTICIPANT - INVESTIGATOR Primary Purpose: TREATMENT #### Enrollment Info Count: 160 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients in the treatment group will be instructed to eat in an 8-hour time window (a set period of time decided by the patients) with supplementation of Lactobacillus plantarum LP-KFY04 over 12 weeks' trial. Intervention Names: - Dietary Supplement: Lactobacillus plantarum LP-KFY04 Label: Lactobacillus plantarum LP-KFY04 Type: EXPERIMENTAL #### Arm Group 2 Description: Patients in the control group will be instructed to eat in an 8-hour time window (a set period of time decided by the patients) with supplementation of placebo over 12 weeks' trial. Intervention Names: - Other: Take placebo in addition to the limited diet. Label: placebo Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Lactobacillus plantarum LP-KFY04 Description: Patients in the treatment group will be instructed to eat in an 8-hour time window (a set period of time decided by the patients) with supplementation of Lactobacillus plantarum LP-KFY04 over 12 weeks' trial. Name: Lactobacillus plantarum LP-KFY04 Type: DIETARY_SUPPLEMENT #### Intervention 2 Arm Group Labels: - placebo Description: Patients in the control group will be instructed to eat in an 8-hour time window (a set period of time decided by the patients) with supplementation of placebo over 12 weeks'trial. Name: Take placebo in addition to the limited diet. Type: OTHER ### Outcomes Module #### Primary Outcomes Measure: Change of body weight from baseline to 12 weeks after intervention Time Frame: 12 weeks #### Secondary Outcomes Measure: Changes of BMI compared with baseline in subjects Time Frame: 12 weeks Measure: Changes of waist circumference compared with baseline in subjects Time Frame: 12 weeks Measure: Changes of body fat percentage (BF%) compared with baseline assessed by dual-energy X-ray absorptiometry (DEXA) Time Frame: 12 weeks Measure: Change of subjects' HOMA-IR compared with baseline Time Frame: 12 weeks Measure: Changes of blood pressure in subjects compared with baseline Time Frame: 12 weeks Measure: Changes of blood glucose in subjects compared with baseline Time Frame: 12 weeks Description: Blood lipids includes total cholesterol、triglyceride、LDL-c、HDL-c. Measure: Changes of blood lipids in subjects compared with baseline Time Frame: 12 weeks Description: Species of intestinal microbial includes Firmicutes、Bacteroidetes、Proteobacteria、Actinobacteriota、Verrucomicrobia、Fusobacteria. Measure: Changes of intestinal microbial composition compared with baseline in subjects Time Frame: 12 weeks Description: Proportion of intestinal microbial such as Firmicutes、Bacteroidetes、Proteobacteria、Actinobacteriota、Verrucomicrobia、Fusobacteria Measure: Changes of intestinal microbial abundance compared with baseline in subjects Time Frame: 12 weeks Description: Plasma metabolite includes arachidonic acid 、betaine、glutathione and so on. Measure: Changes of plasma metabolite compared with baseline in subjects Time Frame: 12 weeks Measure: The incidence of adverse events in two groups of subjects Time Frame: 12 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Men or women aged 18 to 65 years old 2. BMI 24.0 to 40kg/m2 3. Patients who are aware of the purpose of the trail, willing to participate in the trial and sign informed consent forms, and comply with all requirements (including those during follow-up and evaluation investigations) Exclusion Criteria: 1. History of HIV, hepatitis B or C (self-report) or active pulmonary tuberculosis; 2. Diagnosis of type 1 or type 2 diabetes and prescribing hypoglycemic therapy 3. History of malignant tumors 4. Serious liver dysfunction or chronic kidney disease (aspartate aminotransferase (AST) or alanine transaminase (ALT) \> 3 times the upper limit of normal, or estimated glomerular filtration rate (eGFR) \< 30 ml/min/1.73 m2) 5. History of serious cardiovascular or cerebrovascular disease (angina, myocardial infarction, or stroke) within the past 6 months 6. History of serious gastrointestinal disease or gastrointestinal surgery within the past 12 months 7. History of Cushing's syndrome, hypothyroidism, acromegaly, and hypothalamic obesity 8. Smoking or have smoked within the past 3 months of the screening period 9. Drinking alcohol or drinking more than 15 grams of alcohol per day within the past 3 months of the screening period 10. Taking any medicine that may affect weight or metabolism within the past 6 months, including weight loss medications, antipsychotics, or other medications identified by the researchers 11. Currently involving in a weight loss program or having significant weight change within the past 3 months (\> 5% of current weight) 12. Women who are pregnant or planning for pregnant 13. Patients who are unable to complete 12-week follow-up (due to health conditions or immigration reasons) 14. Patients who are unwilling or unable to provide informed consent Maximum Age: 65 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Hong Chen, MD Phone: 13602759769 Role: CONTACT #### Locations Location 1: City: Guangzhou Country: China Facility: Zhujiang Hospital of Southern Medical University State: Guangdong Status: RECRUITING Zip: 510000 #### Overall Officials Official 1: Affiliation: Zhujiang Hospital Name: Hong Chen, MD Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000044343 - Term: Overnutrition - ID: D000009748 - Term: Nutrition Disorders - ID: D000001835 - Term: Body Weight ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M12701 - Name: Obesity - Relevance: LOW - As Found: Unknown - ID: M26186 - Name: Overweight - Relevance: HIGH - As Found: Overweight - ID: M18102 - Name: Weight Loss - Relevance: LOW - As Found: Unknown - ID: M5114 - Name: Body Weight - Relevance: LOW - As Found: Unknown - ID: M25307 - Name: Overnutrition - Relevance: LOW - As Found: Unknown - ID: M12684 - Name: Nutrition Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000050177 - Term: Overweight ### Intervention Browse Module - Browse Branches - Abbrev: Ot - Name: Other Dietary Supplements - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: T355 - Name: Acidophilus - Relevance: HIGH - As Found: Students ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423274 Brief Title: Comparing Artificial Intelligence for Assisted Diagnosis of Diabetic Retinopathy Official Title: A Comparative Analysis of the Diagnostic Outcomes of Artificial Intelligence-assisted Fundus Photography for Diabetic Retinopathy and Diabetic Macular Edema Versus Other Imaging Devices in Ophthalmology: A Controlled Trial #### Organization Study ID Info ID: DR artificial intelligence #### Organization Class: OTHER Full Name: Zhejiang University ### Status Module #### Completion Date Date: 2025-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-09-01 Type: ESTIMATED #### Start Date Date: 2024-05-10 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-09 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Zhejiang University #### Responsible Party Investigator Affiliation: Second Affiliated Hospital, School of Medicine, Zhejiang University Investigator Full Name: Wu Hongkang Investigator Title: Director Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This study plans to compare the accuracy of artificial intelligence (AI)-assisted fundus images with other ophthalmic devices such as optical coherence tomography (OCT) and fundus fluorescence angiography (FFA) in the diagnosis of diabetic retinopathy and diabetic macular edema. Detailed Description: This study plans to compare the accuracy of artificial intelligence (AI)-assisted fundus images with other ophthalmic devices such as optical coherence tomography (OCT) and fundus fluorescence angiography (FFA) in the diagnosis of diabetic retinopathy and diabetic macular edema. This study was conducted as a prospective study. Participants meeting eligibility criteria will be recruited from sites staffed by trained photographers. After assessing eligibility and obtaining informed consent, fundus photographs will be taken using a non-dilated fundus camera. And optical coherence tomography or fundus fluorescence angiography will be performed. ### Conditions Module Conditions: - Diabetic Retinopathy - Diabetic Macular Edema Keywords: - diabetic retinopathy - diabetic macular edema - artificial intelligence ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 1000 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Artificial intelligence-assisted fundus photography in patients with diabetic retinopathy Intervention Names: - Diagnostic Test: fundus photography Label: artificial intelligence-assisted fundus photography #### Arm Group 2 Description: optical coherence tomography in patients with diabetic retinopathy Intervention Names: - Diagnostic Test: optical coherence tomography Label: optical coherence tomography #### Arm Group 3 Description: fundus fluorescence angiography in patients with diabetic retinopathy Intervention Names: - Diagnostic Test: fundus fluorescence angiography Label: fundus fluorescence angiography ### Interventions #### Intervention 1 Arm Group Labels: - artificial intelligence-assisted fundus photography Description: using artificial intelligence to identify diabetic retinopathy using fundus photography Name: fundus photography Type: DIAGNOSTIC_TEST #### Intervention 2 Arm Group Labels: - optical coherence tomography Description: detect diabetic retinopathy and diabetic macular edema by optical coherence tomography Name: optical coherence tomography Type: DIAGNOSTIC_TEST #### Intervention 3 Arm Group Labels: - fundus fluorescence angiography Description: detect diabetic retinopathy by fundus fluorescence angiography Name: fundus fluorescence angiography Type: DIAGNOSTIC_TEST ### Outcomes Module #### Primary Outcomes Description: Detection of DR accuracy using fundus photography, optical coherence tomography, and fundus fluorescence angiography Measure: The accuracy Time Frame: Baseline-Month 12 #### Secondary Outcomes Description: Detection of DME accuracy using fundus photography, optical coherence tomography, and fundus fluorescence angiography Measure: The accuracy Time Frame: Baseline-Month 12 ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Diagnostic for diabetes: Type 1 diabetes of a lest 5 years of evolution; or Type 2 diabetes; 2. Obtaining informed consent; 3. Patient age 18 or above. Exclusion Criteria: 1. Patients under 18 years of age; 2. Failure to Obtain informed consent; 3. Presence of other retinal diseases; 4. A patient who has already undergone the treatment. Healthy Volunteers: True Maximum Age: 90 Years Minimum Age: 18 Years Sampling Method: PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: It is planned to include 1,000 participants in the study, all of whom will undergo fundus photography, 500 additional patients will undergo fundus fluorescence angiography, and 500 additional patients will undergo optical coherence tomography. All participants met inclusion and exclusion criteria. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Hongkang Wu, MMS Phone: +8618969978676 Role: CONTACT #### Locations Location 1: City: Hangzhou Contacts: *Contact 1:* - Email: [email protected] - Name: Hongkang Wu, MMS - Phone: 18969978676 - Role: CONTACT Country: China Facility: The Second Affiliated Hospital Zhejiang University School of Medicine State: Zhejiang Zip: 310000 ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000003920 - Term: Diabetes Mellitus - ID: D000004700 - Term: Endocrine System Diseases - ID: D000008268 - Term: Macular Degeneration - ID: D000012162 - Term: Retinal Degeneration - ID: D000005128 - Term: Eye Diseases - ID: D000003925 - Term: Diabetic Angiopathies - ID: D000014652 - Term: Vascular Diseases - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000048909 - Term: Diabetes Complications ### Condition Browse Module - Browse Branches - Abbrev: BC11 - Name: Eye Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases ### Condition Browse Module - Browse Leaves - ID: M11261 - Name: Macular Edema - Relevance: HIGH - As Found: Macular Edema - ID: M7125 - Name: Diabetic Retinopathy - Relevance: HIGH - As Found: Diabetic Retinopathy - ID: M14999 - Name: Retinal Diseases - Relevance: HIGH - As Found: Retinopathy - ID: M7657 - Name: Edema - Relevance: HIGH - As Found: Edema - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown - ID: M11260 - Name: Macular Degeneration - Relevance: LOW - As Found: Unknown - ID: M14997 - Name: Retinal Degeneration - Relevance: LOW - As Found: Unknown - ID: M8271 - Name: Eye Diseases - Relevance: LOW - As Found: Unknown - ID: M7120 - Name: Diabetic Angiopathies - Relevance: LOW - As Found: Unknown - ID: M17400 - Name: Vascular Diseases - Relevance: LOW - As Found: Unknown - ID: M26004 - Name: Diabetes Complications - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000008269 - Term: Macular Edema - ID: D000012164 - Term: Retinal Diseases - ID: D000003930 - Term: Diabetic Retinopathy - ID: D000004487 - Term: Edema ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423261 Brief Title: Phase I Clinical Study of GB002 Recombinant Peptide Inhalation Solution Official Title: Phase I Clinical Study to Evaluate the Safety, Tolerability, Pharmacokinetics, and Immunogenicity of GB002 Recombinant Polypeptide Inhalation Solution in a Randomized, Double-blind, Placebo-controlled, Dose-increasing Single and Multiple Administration in Chinese Healthy Adult Subjects. #### Organization Study ID Info ID: YKSW-GB002-R01 #### Organization Class: INDUSTRY Full Name: Zhejiang Echon Biopharm Limited ### Status Module #### Completion Date Date: 2024-07-29 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: ACTIVE_NOT_RECRUITING #### Primary Completion Date Date: 2024-05-30 Type: ESTIMATED #### Start Date Date: 2023-08-24 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-30 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Zhejiang Echon Biopharm Limited #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: This trial is conducted in China. The purpose of this clinical trial is to evaluate the safety and tolerability, pharmacokinetic (PK) characteristics, and immunogenicity of single/multiple inhalation of different doses of GB002 recombinant peptide in healthy subjects. ### Conditions Module Conditions: - Healthy ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: QUADRUPLE Who Masked: - PARTICIPANT - CARE_PROVIDER - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 100 Type: ACTUAL Phases: - PHASE1 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Each subject will receive one single administration of GB002 recombinant peptide inhalation solution. The dosage of each group is 0.625mg, 1.25mg, 2.5mg, 5.0mg,7.5mg, respectively. Intervention Names: - Drug: GB002 Recombinant Peptide Inhalation Solution - Drug: Placebo Label: Single Ascending Dose of GB002 Recombinant Peptide Inhalation Solution Type: EXPERIMENTAL #### Arm Group 2 Description: The subjects will receive multiple doses of GB002 recombinant peptide inhalation solution, administered twice a day for 6 consecutive days. The dosage for each group is 2.5mg, 5.0mg, and 6.5mg, respectively. Intervention Names: - Drug: GB002 Recombinant Peptide Inhalation Solution - Drug: Placebo Label: Multiple Ascending Dose of GB002 Recombinant Peptide Inhalation Solution Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Multiple Ascending Dose of GB002 Recombinant Peptide Inhalation Solution - Single Ascending Dose of GB002 Recombinant Peptide Inhalation Solution Description: Inhalation administration Name: GB002 Recombinant Peptide Inhalation Solution Type: DRUG #### Intervention 2 Arm Group Labels: - Multiple Ascending Dose of GB002 Recombinant Peptide Inhalation Solution - Single Ascending Dose of GB002 Recombinant Peptide Inhalation Solution Description: Inhalation administration Name: Placebo Type: DRUG ### Outcomes Module #### Other Outcomes Measure: GB002 Recombinant Peptide concentrations in induced sputum Time Frame: Day 1 to Day 7 #### Primary Outcomes Measure: Number of participants with adverse events Time Frame: Day 1 to Day 28 #### Secondary Outcomes Measure: Plasma GB002 Recombinant Peptide concentrations Time Frame: Day 1 to Day 7 Description: Anti-drug antibody（ADA）and neutralizing antibody Nab Measure: Immunogenicity Time Frame: Day 14 and Day 28 ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Chinese healthy subjects aged 18 years and above (including 18 years old), both male and female; 2. Male weight ≥50kg, female weight ≥45kg, and body mass index (BMI) in the range of 19-26kg /m² (including the critical value), body mass index (BMI) = weight (kg)/height 2 (m²); 3. Sign informed consent before the test, and fully understand the test content, process and possible adverse reactions; 4. The subjects were able to maintain good communication with the investigators, and understood and complied with the requirements of the clinical trial. Exclusion Criteria: 1. Participants in any drug clinical trial or use of investigational drug within 3 months prior to the use of investigational drug; 2. Have a history of respiratory disease, such as acute exacerbation of chronic obstructive pulmonary disease, pulmonary fibrosis, pulmonary hypertension, pulmonary hydroedema, pulmonary interstitial disease, bronchial asthma, paradoxical bronchospasm, or throat ulcers, edema, or edema, or have undergone throat, trachea/bronchus, or lung surgery, or within 4 weeks prior to the use of the study drug, Patients with a history of upper and lower respiratory tract infection or acute sinusitis caused by viruses or bacteria, which is considered clinically significant by researchers; 3. Patients with a medical history of cardiovascular system, digestive system, endocrine system, urinary system, nervous system, hematology, immunology (including personal or family history of inherited immune deficiency), metabolic abnormalities, and researchers believe that the current clinical significance; 4. Allergy to any of the ingredients of the drug, or a history of allergy to drugs, foods, pollen or other substances, in particular a known allergy to protein foods, or a history of respiratory allergic disease; 5. Patients who cannot tolerate venipunctures or have a history of fainting needles and fainting blood; 6. Patients who have undergone surgery within 6 months prior to the use of the investigational drug that researchers judge will affect drug absorption, distribution, metabolism, and excretion; Or have undergone surgical procedures within 4 weeks prior to the use of the investigational drug; Or plan to undergo surgical procedures during the study period; 7. Used any drug (including prescription drugs, over-the-counter drugs, Chinese herbs, health care products, etc.) within 14 days before the use of the experimental drug; 8. Persons who have received the vaccine or live attenuated vaccine within 14 days prior to the use of the investigational product, or who plan to receive the vaccine during the trial period; 9. People who donated blood or lost a large amount of blood (\>400mL) within 3 months prior to the use of the investigational drug, received blood transfusions or used blood products, or intended to donate blood or blood components during or within 3 months after the end of the trial; 10. Drug abusers or those who have used soft drugs (e.g., cannabis) or hard drugs (e.g., cocaine, PCP, etc.) within one year prior to the use of the investigatory drug; 11. Smokers or smokers who smoked more than 5 cigarettes per day in the 3 months prior to the use of the experimental drug, or who could not stop using any tobacco products during the test period; 12. Alcoholics or regular drinkers in the six months prior to the use of the experimental drug, i.e. drinking more than 14 units of alcohol per week (1 unit =360mL beer or 45mL spirits with 40% alcohol or 150mL wine); Or unwilling to stop drinking alcohol or any products containing alcohol during the trial; 13. Those who consumed excessive amounts of tea, coffee and/or caffeinated beverages (more than 8 cups, 1 cup =250mL) per day, or did not agree to stop drinking tea, coffee and/or caffeinated beverages during the study period; 14. Eat any diet (including grapefruit or grapefruit products, dragon fruit, mango, grapefruit, orange, etc.) that may affect the metabolism of the drug in the body within 7 days prior to the use of the investigatory drug, or any other diet that the researcher considers to affect the absorption, distribution, metabolism or excretion of the drug, or do not agree to stop eating the above diet during the trial period; 15. Those who have special requirements for diet and cannot comply with a unified diet; 16. Subjects (or their partners) have pregnancy plans, sperm and egg donation plans, or do not wish to use one or more non-drug contraceptive methods (such as total abstinence, condoms, pregnancy avoidance rings, partner ligation, etc.) during the trial period to 3 months after the trial ends; 17. Female subjects are pregnant or lactating women; Or had unprotected sex within 2 weeks prior to the use of the investigational drug; Use of oral contraceptives within 30 days prior to the use of the investigational drug or use of long-acting estrogen or progesterone injections or implants within 6 months prior to the use of the investigational drug; 18. Patients with clinically significant abnormalities in physical examination, 12-lead electrocardiogram, vital signs (blood pressure, pulse, body temperature, SpO2), chest X-ray, laboratory examination, and pulmonary function examination (as determined by the clinician); 19. Pulmonary function examination: FEV1 measured value /FEV1 estimated value ≤80% or FVC≤ 80% of the estimated value; 20. Positive results of tobacco test; 21. Positive urine screening test; 22. Positive alcohol breath test; 23. Failure to use the inhalant delivery device correctly or unqualified inhalant delivery training; 24. Subjects may not be able to complete the study for other reasons or may have other reasons deemed inappropriate by the investigator. Healthy Volunteers: True Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Changsha Country: China Facility: The Third Hospital of Changsha State: Hunan Zip: 410015 ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012120 - Term: Respiration Disorders - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000010335 - Term: Pathologic Processes ### Condition Browse Module - Browse Branches - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M27137 - Name: Respiratory Aspiration - Relevance: HIGH - As Found: Inhalation - ID: M14957 - Name: Respiration Disorders - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000053120 - Term: Respiratory Aspiration ### Intervention Browse Module - Browse Branches - Abbrev: PhSol - Name: Pharmaceutical Solutions - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M21860 - Name: Pharmaceutical Solutions - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423248 Brief Title: Culinary Spices in Metabolic Syndrome. Official Title: The Effect of Therapeutic Doses of Culinary Spices in Metabolic Syndrome: A Randomized Controlled Trial. #### Organization Study ID Info ID: Protocol Number: 15/22 #### Organization Class: OTHER Full Name: United Arab Emirates University ### Status Module #### Completion Date Date: 2016-11-13 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: COMPLETED #### Primary Completion Date Date: 2016-11-13 Type: ACTUAL #### Start Date Date: 2015-05-10 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: United Arab Emirates University #### Responsible Party Investigator Affiliation: United Arab Emirates University Investigator Full Name: Ayesha Salem Al Dhaheri Investigator Title: Professor, Associate Provost, Student Affairs Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This double blind, placebo controlled randomized controlled trial aims to evaluate the effect of three commonly used culinary spices - ginger (Zingiber officinale), cinnamon (Cinnamomum) and black seed (Nigella sativa) on the cardiometabolic parameters of individuals with risk factors of metabolic syndrome. Participants consume their assigned treatment for 12 weeks, and key cardiovascular and glucometabolic parameters are recorded at baseline, week 6, and week 12 of the study. ### Conditions Module Conditions: - Metabolic Syndrome ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: TRIPLE Masking Description: Both patient and investigators were blind to treatment allocation, with an independent researcher providing the allocated treatments to the participants. Who Masked: - PARTICIPANT - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 120 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Participants consumed 3g of dried powdered Ginger (Zingiber officinale) daily for 12 weeks. Intervention Names: - Dietary Supplement: Culinary spices Label: Ginger Type: ACTIVE_COMPARATOR #### Arm Group 2 Description: Participants consumed 3g of dried powdered Cinnamon (Cinnamomum) daily for 12 weeks. Intervention Names: - Dietary Supplement: Culinary spices Label: Cinnamon Type: ACTIVE_COMPARATOR #### Arm Group 3 Description: Participants consumed 3g of dried powdered Black Seed (Nigella sativa) daily for 12 weeks. Intervention Names: - Dietary Supplement: Culinary spices Label: Black Seed Type: ACTIVE_COMPARATOR #### Arm Group 4 Description: Participants consumed 3g of powdered corn starch daily for 12 weeks. Intervention Names: - Dietary Supplement: Culinary spices Label: Placebo Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Black Seed - Cinnamon - Ginger - Placebo Description: Powdered culinary spices Name: Culinary spices Type: DIETARY_SUPPLEMENT ### Outcomes Module #### Primary Outcomes Description: Fasting plasma glucose blood test taken at baseline, week 6 and week 12. Measure: Mean Change in Fasting Blood Glucose at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Glycated Haemoglobin blood test taken at baseline, week 6 and week 12. Measure: Mean Change in HbA1c at 12 weeks Time Frame: Baseline, Week 6 and Week 12 #### Secondary Outcomes Description: Systolic and diastolic blood pressure taken at baseline, week 6 and week 12. Measure: Mean Change in Blood Pressure at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Total Cholesterol Blood Test taken at baseline, week 6 and week 12. Measure: Mean Change in Total Cholesterol at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Low Density Lipoprotein Blood Test taken at baseline, week 6 and week 12. Measure: Mean Change in LDL Cholesterol at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: High Density Lipoprotein Blood Test taken at baseline, week 6 and week 12. Measure: Mean Change in HDL Cholesterol at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Triglyceride Blood Test taken at baseline, week 6 and week 12. Measure: Mean Change in Triglyceride concentrations at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Weight taken at baseline, week 6 and week 12. Measure: Mean Change in Weight at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Weight taken at baseline, week 6 and week 12, and BMI calculated as weight divided by height squared. Measure: Mean Change in Body Mass Index at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Waist Circumference taken at baseline, week 6 and week 12. Measure: Mean Change in Waist Circumference at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Waist and Hip Circumference taken at baseline, week 6 and week 12, and Waist-Hip ratio calculated. Measure: Mean Change in Waist to Hip ratio at 12 weeks Time Frame: Baseline, Week 6 and Week 12 Description: Dual Energy Xray Absorptiometry performed at baseline, week 6 and week 12, and Fat mass, body fat percentage, visceral fat, fat free mass, and skeletal muscle mass calculated. Measure: Mean Change in Densitometric Body Composition at 12 weeks Time Frame: Baseline, Week 6 and Week 12 ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * age (18-50 years) and had 2 or more of MetS diagnostic criteria: high waist circumference (\>80 cm for female and \>94 cm for males), elevated blood pressure (equal to or greater than 130/85 mm Hg or use of medication for hypertension), high fasting blood glucose (equal to or greater than 100 mg/dL \[5.6 mmol/L\] or use of medication for hyperglycemia), lowered HDL cholesterol (less than 40 mg/dL \[1.03 mmol/L\] for men and less than 50 mg/dL \[1.29 mmol/L\] for women) and increased triglycerides (equal to or greater than 150 mg/dL \[1.7 mmol/L\]). Participants who had at least three risk factors out of five or had two risk factors and one borderline were included in the study. Exclusion Criteria: * did not meet the following inclusion criteria, older than 50 years old or younger than 17 years old and did not meet the metabolic syndrome diagnostic criteria. Additionally, participants were excluded if they are allergic to spices, current smokers, pregnant women, lactating women or currently taking medication and if they refused to provide blood sample. Also, participants with any acute illnesses or any chronic diseases such as kidney, liver, cardiovascular and gastrointestinal diseases were excluded from the study Maximum Age: 50 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT ### Contacts Locations Module #### Locations Location 1: City: Al Ain Country: United Arab Emirates Facility: United Arab Emirates University State: Abu Dhabi ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000004194 - Term: Disease - ID: D000010335 - Term: Pathologic Processes - ID: D000007333 - Term: Insulin Resistance - ID: D000006946 - Term: Hyperinsulinism - ID: D000044882 - Term: Glucose Metabolism Disorders - ID: D000008659 - Term: Metabolic Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M23005 - Name: Metabolic Syndrome - Relevance: HIGH - As Found: Metabolic Syndrome - ID: M16355 - Name: Syndrome - Relevance: HIGH - As Found: Syndrome - ID: M10370 - Name: Insulin Resistance - Relevance: LOW - As Found: Unknown - ID: M9997 - Name: Hyperinsulinism - Relevance: LOW - As Found: Unknown - ID: M11639 - Name: Metabolic Diseases - Relevance: LOW - As Found: Unknown - ID: M25403 - Name: Glucose Metabolism Disorders - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000024821 - Term: Metabolic Syndrome - ID: D000013577 - Term: Syndrome ### Intervention Browse Module - Browse Branches - Abbrev: HB - Name: Herbal and Botanical - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: T238 - Name: Nigella - Relevance: LOW - As Found: Unknown - ID: T166 - Name: Ginger - Relevance: LOW - As Found: Unknown - ID: T115 - Name: Cinnamon - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423235 Acronym: ESPTTN Brief Title: Efficacy and Safety of Prunella Oral Liquid in the Treatment of Thyroid Nodules Official Title: Efficacy and Safety of Prunella Oral Liquid in the Treatment of Thyroid Nodules: a Multicenter, Prospective, Randomized, Double-blind, Placebo-controlled Study #### Organization Study ID Info ID: XK-22-A-002-YJ-002 #### Organization Class: INDUSTRY Full Name: Xintian Pharmaceutical ### Status Module #### Completion Date Date: 2028-07-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-07-30 Type: ESTIMATED #### Start Date Date: 2024-07-30 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-07 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Xintian Pharmaceutical #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: A multicenter, prospective, randomized, double-blind, placebo-controlled clinical trial was designed to evaluate the efficacy and safety of Prunella oral liquid in patients with benign thyroid nodules, which belongs to the post-marketing reevaluation clinical study. In this study, 426 subjects will be enrolled by competitive enrollment at several research centers across China. The main inclusion criteria are: ① Thyroid ultrasound examination found thyroid nodules, can be accompanied by goiter, and the nodules meet the following conditions: 1) There were dominant nodules in single or multiple nodules (the largest diameter of the second largest nodules was not more than 50% of the largest nodules), 2) solid nodules, 3) the longest diameter of nodules was ≥1cm and \< 3cm, 4) C-TIRADS 3\~4A nodules. ② Patients who met the puncture indication were confirmed by fine needle aspiration biopsy (FNAB) as benign nodules (Bethesda II). ③ Levels of TSH, FT3 and FT4 were normal, and the antibody titers of TgAb and TPOAb were normal. Eligible subjects will be randomly assigned on a 1:1:2:2 scale to: Group A (placebo conventional dose group, 10 mL/times, 2 times/day), group B (placebo 2x dose group, 10ml/times, 2 times/day), group C (conventional dose group of Prunella oral liquid), group D (Prunella oral liquid 2x dose group). All subjects will receive the treatment for 9 months and follow up at 3rd, 6th, 9th and 12th month. The primary efficacy endpoint of this study was the rate of change in thyroid nodule volume from baseline at 6 months of treatment. The rate of change in thyroid nodule volume from baseline at 3 and 9 months of treatment was a secondary efficacy endpoint. Other secondary efficacy endpoints included maximum thyroid nodule diameter, number of thyroid nodules, proportion of patients with reduced thyroid nodule volume or ≥50% from baseline, thyroid volume, thyroid function (serum TSH, FT3, FT4, thyroid egg levels (Tg), thyroid antibody levels (TgAb, TPOAb), quality of life evaluation (SF-36), etc. Safety endpoints included incidence of AE/ serious adverse events (SAE), causality, and outcomes. Incidence of AE/SAE leading to discontinuation. Changes in safety laboratory test values from baseline. ### Conditions Module Conditions: - Thyroid Nodule ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: DOUBLE Who Masked: - PARTICIPANT - INVESTIGATOR Primary Purpose: TREATMENT #### Enrollment Info Count: 426 Type: ESTIMATED Phases: - PHASE4 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Drug: regular dose of placebo Label: placebo regular dose group Type: PLACEBO_COMPARATOR #### Arm Group 2 Intervention Names: - Drug: 2x regular dose of placebo Label: placebo 2x regular dose group Type: PLACEBO_COMPARATOR #### Arm Group 3 Intervention Names: - Drug: regular dose of JiRui® Prunella oral liquid Label: regular dose group of Prunella oral liquid group Type: ACTIVE_COMPARATOR #### Arm Group 4 Intervention Names: - Drug: 2x regular dose of JiRui® Prunella oral liquid Label: 2x regular dose group of Prunella oral liquid group Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - regular dose group of Prunella oral liquid group Description: Take 10ml twice a day Name: regular dose of JiRui® Prunella oral liquid Type: DRUG #### Intervention 2 Arm Group Labels: - 2x regular dose group of Prunella oral liquid group Description: Take 20ml twice a day Name: 2x regular dose of JiRui® Prunella oral liquid Type: DRUG #### Intervention 3 Arm Group Labels: - placebo regular dose group Description: Take 10ml twice a day Name: regular dose of placebo Type: DRUG #### Intervention 4 Arm Group Labels: - placebo 2x regular dose group Description: Take 20ml twice a day Name: 2x regular dose of placebo Type: DRUG ### Outcomes Module #### Primary Outcomes Measure: Rate of change in thyroid nodule volume from baseline at 6 months of treatment. Time Frame: 180 ± 10 days #### Secondary Outcomes Measure: Rate of change in thyroid nodule volume from baseline at 3 months of treatment. Time Frame: 90 ± 7 days. Measure: Rate of change in thyroid nodule volume from baseline at 9 months of treatment. Time Frame: 270 ± 14 days. Measure: Rate of change in thyroid nodule volume from baseline at 12 months of treatment. Time Frame: 360 ± 14 days. Measure: The change value of the maximum diameter of thyroid nodules from baseline at 3 months of treatment. Time Frame: 90 ± 7 days Measure: The change value of the maximum diameter of thyroid nodules from baseline at 6 months of treatment. Time Frame: 180 ± 10 days Measure: The change value of the maximum diameter of thyroid nodules from baseline at 9 months of treatment. Time Frame: 270 ± 14 days Measure: The change value of the maximum diameter of thyroid nodules from baseline at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Proportion of patients with reduced thyroid nodule volume from baseline at 3 months of treatment. Time Frame: 90 ± 7 days Measure: Proportion of patients with reduced thyroid nodule volume from baseline at 6 months of treatment. Time Frame: 180 ± 10 days Measure: Proportion of patients with reduced thyroid nodule volume from baseline at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Proportion of patients with reduced thyroid nodule volume from baseline at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Proportion of patients with reduced thyroid nodule volume ≥50% from baseline at 3 months of treatment. Time Frame: 90 ± 7 days Measure: The proportion of patients with reduced thyroid nodule volume ≥50% from baseline at 6 months of treatment. Time Frame: 180 ± 10 days Measure: Proportion of patients with reduced thyroid nodule volume ≥50% from baseline at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Proportion of patients with reduced thyroid nodule volume ≥50% from baseline at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Changes in the number of thyroid nodules from baseline at the 3 months of treatment. Time Frame: 90 ± 7 days Measure: Changes in the number of thyroid nodules from baseline at the 6 months of treatment. Time Frame: 180 ± 10 days Measure: Changes in the number of thyroid nodules from baseline at the 9 months of treatment. Time Frame: 270 ± 14 days Measure: Changes in the number of thyroid nodules from baseline at the 12 months of treatment. Time Frame: 360 ± 14 days Measure: Proportion of patients with thyroid nodule progression (greater than 50% in volume or greater than 20% in at least 2 diameters from baseline) at 3 months of treatment. Time Frame: 90 ± 7 days Measure: Proportion of patients with thyroid nodule progression (greater than 50% in volume or greater than 20% in at least 2 diameters from baseline) at 6 months of treatment. Time Frame: 180 ± 10 days Measure: Proportion of patients with thyroid nodule progression (greater than 50% in volume or greater than 20% in at least 2 diameters from baseline) at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Proportion of patients with thyroid nodule progression (greater than 50% in volume or greater than 20% in at least 2 diameters from baseline) at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Rate of change in thyroid volume from baseline at 3 months of treatment. Time Frame: 90 ± 7 days Measure: Rate of change in thyroid volume from baseline at 6 months of treatment. Time Frame: 180 ± 10 days Measure: Rate of change in thyroid volume from baseline at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Rate of change in thyroid volume from baseline at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Changes in serum TSH, FT3 and FT4 from baseline at the months of treatment. Time Frame: 90 ± 7 days Measure: Changes in serum TSH, FT3 and FT4 from baseline at the months of treatment. Time Frame: 180 ± 10 days Measure: Changes in serum TSH, FT3 and FT4 from baseline at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Changes in serum TSH, FT3 and FT4 from baseline at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Changes in Tg, TgAb and TPOAb levels from baseline at the 6th month of treatment. Time Frame: 180 ± 10 days Measure: Proportion of patients with normal thyroid function at 3 months of treatment. Time Frame: 90 ± 7 days Measure: Proportion of patients with normal thyroid function at 6 months of treatment. Time Frame: 180 ± 10 days Measure: Proportion of patients with normal thyroid function at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Proportion of patients with normal thyroid function at 12 months of treatment. Time Frame: 360 ± 14 days Measure: Subjects' quality of life scores (SF-36) at 3 months of treatment. Time Frame: 90 ± 7 days Measure: Subjects' quality of life scores (SF-36) at 6 months of treatment. Time Frame: 180 ± 10 days Measure: Subjects' quality of life scores (SF-36) at 9 months of treatment. Time Frame: 270 ± 14 days Measure: Subjects' quality of life scores (SF-36) at 12 months of treatment. Time Frame: 360 ± 14 days ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * 18 years old ≤65 years old; * Thyroid ultrasonography found thyroid nodules, may be accompanied by goiter, and the nodules meet the following conditions: 1) single nodules, or dominant nodules in multiple nodules (the largest diameter of the second largest nodules does not exceed 50% of the largest nodules), 2) solid nodules, 3) the longest diameter of nodules ≥1cm and \< 3cm, 4) C-TIRADS 3\~4A nodules; * Patients who met the puncture indications were confirmed by fine needle aspiration biopsy (FNAB) as benign nodules (Bethesda Class II); * Serum TSH, free thyroid hormone (FT3, FT4) levels were normal, anti-thyroglobulin (TgAb) and anti-thyroid peroxidase (TPOAb) antibody titers were normal; * Meet the diagnostic criteria of thyroid nodules in TCM; * Sign the informed consent. Exclusion Criteria: * Exclude the patients with Deficiency of Yang syndrome, and the following two conditions can be diagnosed: Shortness of breath, abdominal pain and diarrhea, diarrhea with undigested food, Insufficiency with chills, exhaustion and lethargy, pale tongue and white fur, deep and weak pulse * Those who have reproductive needs during pregnancy, lactation and within the last 12 months; * Patients with high possibility of thyroid cancer indicated by ultrasonic signs and malignant confirmed by fine needle biopsy; * Patients who meet the indications for thyroid nodule surgery, such as local compression symptoms obviously related to the nodule, the tumor is located behind the sternum or in the mediastinum, or strongly require surgery due to appearance or ideological concerns affecting normal life; * Patients who have taken prunella preparations or other similar Chinese medicines to treat the disease within the past 1 month; Patients using glucocorticoids in the last 3 months; * Patients who have had or plan to take thyroid hormone, iodine compound, or antithyroid drug therapy during the study period; * Patients who have previously or plan to undergo ablation, neck radiation, surgery and other non-drug treatments during the study period; * Patients with parathyroid tumor (PTA), medullary thyroid cancer (MTC) or other malignant tumors, or patients with serious cardiovascular disease, liver and kidney disease, osteoporosis, or patients with a history of mental illness; * Patients with a family history of thyroid cancer or thyroid cancer syndrome; * Laboratory test index ALT, AST \> 1.5 times the upper limit of reference value or blood creatinine (Scr) \> the upper limit of reference value; * Persons who are known to be allergic to the investigational drug or its ingredients; * Other patients determined by the investigator to be unsuitable for participation in the study. Maximum Age: 65 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Wenjing Ji Phone: +86 18365572279 Role: CONTACT Contact 2: Email: [email protected] Name: Biao Chen Phone: +86 13915637727 Role: CONTACT #### Locations Location 1: City: Chongqing Contacts: *Contact 1:* - Name: Hongting Zheng - Role: SUB_INVESTIGATOR Country: China Facility: Second Hospital of Army Military Medical University State: Chongqing Location 2: City: Xiamen Contacts: *Contact 1:* - Name: Tianchi Hu - Role: SUB_INVESTIGATOR Country: China Facility: Xiamen Hospital of Traditional Chinese Medicine State: Fujian Location 3: City: Guangzhou Contacts: *Contact 1:* - Phone: （020）83827812 - Role: CONTACT *Contact 2:* - Name: Haixia Guan - Role: SUB_INVESTIGATOR Country: China Facility: People's Hospital of Guangdong Province State: Guangdong Location 4: City: Shenzhen Contacts: *Contact 1:* - Name: Fan Zhang - Role: SUB_INVESTIGATOR Country: China Facility: Shenzhen Hospital of Peking University State: Guangdong Location 5: City: Shunde Contacts: *Contact 1:* - Phone: 0757-22318000 - Role: CONTACT *Contact 2:* - Name: Jie Shen - Role: SUB_INVESTIGATOR Country: China Facility: Shunde Hospital of Southern Medical University State: Guangdong Location 6: City: Wuhan Contacts: *Contact 1:* - Name: Mingsong Gao - Role: SUB_INVESTIGATOR Country: China Facility: Wuhan First Hospital State: Hubei Location 7: City: Nanjing Contacts: *Contact 1:* - Name: Chao Liu - Role: SUB_INVESTIGATOR Country: China Facility: Jiangsu Province Hospital of Integrated Chinese and Western Medicine State: Jiangsu Location 8: City: Xuzhou Contacts: *Contact 1:* - Name: Hongwei Lin - Role: SUB_INVESTIGATOR Country: China Facility: Xuzhou Medical University Hospital State: Jiangsu Location 9: City: Dalian Country: China Facility: The Second Hospital of Dalian Medical University State: Liaoning Location 10: City: Shenyang Contacts: *Contact 1:* - Name: Yuqing Li - Phone: +86 15140139773 - Role: CONTACT *Contact 2:* - Name: Zhongyan Shan - Role: PRINCIPAL_INVESTIGATOR Country: China Facility: The First Hospital of China Medical University State: Liaoning Zip: 200032 Location 11: City: Shenyang Contacts: *Contact 1:* - Phone: 82961387 - Role: CONTACT *Contact 2:* - Name: Tianshu Gao - Role: SUB_INVESTIGATOR Country: China Facility: Hospital of Liaoning University of Chinese Medicine State: Liaoning Location 12: City: Shenyang Contacts: *Contact 1:* - Phone: 024-24016001 - Role: CONTACT *Contact 2:* - Name: Binhong Wen - Role: SUB_INVESTIGATOR Country: China Facility: People's Hospital of Liaoning Province State: Liaoning Location 13: City: Qingdao Contacts: *Contact 1:* - Name: Jie Zhu - Role: CONTACT *Contact 2:* - Name: Yangang Wang - Role: PRINCIPAL_INVESTIGATOR Country: China Facility: The First Hospital of Qingdao University State: Shandong Location 14: City: Weifang Contacts: *Contact 1:* - Phone: 963360 - Role: CONTACT *Contact 2:* - Name: Haixia Liu - Role: SUB_INVESTIGATOR Country: China Facility: Weifang People's Hospital State: Shandong Location 15: City: Weihai Contacts: *Contact 1:* - Phone: 0631-5287120 - Role: CONTACT *Contact 2:* - Name: Yachao Yang - Role: SUB_INVESTIGATOR Country: China Facility: Weihai Hospital State: Shandong Location 16: City: Shanghai Contacts: *Contact 1:* - Phone: 02163864050-510905 - Role: CONTACT *Contact 2:* - Name: Dongjie Shen - Role: SUB_INVESTIGATOR Country: China Facility: Ruijin Hospital Luwan Branch, Shanghai Jiao Tong University School of Medicine State: Shanghai Location 17: City: Shanghai Contacts: *Contact 1:* - Name: Shen Qu - Role: SUB_INVESTIGATOR Country: China Facility: Shanghai 10th People's Hospital State: Shanghai Location 18: City: Shanghai Contacts: *Contact 1:* - Name: Yongde Peng - Role: SUB_INVESTIGATOR Country: China Facility: Shanghai First People's Hospital State: Shanghai Location 19: City: Shanghai Contacts: *Contact 1:* - Name: Jin'an Zhang - Role: SUB_INVESTIGATOR Country: China Facility: Shanghai Pudong Zhoupu Hospital State: Shanghai Location 20: City: Kunming Contacts: *Contact 1:* - Name: Heng Su - Role: SUB_INVESTIGATOR Country: China Facility: First People's Hospital of Yunnan Province State: Yunnan Location 21: City: Kunming Contacts: *Contact 1:* - Phone: 0871-65324888 - Role: CONTACT *Contact 2:* - Name: Yushan Xu - Role: SUB_INVESTIGATOR Country: China Facility: The First Hospital of Kunming Medical University State: Yunnan Location 22: City: Hangzhou Contacts: *Contact 1:* - Name: Xin Mu - Role: SUB_INVESTIGATOR Country: China Facility: Zhejiang Province Hospital of Integrated Chinese and Western Medicine State: Zhejiang ## Derived Section ### Condition Browse Module - Ancestors - ID: D000004700 - Term: Endocrine System Diseases - ID: D000013964 - Term: Thyroid Neoplasms - ID: D000004701 - Term: Endocrine Gland Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000006258 - Term: Head and Neck Neoplasms ### Condition Browse Module - Browse Branches - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC04 - Name: Neoplasms ### Condition Browse Module - Browse Leaves - ID: M16718 - Name: Thyroid Diseases - Relevance: HIGH - As Found: Thyroid - ID: M18986 - Name: Thyroid Nodule - Relevance: HIGH - As Found: Thyroid Nodules - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown - ID: M16723 - Name: Thyroid Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7863 - Name: Endocrine Gland Neoplasms - Relevance: LOW - As Found: Unknown - ID: M9348 - Name: Head and Neck Neoplasms - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000016606 - Term: Thyroid Nodule - ID: D000013959 - Term: Thyroid Diseases ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423222 Brief Title: Anal Incontinence and Its Impact on Quality of Life and Physical Activity Among Hungarian Women and the Hungarian Language Validation of the International Consultation on Incontinence Modular Questionnaire-Bowels (ICIQ-B) Official Title: Prevalence of Anal Incontinence and Its Impact on Quality of Life and Physical Activity Among Hungarian Women Who Have Given Birth, and the Hungarian Language Validation of the International Consultation on Incontinence Modular Questionnaire-Bowels (ICIQ-B) #### Organization Study ID Info ID: BM/5814-3/2024 #### Organization Class: OTHER Full Name: University of Pecs ### Status Module #### Completion Date Date: 2027-07 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2026-01 Type: ESTIMATED #### Start Date Date: 2024-04-22 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-05 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: University of Pecs #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The aim of the study is to assess the prevalence of anal incontinence among Hungarian women who have given birth at least once before, and to examine the impact of anal incontinence on the quality of life and physical activity of these women. A further aim of our study is to adapt the Hungarian version of the International Consultation on Incontinence Modular Questionnaire - Bowels (ICIQ-B) and to assess its validity and reliability. ### Conditions Module Conditions: - Anal Incontinence Keywords: - Anal Incontinence - Quality of Life - Physical Activity - Questionnaire ### Design Module #### Design Info Observational Model: CASE_ONLY Time Perspective: CROSS_SECTIONAL #### Enrollment Info Count: 250 Type: ESTIMATED Study Type: OBSERVATIONAL ### Outcomes Module #### Primary Outcomes Description: Assessing with questionnaire: International Consultation on Incontinence Modular Questionnaire-Bowels (ICIQ-B). The ICIQ-B is a patient-completed questionnaire to assess the symptoms and impact on quality of life (QoL) of anal incontinence (including flatus incontinence). The ICIQ-B consists of 21 items, divided into three domains: Bowel pattern (1 - 21), bowel control (0 - 28), Quality of life (0 - 26). Seventeen items are scored items and the remaining four are unscored. Higher scores indicate more symptoms. Measure: Anal Incontinence Impact on Quality of Life Time Frame: Through study completion, an average of 3 years Description: Assessing with questionnaire: Global Physical Activity Questionnaire (GPAQ). The Global Physical Activity Questionnaire was developed by WHO to monitor physical activity in countries. It collects information from 16 questions (P1-P16) on participation in physical activity in three domains (Workplace activity, Travel to and from places, Leisure activities) and sedentary behavior. Metabolic equivalent (MET) values are applied to the time variables according to the intensity of the activity (moderate or high). The application of MET values to activity levels allows the calculation of total physical activity. Measure: Anal Incontinence Impact on Physical Activity Time Frame: Through study completion, an average of 3 years Description: Evaluating with statistical analysis the content/face validity, internal consistency, construct validity, test-retest reproducibility, discriminant validity and convergent validity. Measure: Adaptation, validity and reliability of the Hungarian version of the International Consultation on Incontinence Modular Questionnaire-Bowels (ICIQ-B) Time Frame: Through study completion, an average of 3 years #### Secondary Outcomes Description: Assessing with questionnaire: The Hungarian version of the Australian Pelvic Floor Questionnaire (APFQ-H). The APFQ-H consists of four domains: bladder function (15 items), bowel function (12 items), prolapse symptoms (5 items) and sexual function (10 items). Thirty-eight of the items assess pelvic floor symptoms and four questions assess the bother caused by symptoms in each domain. Most items in the questionnaire use a 4-point scoring system. The score obtained for each domain ranges from 0 to 10. The sum of the subscores in the four domains gives the APFQ-H global score. The higher the score, the more severe the pelvic floor symptoms. Measure: Additional pelvic floor symptoms Time Frame: Through study completion, an average of 3 years Description: Assessing with questionnaire: Hungarian WHOQOL-BREF. The WHOQOL-BREF is a self-administered questionnaire that contains 26 questions about an individual's health and well-being over the previous two weeks. Answers to the questions are given on a Likert scale of 1-5. The WHOQOL-BREF covers four domains (physical health, psychological, social relationships, environment). Scores in each of the 4 domains are converted into a scale ranging from 0 to 100. A score of 0 represents the worst possible health status, while a score of 100 represents the best possible health status for that domain. Measure: Global Quality of Life Time Frame: Through study completion, an average of 3 years ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Have given birth at least once before * Native Hungarian language Exclusion Criteria: * Menopause * Irritable Bowel Syndrome (IBS) * Chron's disease * Ulcerative colitis * Developmental abnormalities at the level of the pelvic organs * Uninvestigated pelvic pain * Malignant pelvic tumor * Radiotherapy involving the pelvis * Neurological diseases with muscle weakness * Parkinson's disease * Intellectual disability Healthy Volunteers: True Maximum Age: 50 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: FEMALE Standard Ages: - ADULT Study Population: We plan to include subjects who are female, over the age of 18, under the age of 50 and who have given birth at least once before. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Márta Hock, PhD Phone: +36-30-7213156 Role: CONTACT Contact 2: Email: [email protected] Name: Eszter Ambrus Role: CONTACT #### Locations Location 1: City: Pécs Contacts: *Contact 1:* - Email: [email protected] - Name: Márta Hock, Phd - Phone: +36-30-7213156 - Role: CONTACT Country: Hungary Facility: Doctoral School of Health Sciences, Faculty of Health Sciences, University of Pécs State: Baranya Status: RECRUITING Zip: H-7621 #### Overall Officials Official 1: Affiliation: University of Pécs Faculty of Health Sciences Name: Márta Hock, PhD Role: STUDY_DIRECTOR Official 2: Affiliation: Doctoral School of Health Sciences, Faculty of Health Sciences, University of Pécs, Pécs, Hungary Name: Eszter Ambrus Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000012002 - Term: Rectal Diseases - ID: D000007410 - Term: Intestinal Diseases - ID: D000005767 - Term: Gastrointestinal Diseases - ID: D000004066 - Term: Digestive System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: All - Name: All Conditions - Abbrev: BXM - Name: Behaviors and Mental Disorders ### Condition Browse Module - Browse Leaves - ID: M8381 - Name: Fecal Incontinence - Relevance: HIGH - As Found: Anal Incontinence - ID: M14844 - Name: Rectal Diseases - Relevance: LOW - As Found: Unknown - ID: M10444 - Name: Intestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: T6034 - Name: Quality of Life - Relevance: HIGH - As Found: Quality of Life ### Condition Browse Module - Meshes - ID: D000005242 - Term: Fecal Incontinence ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423209 Acronym: Vegan Brief Title: Efficacy of a Training Program in Adults Following a Vegan Diet Versus an Omnivorous Diet Official Title: Efficacy of an Omnivorous Versus a Vegan Diet in the Prevention or Treatment of Sarcopenia in Chilean Adults Following a Strength Training Program #### Organization Study ID Info ID: CEBB 1068-2021 #### Organization Class: OTHER Full Name: Universidad de Concepcion ### Status Module #### Completion Date Date: 2022-10-30 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: COMPLETED #### Primary Completion Date Date: 2022-05-02 Type: ACTUAL #### Start Date Date: 2022-02-02 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-20 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Universidad de Concepcion #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The study consisted of a non-randomized controlled clinical trial with measurements at baseline and at the end of a 16 week intervention. Participants will be assigned to the intervention or control group according to their own choice and convenience. A 4 arm split was performed where the Veg-Int group was composed of people on a vegan diet who participated in the intervention, the Veg-Con group was composed of people on a vegan diet who were part of the control group, the Omn-Int group was composed of people on an omnivorous diet who participated in the intervention, and the Omn-Con group was composed of people on an omnivorous diet who were part of the control group. The Veg-Int and Omn-Int intervention groups, participated in a physical exercise program in remote modality through a digital mHealth platform. During the 16 weeks of intervention, a total of 50 training sessions were carried out, distributed in three sessions per week, with a duration per session ranging from 40 to 50 minutes. The exercise program was designed and supervised by a physical education teacher and focused on strength training using body weight exercises targeting the major muscle groups, including upper body, lower body and abdominals. The platform recorded participants attendance and the time they spent on each exercise session. At the end of the sessions, participants had the option to evaluate and share their perception of effort during the workout through a Modified Borg scale (0-10). In addition, they were given the opportunity to communicate with the teacher via phone call, text message or e-mail, to receive feedback or raise doubts. Detailed Description: All participants were evaluated in weeks 0 and 17, immediately after the intervention program, under the same conditions in terms of protocol, calibrated instruments and the same evaluator. The evaluation of nutritional status was carried out using the body mass index (BMI, Kg/m2), while the waist circumference was measured by passing a measuring tape at the height of the navel, midpoint between the costal margin and the crest. iliac, at the end of a normal expiration and recorded in centimeters. Body composition analysis was obtained by the bioimpedance method, using a segmented bioimpedance meter. The measurements were carried out under fasting conditions for at least 4 hours, without having performed physical exercise in the last 12 hours, without consuming stimulating drinks such as caffeine and avoiding the menstrual period. From the body composition information, the data Percentage of Fat Mass, Kilos of Fat Mass and Kilos of Lean Mass were recorded. The level of physical activity was assessed through a self-report questionnaire of physical activity and sitting time in the last 7 days, using the abbreviated version of the International Physical Activity Questionnaire (. The questionnaire was administered by a physical activity professional, and the data were reported in minutes per day to estimate the total PA performed, and the time reported was corrected by its metabolic equivalent . The type of diet was corroborated through a quantified food consumption trend survey, which included 14 groups; vegetables, fruits, dairy and vegetable options, meat-fish-seafood and egg, legumes, vegan protein preparations, grains and cereals, fats and oils, nuts, sugars and sweets, alcohol, snacks, coffee and infusions, food supplements. The questionnaire was administered individually by a dietitian nutritionist to each participant. ### Conditions Module Conditions: - Physical Activity Keywords: - vegan diet - omnivorous diet - strength training ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: The study consisted of a 4-arm non-randomized controlled clinical trial, with measurements at the beginning and end of a 16-week intervention. ##### Masking Info Masking: DOUBLE Who Masked: - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: OTHER #### Enrollment Info Count: 83 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The intervention group is composed of people who follow a vegan diet and who will be part of an intervention program for 16 weeks, consisting of a physical exercise program of strength resistance with 3 sessions per week. Each session will be guided by a physical activity professional and will last from 45 to 50 minutes. Intervention Names: - Other: Strength training program Label: Vegan Intervention Type: EXPERIMENTAL #### Arm Group 2 Description: The intervention group is composed of people who follow a omnivorous diet and who will be part of an intervention program for 16 weeks, consisting of a physical exercise program of strength resistance with 3 sessions per week. Each session will be guided by a physical activity professional and will last from 45 to 50 minutes. Intervention Names: - Other: Strength training program Label: omnivorous intervention Type: EXPERIMENTAL #### Arm Group 3 Description: People who follow an vegan diet who were part of the control group. They were evaluated before and after the intervention. Label: vegan control Type: NO_INTERVENTION #### Arm Group 4 Description: People who follow an omnivorous diet who were part of the control group. They were evaluated before and after the intervention. Label: omnivorous control Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Vegan Intervention - omnivorous intervention Description: Strength training program to be developed during 16 weeks. There will be 3 exercise sessions per week and those participants who perform at least 2 sessions during the program will be considered for the statistical analysis. Name: Strength training program Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Differential between kg of body weight before and after the development of the intervention Measure: Body weight Time Frame: 16 weeks of intervention Description: Differential between centimeters of waist circumference before and after the development of the intervention Measure: waist circumference Time Frame: 16 weeks of intervention Description: Differential of the percentage of fat mass before and after the intervention Measure: fat mass Time Frame: 16 weeks of intervention Description: Differential of kilograms of lean mass before and after the intervention Measure: Lean mass Time Frame: 16 weeks of intervention Description: Differential of kilograms of maximum strength by biceps curl exercise Measure: maximum strength Time Frame: 16 weeks of intervention Description: Differential of manual grip strength of both hands using a hydraulic dynamometer. Measure: Manual grip strength Time Frame: 16 weeks of intervention Description: Differential evaluation of muscle power by means of a vertical jump Measure: Vertical jump Time Frame: 16 weeks of intervention ### Eligibility Module Eligibility Criteria: Inclusion Criteria:People between 18 and 59 years old who follow a vegan or omnivorous diet for at least the last 6 months prior to the study. - Exclusion Criteria: Those who were doing strength training or doing less than 3 hours of vigorous exercise per week did not have health compatible with the activities of this study. People with a diagnosis of diabetes, uncontrolled hypertension (Systolic Blood Pressure ≥150 and/or Diastolic Blood Pressure ≥90 mmHg). People who were undergoing treatment for cancer, chronic kidney failure, or who reported a health problem in the previous fitness for physical activity questionnaire (PAR-Q). - Healthy Volunteers: True Maximum Age: 59 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT ### Contacts Locations Module #### Locations Location 1: City: Concepción Country: Chile Facility: Richar Carcamo Regla State: Concepcion Zip: 4030000 #### Overall Officials Official 1: Affiliation: Universidad de Concepcion Name: Rafael E Zapata Lamana, Doctor Role: STUDY_DIRECTOR ### IPD Sharing Statement Module Description: Has not been considered or discussed yet IPD Sharing: NO ### References Module #### References Citation: Boutros GH, Landry-Duval MA, Garzon M, Karelis AD. Is a vegan diet detrimental to endurance and muscle strength? Eur J Clin Nutr. 2020 Nov;74(11):1550-1555. doi: 10.1038/s41430-020-0639-y. Epub 2020 Apr 24. PMID: 32332862 Citation: Hevia-Larrain V, Gualano B, Longobardi I, Gil S, Fernandes AL, Costa LAR, Pereira RMR, Artioli GG, Phillips SM, Roschel H. High-Protein Plant-Based Diet Versus a Protein-Matched Omnivorous Diet to Support Resistance Training Adaptations: A Comparison Between Habitual Vegans and Omnivores. Sports Med. 2021 Jun;51(6):1317-1330. doi: 10.1007/s40279-021-01434-9. Epub 2021 Feb 18. PMID: 33599941 Citation: Reid-McCann RJ, Brennan SF, McKinley MC, McEvoy CT. The effect of animal versus plant protein on muscle mass, muscle strength, physical performance and sarcopenia in adults: protocol for a systematic review. Syst Rev. 2022 Apr 13;11(1):64. doi: 10.1186/s13643-022-01951-2. PMID: 35418173 Citation: van de Brekel JA, Duurkens VA, Vanderschueren RG. Pneumothorax. Results of thoracoscopy and pleurodesis with talc poudrage and thoracotomy. Chest. 1993 Feb;103(2):345-7. doi: 10.1378/chest.103.2.345. PMID: 8432116 Citation: Hannaian SJ, Churchward-Venne TA. Meatless Muscle Growth: Building Muscle Size and Strength on a Mycoprotein-Rich Vegan Diet. J Nutr. 2023 Jun;153(6):1665-1667. doi: 10.1016/j.tjnut.2023.04.011. Epub 2023 Apr 14. No abstract available. PMID: 37062484 Citation: Pohl A, Schunemann F, Bersiner K, Gehlert S. The Impact of Vegan and Vegetarian Diets on Physical Performance and Molecular Signaling in Skeletal Muscle. Nutrients. 2021 Oct 29;13(11):3884. doi: 10.3390/nu13113884. PMID: 34836139 ## Derived Section ### Condition Browse Module - Browse Branches - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M28396 - Name: Sarcopenia - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423196 Brief Title: Upper Limb Blood Flow Restriction in Handball Players Official Title: Efficacy of Upper Limb Blood Flow Restriction in Handball Players. Randomised Clinical Study #### Organization Study ID Info ID: Floss-Hand #### Organization Class: OTHER Full Name: Universidad Católica San Antonio de Murcia ### Status Module #### Completion Date Date: 2024-07-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-06-15 Type: ESTIMATED #### Start Date Date: 2024-05-19 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-20 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Universidad Católica San Antonio de Murcia #### Responsible Party Investigator Affiliation: Universidad Católica San Antonio de Murcia Investigator Full Name: Rubén Cuesta-Barriuso, PhD Investigator Title: Principal Investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Introduction. Blood flow restriction therapy involves the use of an occlusion cuff placed over an extremity resulting in a partial reduction of arterial blood flow and total restriction of venous return. Objectives. To analyse the efficacy of a physiotherapy intervention using blood flow restriction in improving upper limb strength in adult handball players. Methods. Randomised, single-blind, clinical study. 20 athletes will be recruited and randomly assigned to the experimental and control groups. The intervention of the experimental group will consist of performing an exercise protocol after blood flow restriction. The intervention period will last 4 weeks, with a periodicity of 2 weekly sessions of 30 minutes each. The primary variable will be the strength of the triceps, epicondyle and epitrochlear musculature (pressure hand dynamometer). The secondary variable will be the muscle activation of this musculature (surface electromyography). ### Conditions Module Conditions: - Sports Physical Therapy Keywords: - Handball - Blood flow restriction - Muscle strength - Muscle activation - Upper limbs - Physiotherapy ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Masking Description: Three assessments will be made throughout the study: before the intervention (T0), after the experimental phase (T1) and after a 4-week follow-up period (T2). All variables will be assessed by an evaluator blinded to the assignment of the athletes to the study groups. Who Masked: - OUTCOMES_ASSESSOR Primary Purpose: PREVENTION #### Enrollment Info Count: 20 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The intervention of the experimental group will consist of performing an exercise protocol after carrying out the blood flow restriction. A total of 6 muscle strength exercises will be performed for the proximal (triceps brachii) and forearm (epitrochlear and epicondylar muscles). Intervention Names: - Other: Experimental group Label: Experimental group Type: EXPERIMENTAL #### Arm Group 2 Description: Patients included in the control group will continue with their pre-study training and activities, without modifying their routine. Label: Control group Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Experimental group Description: In the development of the exercises, the players will mobilise dumbbells of different weights that will be estimated according to the calculation of 30% of 1 RM. This workload with dumbbells is based on previous work where blood flow restriction was used in healthy athletes. Name: Experimental group Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Muscle strength will be assessed with a pressure dynamometer (Lafayette Manual Muscle model). The strength of the triceps brachii, epicondyle and epitrochlear musculature will be measured. The evaluation protocol used by Morin et al. will be used. The unit of measurement is the Newton (the higher the value, the greater the muscle strength). The measurements are taken bilaterally. The mean value of the 2 measurements taken shall be used as a measure. Measure: Assess the muscle strength at screening visit Time Frame: Screening visit, within the first seven days after treatment and after four weeks follow-up #### Secondary Outcomes Description: Muscle activation will be measured by surface electromyography (model SHIMMMER2, Shimmer, Ireland). Electrode placement will be marked on standing subjects, and will be positioned according to European recommendations for the use of surface electromyography. A bipolar SEMG system will be used with circular electrodes of 10 mm diameter, 20 mm apart, placed longitudinally, in the direction of the muscle fibres under study, and with a reference electrode at a distance. The unit of measurement is µV, where the higher the score, the greater the muscle activation. Measure: Assess the muscle activation at screening visit Time Frame: Screening visit, within the first seven days after treatment and after four weeks follow-up ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Athletes over 18 years of age. * Federated in handball at the time of the study. * No lower limb injuries in the three months prior to the study. * Signing the informed consent document. Exclusion Criteria: * Athletes who have undergone surgery in the year prior to the study. * People who do not attend at least 80% of the treatment sessions. * Players who are receiving physiotherapy treatment in parallel to the physical preparation of the team they are playing for. Healthy Volunteers: True Maximum Age: 30 Years Minimum Age: 18 Years Sex: MALE Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Rubén Cuesta-Barriuso, PhD Phone: 607547274 Role: CONTACT #### Locations Location 1: City: Murcia Country: Spain Facility: Universidad Católica San Antonio, Murcia Zip: 30107 ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423183 Acronym: IMPACT Brief Title: Interprofessional Mindfulness Practices Advancing Cancer Teamwork Official Title: Interprofessional Mindfulness Practices Advancing Cancer Teamwork (IMPACT Study) #### Organization Study ID Info ID: 2024-0517 #### Organization Class: OTHER Full Name: University of Wisconsin, Madison #### Secondary ID Infos Domain: UW Madison ID: A539713 Type: OTHER Domain: UW Madison ID: Protocol Version Type: OTHER ### Status Module #### Completion Date Date: 2025-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-06 Type: ESTIMATED #### Start Date Date: 2024-06 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: University of Wisconsin, Madison #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: The purpose of the research is to understand if mindfulness team training can improve the well-being and teamwork in caring for oncology patients. This study will enroll healthcare professionals in oncology teams, including clinic nurses, nurse managers, medical assistants, social workers, technicians, patient navigators, advanced practice providers, and physicians at UW Madison. Participants will be on study for up to approximately 6 months. Detailed Description: Aim 1: Determine the effect of resilience training on team resilience and well-being. The investigators test the hypothesis that resilience training provided to interprofessional oncology care teams will improve team resilience and individual well-being. Aim 2: Determine the feasibility and acceptability of a resilience training on team resilience. The investigators test the hypothesis that resilience training is feasible and acceptable in interprofessional oncology care teams. ### Conditions Module Conditions: - Burn Out Keywords: - oncology - health care - clinicians - mindfulness - well-being ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP Intervention Model Description: This study is a prospective, pre-post study at a single institution ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 50 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Behavioral: A Mindful Approach to Building a Resilient Healthcare Workforce (RENEW) Label: Mindfulness-Based Team Resilience Training Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Mindfulness-Based Team Resilience Training Description: Synchronous, 4-month intervention that teaches skills in mindfulness, stress management, and resilience as an individual and as a team. Sessions occur monthly and include a 1 hour in-person introductory session followed by 3 50-minute virtual sessions. Name: A Mindful Approach to Building a Resilient Healthcare Workforce (RENEW) Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: 4-item Edmondson's psychology safety scale is scored on a likert scale from 1 (strongly disagree) to 7 (strongly agree), where higher scores indicate higher psychology safety Measure: Change in Teamwork Measure Time Frame: baseline (pre-intervention), post-intervention (3 months), follow up (6 months) Description: Session 1 baseline, session 2 at 1 month, session 3 at 2 months, session 4 at 3 months Measure: Number of Participants Who Attend Each Session Time Frame: up to 3 months Description: AIM is a 4-item survey scored on a 5 point likert scale from 1 (completely disagree) to 5 (completely agree), where higher scores indicate greater acceptability. Measure: Acceptability of Intervention Measure (AIM) Time Frame: up to 3 months Description: IAM is a 4-item survey scored on a 5 point likert scale from 1 (completely disagree) to 5 (completely agree), where higher scores indicate greater appropriateness. Measure: Intervention Appropriateness Measure (IAM) Time Frame: up to 3 months Description: FIM is a 4-item survey scored on a 5 point likert scale from 1 (completely disagree) to 5 (completely agree), where higher scores indicate greater feasibility. Measure: Feasibility of Intervention Measure (FIM) Time Frame: up to 3 months #### Secondary Outcomes Description: PSS is a 10-item survey scored from 0 (never) to 4 (very often) for a total possible range of scores from 0-40 where higher scores indicate higher perceived stress. Measure: Change in Stress measured by Perceived Stress Scale (PSS) Time Frame: baseline (pre-intervention), post-intervention (3 months), follow up (6 months) Description: This is a 2-item survey scored from 0-6 where higher scores indicate increased burnout. Measure: Change in Burnout measured by Maslach Burnout Inventory Time Frame: baseline (pre-intervention), post-intervention (3 months), follow up (6 months) Description: CD-RISC 2 is a 2-item survey each scored on a 5 point likert scale from 0 (not true at all) to 4 (true nearly all of the time), higher scores indicate increased resilience. Measure: Change in Resilience measured by Connor Davidson Resilience Scale (CD-RISC 2) Time Frame: baseline (pre-intervention), post-intervention (3 months), follow up (6 months) Description: Flourishing measure is a 12-item survey that measure well being in each of 6 domains: happiness and life satisfaction; mental and physical health; meaning and purpose; character and virtue; close social relationships; financial and material stability. Each domain is scored from 0 - 10 where higher numbers are indicative of increased well being. Measure: Change in Well-being measured by Flourishing Index Time Frame: baseline (pre-intervention), post-intervention (3 months), follow up (6 months) ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * A care provider in an oncology clinic team (clinic nurse, nurse manager, medical assistant, technician, social worker, patient navigator, advanced practice provider, physician) Exclusion Criteria: * Does not participate in patient care or support services Healthy Volunteers: True Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Syndey Tan, MD Phone: 608-263-7502 Role: CONTACT #### Locations Location 1: City: Madison Country: United States Facility: UW Carbone Cancer Center State: Wisconsin Zip: 53792 #### Overall Officials Official 1: Affiliation: UW Carbone Cancer Center Name: Lee Wilke, MD, FACS Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000013315 - Term: Stress, Psychological - ID: D000001526 - Term: Behavioral Symptoms ### Condition Browse Module - Browse Branches - Abbrev: BC26 - Name: Wounds and Injuries - Abbrev: All - Name: All Conditions - Abbrev: BXM - Name: Behaviors and Mental Disorders ### Condition Browse Module - Browse Leaves - ID: M5326 - Name: Burns - Relevance: LOW - As Found: Unknown - ID: M1658 - Name: Burnout, Psychological - Relevance: HIGH - As Found: Burn Out - ID: M16105 - Name: Stress, Psychological - Relevance: LOW - As Found: Unknown - ID: M4818 - Name: Behavioral Symptoms - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000077062 - Term: Burnout, Psychological ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423170 Brief Title: A Single-arm Phase II Clinical Study of the Efficacy and Safety of Camrelizumab Combined With GEMOX for Unresectable GBCs Official Title: Camrelizumab Plus Gemcitabine and Oxaliplatin (GEMOX) in Patients for Unresectable Gallbladder Cancer: a Single-arm, Phase II Trial #### Organization Study ID Info ID: SYSKY-2022-516 #### Organization Class: OTHER Full Name: Sun Yat-Sen Memorial Hospital of Sun Yat-Sen University ### Status Module #### Completion Date Date: 2026-12-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-12-31 Type: ESTIMATED #### Start Date Date: 2023-06-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Sun Yat-Sen Memorial Hospital of Sun Yat-Sen University #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: The aim of this study was to evaluate the efficacy and safety of Camrelizumab combined with gemcitabine and oxaliplatin (GEMOX) for unresectable gallbladder cancer. Patients with unresectable gallbladder cancer were enrolled to receive gemcitabine 1000mg/m2 D1+oxaliplatin 100mg/m2, D1+Camrelizumab 200mg, D1, in 21-day cycles for 6-8 cycles, with serum tumour markers assessed at each course and abdominal CTA performed every two courses, until tumour progression occurs.The primary indicators of this study are radical tumor resection rate; secondary indicators are disease control rate, objective response rate,progression-free survival and overall survival; safety indicators: incidence and severity of adverse events (AEs) and serious adverse events (SAEs) according to NCI-CTCAEv5.0 criteria. 37 patients are expected to be recruited for this study. ### Conditions Module Conditions: - Unresectable Gallbladder Cancer Keywords: - PD-1；GEMOX；Unresectable gallbladder cancer. ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 37 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Camrelizumab plus GEMOX was given as conversion therapy for unresectable gallbladder cancer Intervention Names: - Drug: Camrelizumab plus GEMOX Label: Camrelizumab plus GEMOX Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Camrelizumab plus GEMOX Description: 1. Camrelizumab：200mg，D1，intravenous infusion, the administration time is 60 (+15) minutes. 2. GEMOX chemotherapy : oxaliplatin 100mg/m2，D1, gemcitabine1000mg/m2，D1，intravenous infusion. 3. Carrilizumab and GEMOX chemotherapy will be intravenous infused atone day. Three weeks is a course of treatment,a total of 6-8 courses. Name: Camrelizumab plus GEMOX Type: DRUG ### Outcomes Module #### Primary Outcomes Description: The proportion of patients with negative surgical resection margins in the study group Measure: radical tumor resection rate Time Frame: 6 months #### Secondary Outcomes Description: The proportion of patients whose tumours shrink or remain stable for a certain period of time and includes cases of complete remission (CR), partial remission (PR) and stable (SD). Measure: Disease Control Rate，DCR Time Frame: 6 months Description: The time between the start of treatment for disease and the observation of disease progression or the occurrence of death from any cause Measure: Progress Free Survival，PFS Time Frame: 6 months Description: The time between the start of the diagnosis of unresectable gallbladder cancerand death from any cause Measure: Overall Survival，OS Time Frame: 6 months Description: The proportion of patients whose tumour volume shrinks to a pre-defined value and who are able to maintain the minimum time requirement is the sum of the proportion in complete remission (CR) and partial remission (PR) Measure: Objective response rate，ORR Time Frame: 6 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Patients aged 18-75 years 2. Patients with unresectable gallbladder cancer clearly diagnosed by puncture pathology or the presence of tumour cells in the bile 3. No history of chemotherapy or immunotherapy 4. ECOG score 0-1 within 1 week prior to enrollment 5. Expected survival \> 3 months 6. The functional indicators of important organs meet the following requirements： (1)Neutrophils≥1.5\109/L; platelets≥100\109/L; hemoglobin≥9g/dl; serum albumin≥3g/dl; (2)Thyroid-stimulating hormone (TSH) ≤ 2 times the upper limit of normal, and T3 and T4 are in the normal range; (3)Bilirubin ≤ 1.5 times the upper limit of normal; ALT and AST ≤ 3 times the upper limit of normal; (4)Serum creatinine ≤ 1.5 times the upper limit of normal, and creatinine clearance ≥ 60ml/min(calculated by Cockcroft-Gault formula); 7. Female subjects of childbearing potential must have had a negative serum pregnancy study within 14 days prior to the start of study treatment and be willing to use a reliable method of contraception during the study and for 60 days after the final administration of study drug 8. Male subjects whose partner is a woman of childbearing age should agree to use a reliable method of contraception for the duration of the study and for 120 days after the last dose of study drug 9. Subjects who voluntarily enter the study, sign an informed consent form, are compliant and willing to cooperate with follow-up Exclusion Criteria: 1. Past or simultaneous suffering from other malignant tumors, except for fully treated non-melanoma skin cancer, cervical carcinoma in situ, and thyroid papillary carcinoma; 2. Have used gemcitabine-based chemotherapy or have used PD-1 monoclonal antibody or PD-L1 monoclonal antibody treatment within 6 months; 3. Severe cardiopulmonary and renal dysfunction; 4. Hypertension that is difficult to control with drugs (systolic blood pressure (BP) ≥140 mmHg and/or diastolic blood pressure≥90mmHg) (based on the average of ≥3 BP readings obtained by ≥2measurements); 5. Abnormal coagulation function (PT\>14s), have bleeding tendency or are receiving thrombolysis or anticoagulation therapy; 6. After antiviral treatment, HBV DNA\>2000 copies/ml, HCV RNA\>1000; 7. A history of esophageal and gastric varices, significant clinically significant bleeding symptoms or a clear tendency to appear within 3 months before enrollment; 8. Active infections requiring systemic treatment; patients with active tuberculosis infection within 1 year before enrollment; a history of active tuberculosis infection more than 1 year before enrollment, and no formal anti-tuberculosis treatment or tuberculosis Still in the active period; 9. Human immunodeficiency virus (HIV, HIV1/2 antibody) positive; 10. A history of psychotropic drug abuse, alcohol or drug abuse; 11. Known to have a history of severe allergies to any monoclonal antibodies, platinum drugs, or gemcitabine; 12. Other factors judged by the investigator may affect the safety of the subjects or the compliance of the trial. Such as serious diseases (including mental illness) that require combined treatment, serious laboratory abnormalities, or other family or social factors. - Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Zhang Rui, PhD Phone: 020-34078840 Role: CONTACT Contact 2: Email: [email protected] Name: Ye Yanfang Phone: 02081332587 Role: CONTACT #### Locations Location 1: City: Guangzhou Contacts: *Contact 1:* - Email: [email protected] - Name: Zhang Rui, PhD - Phone: 020-34078840 - Role: CONTACT Country: China Facility: Sun Yat-sen Memorial Hospital, Sun Yat-sen University State: Guangdong Status: RECRUITING Zip: 510288 #### Overall Officials Official 1: Affiliation: Department of Biliary and Pancreatic Surgery, Sun Yat-sen Memorial Hospital, Sun Yat-sen University Name: Zhang Rui, PhD Role: STUDY_CHAIR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001661 - Term: Biliary Tract Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000001660 - Term: Biliary Tract Diseases - ID: D000004066 - Term: Digestive System Diseases - ID: D000005705 - Term: Gallbladder Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M8824 - Name: Gallbladder Neoplasms - Relevance: HIGH - As Found: Gallbladder Cancer - ID: M4947 - Name: Biliary Tract Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M4946 - Name: Biliary Tract Diseases - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M8823 - Name: Gallbladder Diseases - Relevance: LOW - As Found: Unknown - ID: T2425 - Name: Gallbladder Cancer - Relevance: HIGH - As Found: Gallbladder Cancer ### Condition Browse Module - Meshes - ID: D000005706 - Term: Gallbladder Neoplasms ### Intervention Browse Module - Browse Branches - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M2985 - Name: Gemcitabine - Relevance: LOW - As Found: Unknown - ID: M1674 - Name: Oxaliplatin - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423157 Brief Title: Plyometric and Stability Exercise Protocol in Female Basketball Players Official Title: Efficacy of a Plyometric and Stability Exercise Protocol in Female Basketball Players. A Controlled Clinical Study. #### Organization Study ID Info ID: PlyoBask #### Organization Class: OTHER Full Name: Universidad Católica San Antonio de Murcia ### Status Module #### Completion Date Date: 2024-07-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-06-15 Type: ESTIMATED #### Start Date Date: 2024-05-19 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Universidad Católica San Antonio de Murcia #### Responsible Party Investigator Affiliation: Universidad Católica San Antonio de Murcia Investigator Full Name: Rubén Cuesta-Barriuso, PhD Investigator Title: Principal Investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Introduction. Basketball is a high intensity intermittent sport, requiring jumping, running, accelerations and decelerations with changes of direction and lateral movements. Plyometric exercises are a training technique that consists of a cycle of muscle stretching and shortening in which the energy stored in the eccentric phase (lengthening) is released facilitating the production of maximum power in the concentric phase (shortening). Objective. To analyse the efficacy of a physiotherapy intervention through a protocol of plyometric and stability exercises in the improvement of vertical jump, stability, flexibility and agility in federated female basketball players. The primary variable will be the vertical jump (My jump 2.0). Secondary variables will be stability (Y balance test), flexibility (Sit and Reach) and agility (T-Test). Methods. Controlled, single-blind clinical study. 20 athletes will be randomised to the experimental and control groups. The intervention of the experimental group will consist of a protocol using plyometric and stability exercises. The athletes included in the control group will not perform any intervention and will continue with their usual routine. The intervention period will last 6 weeks, with a periodicity of 2 weekly sessions of 20 minutes each. ### Conditions Module Conditions: - Sports Physical Therapy Keywords: - Basketball - Plyometric Exercises - Stability - Flexibility - Agility - Physiotherapy ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Masking Description: Three assessments will be made throughout the study: before the intervention (T0), after the experimental phase (T1) and after a 6-week follow-up period (T2). All variables will be assessed by an evaluator blinded to the assignment of the athletes to the study groups. Who Masked: - OUTCOMES_ASSESSOR Primary Purpose: PREVENTION #### Enrollment Info Count: 20 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The intervention period will last 6 weeks, with a periodicity of 2 weekly sessions of 20 minutes each. All interventions will take place at the Palacio de los Deportes de Murcia. All interventions will be carried out by the same physiotherapist, following the same protocol. The intervention of the experimental group will consist of a protocol using plyometric and stability exercises. Intervention Names: - Other: Intervention Label: Experimental group Type: EXPERIMENTAL #### Arm Group 2 Description: The athletes included in the control group will not undergo any intervention and will continue with their usual routine. Label: Control group Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Experimental group Description: The intervention period will last 6 weeks, with a periodicity of 2 weekly sessions of 20 minutes each. All interventions will take place at the Palacio de los Deportes de Murcia. All interventions will be carried out by the same physiotherapist, following the same protocol. The intervention of the experimental group will consist of a protocol using plyometric and stability exercises. Name: Intervention Type: OTHER ### Outcomes Module #### Primary Outcomes Description: The vertical jump will be measured with the My jump 2.0® application. The athlete will be asked to jump as high as possible from a standing position, raising the body in the air by means of an impulse generated by the leg muscles. The evaluation consists of the recording of the jump, the calculation of the height of the vertical jump and the athlete's strength and speed levels. The unit of measurement of this tool is the centimetre, where the greater the distance, the higher the vertical jump. Measure: Assess the changes in vertical jump Time Frame: Screening visit, within the first seven days after treatment and after six weeks follow-up #### Secondary Outcomes Description: Stability is measured using the Y balance test. Three strips of adhesive tape are placed on the floor in a Y shape. The athlete, placed in the centre of the Y, will maintain unipodal balance while with the contralateral leg trying to reach the farthest point in each direction (anterior, posteromedial and posterolateral), without lifting the heel of the supporting foot which is the one being evaluated. Three attempts shall be made with each leg. The distance is measured with a tape measure, in centimetres (19), where the greater the distance, the greater the stability. Measure: Assess the changes in stability Time Frame: Screening visit, within the first seven days after treatment and after six weeks follow-up Description: Flexibility will be assessed with the Sit and Reach test. The athlete will sit on the floor, with her knees straight and her feet placed against the edge of a box. From this position, the participant shall progressively perform a trunk flexion, trying to reach as far as possible with the tips of her hands on the scale graduated in centimetres on the box. The unit of measurement for this test is the centimetre, where the greater the distance reached, the greater the flexibility. Measure: Assess the changes in flexibility Time Frame: Screening visit, within the first seven days after treatment and after six weeks follow-up Description: Agility will be assessed with the T-Test. Four cones should be placed in a T-shape: A at the starting point; B at 9.14 m forward; and C and D at the sides of this at 4.57 m the other two cones. The athlete must go as fast as possible to cone B and touch it with the tip with her right hand, then she must go to the sides touching cones C and D with the hand of the same side, return to touch cone B with the left hand and lastly, move backwards and go over cone A. The unit of measurement is the second, where lower times indicate efficient agility. Measure: Assess the changes in agility Time Frame: Screening visit, within the first seven days after treatment and after six weeks follow-up ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Female players over 18 years of age. * That during the study period they play basketball competing in the 1st Women's Division 1 category of the Basketball Federation of the Region of Murcia. * That they perform strength exercises at least once a week. * That they sign the informed consent document. Exclusion Criteria: * Players with knee or ankle injuries in the 6 months prior to the study. * Players who use ankle or knee braces regularly. * Players with lower limb surgery in the last year. * Players whose participation is contraindicated by the team doctor, physiotherapist or physical trainer. Healthy Volunteers: True Maximum Age: 30 Years Minimum Age: 18 Years Sex: FEMALE Standard Ages: - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Rubén Cuesta-Barriuso, PhD Phone: 607547274 Role: CONTACT #### Locations Location 1: City: Murcia Country: Spain Facility: Universidad Católica San Antonio, Murcia Zip: 30107 ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423144 Brief Title: PD-1/PD-L1 Inhibitors and Anti-angiogenic Therapy Combined With/Without TACE/HAIC in Patients With BCLC B/C Hepatocellular Carcinoma Beyond Up-to-7 Official Title: A Retrospective Study Comparing Interventional Therapy (TACE/HAIC) Combined With PD-1/PD-L1 Inhibitors and Anti-angiogenic Agents Versus PD-1/PD-L1 Inhibitors and Anti-angiogenic Agents Alone in the First-line Treatment of Intermediate and Advanced Hepatocellular Carcinoma Beyond up to Seven #### Organization Study ID Info ID: ZL-2024-06 #### Organization Class: OTHER Full Name: Shanghai Zhongshan Hospital ### Status Module #### Completion Date Date: 2024-10 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-08 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Shanghai Zhongshan Hospital #### Responsible Party Investigator Affiliation: Shanghai Zhongshan Hospital Investigator Full Name: Lan Zhang Investigator Title: Chief physician Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: This is a retrospective study that retrospectively included patients with intermediate and advanced HCC beyond up to seven who received first-line treatment with PD-1/PD-L1 inhibitors and anti-angiogenic agents combined with/without TACE/HAIC from January 01, 2019 to December 31, 2023 in the Department of Hepatic Oncology and Department of Liver Cancer Surgery, Zhongshan Hospital, Fudan University. ### Conditions Module Conditions: - Hepatocellular Carcinoma ### Design Module #### Design Info Observational Model: COHORT Time Perspective: RETROSPECTIVE #### Enrollment Info Count: 150 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Logical therapy combined with systemic therapy Intervention Names: - Procedure: TACE/HAIC - Drug: PD-1/PD-L1 inhibits and anti-angiogenic agents Label: Group LS #### Arm Group 2 Description: Systemic therapy alone（PD-1/PD-L1 inhibits and anti-angiogenic agents） Intervention Names: - Drug: PD-1/PD-L1 inhibits and anti-angiogenic agents Label: Group S ### Interventions #### Intervention 1 Arm Group Labels: - Group LS Description: TACE/HAIC were performed within 1 month prior/after the first PD-1/PD-L 1 inhibitor/antiangiogenic drug treatment; Name: TACE/HAIC Type: PROCEDURE #### Intervention 2 Arm Group Labels: - Group LS - Group S Description: Agents were administrated based on the instructions recommended Name: PD-1/PD-L1 inhibits and anti-angiogenic agents Type: DRUG ### Outcomes Module #### Primary Outcomes Description: The time from the beginning of treatment to the time of tumor progression or death from any cause (according to mRECIST and RECIST v1.1) Measure: PFS Time Frame: Up to 48 months Description: The percentage of patients who have best overall response of complete response (CR) or partial response (PR) according to mRECIST and RECIST v1.1 Measure: ORR Time Frame: Up to 48 months #### Secondary Outcomes Description: OS was defined as the interval from the date of the initial administration of any drug/procedure to death from any cause. Measure: OS Time Frame: Up to 48 months Description: Safety was defined the incidence and severity of adverse events (AEs) and serious adverse events (SAEs). The severity of AEs were evaluated based on the National Cancer Institute Common Terminology Criteria for Adverse Events version (NCI-CTCAE) v5.0. Measure: Safety Time Frame: Up to 48 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Patients who have been diagnosed with advanced hepatocarcinoma (HCC), confirmed histologically or clinically. * Patients with Barcelona (BCLC) stage B and C beyond up to seven; * Have not received any prior systemic therapy for HCC (including: chemotherapy, molecular targeted therapy, immunotherapy); * Receiving only post-marketing PD-1/PD-L1 inhibitors in combination with anti-angiogenic agents (including, but not limited to, drugs containing hepatocellular carcinoma indications); \The interval between the first use of PD-1/PD-L 1 inhibitors and the use of anti-angiogenic drugs is ≤ 1 week TACE was performed within 1 month prior/after the first PD-1/PD-L 1 inhibitor/antiangiogenic drug treatment; * TACE treatment followed by at least 1 cycle of combination therapy, including: cTACE and DEB-TACE; * There is at least 1 measurable lesion in the liver according to RECIST v1.1 criteria Exclusion Criteria: * Cholangiocellular carcinoma, mixed hepatocellular carcinoma, sarcomatoid hepatocellular carcinoma, or hepatic fibrous laminar carcinoma that has been pathologically/histologically confirmed; * Patients who do not meet the above definition of combination therapy; * Patients had malignant tumors other than HCC within 5 years prior to enrollment (except cured limited tumors, including cervical carcinoma in situ, basal cell carcinoma of the skin, and prostate carcinoma in situ) Maximum Age: 100 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Patients with intermediate and advanced hepatocellular carcinoma beyond up to seven ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Lan Zhang, MD, Ph.D Phone: 13918876432 Role: CONTACT ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009375 - Term: Neoplasms, Glandular and Epithelial - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000000230 - Term: Adenocarcinoma - ID: D000008113 - Term: Liver Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000004066 - Term: Digestive System Diseases - ID: D000008107 - Term: Liver Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: All - Name: All Conditions - Abbrev: BC06 - Name: Digestive System Diseases ### Condition Browse Module - Browse Leaves - ID: M5534 - Name: Carcinoma - Relevance: HIGH - As Found: Carcinoma - ID: M9613 - Name: Carcinoma, Hepatocellular - Relevance: HIGH - As Found: Hepatocellular Carcinoma - ID: M12320 - Name: Neoplasms, Glandular and Epithelial - Relevance: LOW - As Found: Unknown - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M3585 - Name: Adenocarcinoma - Relevance: LOW - As Found: Unknown - ID: M11113 - Name: Liver Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M11107 - Name: Liver Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000002277 - Term: Carcinoma - ID: D000006528 - Term: Carcinoma, Hepatocellular ### Intervention Browse Module - Ancestors - ID: D000043924 - Term: Angiogenesis Modulating Agents - ID: D000006133 - Term: Growth Substances - ID: D000045505 - Term: Physiological Effects of Drugs - ID: D000006131 - Term: Growth Inhibitors - ID: D000000970 - Term: Antineoplastic Agents ### Intervention Browse Module - Browse Branches - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M22318 - Name: Angiogenesis Inhibitors - Relevance: HIGH - As Found: TPMT - ID: M5982 - Name: Chlorotrianisene - Relevance: LOW - As Found: Unknown - ID: M9231 - Name: Growth Inhibitors - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000020533 - Term: Angiogenesis Inhibitors ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423131 Brief Title: Prospective Clinical Trial for Children With TCRαβ Depleted vs Traditional Haplo Identicle HSCT Official Title: TCRαβ+ Cell Deleted Versus Traditional Haploidentical Hematopoietic Stem Cell Transplantation ：A Single-center, Prospective, Non-randomized Controlled Clinical Study #### Organization Study ID Info ID: SCMCIRB-K2024030-2 #### Organization Class: OTHER Full Name: Shanghai Jiao Tong University School of Medicine ### Status Module #### Completion Date Date: 2028-03-31 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-29 Type: ACTUAL Last Update Submit Date: 2024-05-26 Overall Status: RECRUITING #### Primary Completion Date Date: 2027-03-31 Type: ESTIMATED #### Start Date Date: 2024-05-26 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Sijia Gu #### Responsible Party Investigator Affiliation: Shanghai Jiao Tong University School of Medicine Investigator Full Name: Sijia Gu Investigator Title: Principal investigator Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: This is a single-center prospective, non-randomized controlled clinical study in China using CliniMACS TCRα/β+ cell depleted stem cell haploidentical donors versus conventional Beijing protocol for haploidentical hematopoietic stem cell transplantation in children. Detailed Description: 1:1 non-randomized controlled clinical study in single center using CliniMACS TCRα/β+ cell depleted stem cell versus conventional Beijing protocol for haploidentical hematopoietic stem cell transplant. The purpose of this study is to obtain 30% decrease grade II-IV aGVHD and better qulity of life for TCRα/β+ cell depleted haploidentical stem cell transplantaion. ### Conditions Module Conditions: - Graft-Versus-Host Disease - Hematopoietic Stem Cell Transplantation - Child, Only - Haploidentical Hematopoietic Stem Cell Transplantation ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: TCRαβ depleted HSCT compare to traditional Beijing haploidentical HSCT ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 110 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Beijing haploidenticla HCT is the routinely traditional way used for haploidentical HCT Label: Traditional Haplo identicle HCT Type: NO_INTERVENTION #### Arm Group 2 Description: TCRαβ Depleted haploidentical HCT is experimental used to decrease GVHD and obtain better qulity of life for children with haploidentical HCT. Intervention Names: - Procedure: TCRαβ Depleted haploidentical HCT Label: TCRαβ Depleted haploidentical HCT Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - TCRαβ Depleted haploidentical HCT Description: Use the CliniMACS TCRα/β deplete from the mobilized peripheral blood stem cells of haploidentical donor in children Name: TCRαβ Depleted haploidentical HCT Type: PROCEDURE ### Outcomes Module #### Primary Outcomes Description: Incidence of grade II-IV acute graft-versus-host disease (GVHD) until Day 100 post-transplantation. Measure: Incidence of grade II-IV acute GVHD Time Frame: day+100 Description: compare the incidence of TRM until Day 100 post-transplantation Measure: incidence of treatment related mortality(TRM) Time Frame: day +100 #### Secondary Outcomes Description: compare the incidence of GRFS and OS post HSCT 1y and 2y Measure: post HSCT day 1y and 2y GRFS and OS Time Frame: day +1y and +2y Description: compare the incidence of cGVHD post HSCT 1y and 2y Measure: cGVHD post day 1y and 2y Time Frame: day +1y and +2y Description: compre the incidence of TRM post HSCT day 1y and 2y Measure: TRM post day +1y and +2y Time Frame: day +1y and +2y ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Age 8 weeks to 18 years * Children who meet the indicators haploidentical hematopoietic cell transplantation * No HLA ≥ 9/10 donor or not suitable for this type of donor due to illness * Informed consent must be signed (by the patient or legal representative) Exclusion Criteria: * Liver function abnormalities with bilirubin \>2 mg/dL and elevation of transaminases higher than 400 U/L * Chronic active viral hepatitis * Ejection fraction \<50% * Respiratory failure necessitating supplemental oxygen * Patients with a history of psychiatric illness or a condition which could interfere with their ability to understand the requirements of the study * Patients unwilling or unable to comply with the protocol or unable to give informed consent * Concurrent severe or uncontrolled infection Maximum Age: 18 Years Minimum Age: 8 Weeks Sex: ALL Standard Ages: - CHILD - ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Jing Chen, PhD Phone: 38626161 Phone Ext: 82073 Role: CONTACT #### Locations Location 1: City: Shanghai Contacts: *Contact 1:* - Email: [email protected] - Name: J Chen, PhD - Phone: 38626161 - Phone Ext: 82073 - Role: CONTACT Country: China Facility: Shanghai Children's Medical Center, School of Medicine, Shanghai Jiao Tong University State: Shanghai Status: RECRUITING #### Overall Officials Official 1: Affiliation: Shanghai Children's Medical Center Name: Jing Chen, PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000007154 - Term: Immune System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC20 - Name: Immune System Diseases - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M9189 - Name: Graft vs Host Disease - Relevance: HIGH - As Found: Graft Versus Host Disease - ID: M10200 - Name: Immune System Diseases - Relevance: LOW - As Found: Unknown - ID: T2832 - Name: Homologous Wasting Disease - Relevance: HIGH - As Found: Graft Versus Host Disease ### Condition Browse Module - Meshes - ID: D000006086 - Term: Graft vs Host Disease ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423118 Brief Title: Sleep Apnea and Cognition in Older Adults Official Title: Cross-sectional Investigation of Sleep Apnea and Cognition in Older Adults Using the ANNE Vital Sign System #### Organization Study ID Info ID: 5140 #### Organization Class: OTHER Full Name: Sunnybrook Health Sciences Centre ### Status Module #### Completion Date Date: 2034-04 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2034-04 Type: ESTIMATED #### Start Date Date: 2024-04-09 Type: ACTUAL Status Verified Date: 2024-04 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Alzheimer Society of Canada #### Lead Sponsor Class: OTHER Name: Sunnybrook Health Sciences Centre #### Responsible Party Investigator Affiliation: Sunnybrook Health Sciences Centre Investigator Full Name: Dr. Jennifer Rabin Investigator Title: Scientist Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: True Is FDA Regulated Drug: False Is US Export: True Oversight Has DMC: False ### Description Module Brief Summary: The goal of this cross-sectional, observational, medical device trial is to examine the association of several sleep parameters, including specific respiratory events and an apnea-hypopnea index, with cognitive performance in older adults. The main question the study aims to answer is: Is there an association between sleep parameters with cognitive performance? Researchers will collect sleep parameters from participants using a device called the ANNE Vital Sign System and will test whether they are associated with performance on different memory and thinking tasks. Participants will: Complete a battery of cognitive tests to assess their memory and thinking performance. Wear the ANNE Vital Sign System continuously for a period of 24 hours. Detailed Description: Nearly a third of older adults experience difficulty initiating or maintaining sleep and nearly half have sleep apnea. However, current reliance on gold-standard in-lab polysomnography has been a barrier to detecting, quantifying, and measuring these sleep problems. Polysomnography is difficult for many older adults to tolerate, requires specialized technologists to obtain and analyze the recordings, is labour intensive and expensive, and not widely available in many jurisdictions, all of which impede use by primary care clinicians or end-users. Recent advances in wearable sensor development have led to a new generation of wearable sensors that have good potential to overcome these barriers. Accumulating evidence suggests that poor sleep quality increases the risk of cognitive impairment and dementia, however studies in older adults linking objectively measured sleep function with comprehensive cognitive testing are lacking. The primary objective of this cross-sectional study is to examine the association of several objectively measured sleep parameters (e.g., sleep apnea) with cognitive performance. The Advanced NeoNatal Epidermal (ANNE) Vital Sign System was created for the purposes of providing real-time vital signs monitoring in the paediatric intensive care unit. The ANNE Vital Sign System integrates simultaneous synchronized ambulatory measurement of electrocardiography, photoplethysmography with derived pulse oximetry, pulse arrival time with derived beat-to-beat blood pressure, triaxial accelerometry, respiratory rate, and temperature, to enable accurate measurement of sleep apnea. The characteristics that make the ANNE Vital Sign System ideal for use in children (non-invasive, flexible, ease of use, comfort, skin safety) also make it ideal for use in adults. Compelling in-laboratory preliminary data from our collaborator at Sunnybrook Research Institute (SRI) has demonstrated the capacity for ANNE to detect and characterize sleep apnea in older adults. After the informed consent process, participants will complete a 1-hour battery of cognitive tests. If participants have completed the same set of cognitive tests in the past year at SRI no cognitive testing will take place. Following testing, participants will be shown how to affix and remove the sensors to their chest and dominant index finger (or non-dominant if dominant is not available) according to manufacturer recommendations. Participants will be given the device to take home and asked to wear the sensors for a 24-hour period. They will also be provided with ANNE chest adhesive, ANNE limb adhesive, and a clinical waterproof 3M Tegaderm dressing. Participation in the study concludes after the device is worn for the 24-hour period. Though there are no substantial benefits for participants, this study may lead to a better understanding of the association between sleep apnea and cognition in older adults. Given that poor sleep quality is a risk factor for dementia, there is a need to better characterize the relationship between objective sleep parameters and cognition. ### Conditions Module Conditions: - Sleep - Cognition - Aging Keywords: - sleep - cognition - aging ### Design Module #### Design Info Observational Model: COHORT Time Perspective: CROSS_SECTIONAL #### Enrollment Info Count: 300 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: * Age 55-85 * 8+ years of education * No frank cognitive impairment or dementia Intervention Names: - Device: ANNE Vital Sign System Label: Healthy Older Adults ### Interventions #### Intervention 1 Arm Group Labels: - Healthy Older Adults Description: The ANNE Vital Sign System is a pair of non-invasive, flexible sensors originally designed for vital signs monitoring in the paediatric intensive care unit. Name: ANNE Vital Sign System Other Names: - ANNE One Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: An apnea-hypopnea index, the combined average number of apneas and hypopneas that occur per hour of sleep, will be calculated from ANNE Vital Sign System data. Study staff will annotate apneas and hypopneas to calculate the index using an EEG annotation tool. A linear regression model will be constructed to examine the association between apnea-hypopnea index and performance on a battery of neuropsychological tests, which includes: 1. Montreal Cognitive Assessment 2. Free and Cued Selective Reminding Test 3. Benson Complex Figure Copy 4. Doors Test, Parts A and B 5. WAIS-III Symbol Digit Coding 6. Benson Complex Figure Delay 7. Benson Complex Figure Recognition 8. 7-24 Spatial Recall Test 9. Colour Trails Test, parts 1 and 2 10. Controlled Oral Word Association Test (FAS) 11. Semantic Fluency (Animals) 12. Trail Making Test, parts A and B Measure: Association between apnea-hypopnea index and cognitive performance Time Frame: 24 hours ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Sufficient knowledge of English to understand and provide informed consent 2. Competent to provide consent 3. Aged 55-85, Male and Female 4. ≥ 8 years of education 5. Capable of cooperating for the duration of the study procedures and assessments 6. No frank cognitive impairment or dementia 7. Sufficient (corrected) vision to participate in cognitive testing 8. Sufficient (corrected) hearing to participate in cognitive testing Exclusion Criteria: 1. Cannot read and comprehend English language instructions 2. Major cardio- or cerebro-vascular event (heart attack, stroke, significant white matter changes) 3. Unstable diseases (e.g., pulmonary, endocrine disorder) 4. Active malignancy or infectious diseases 5. History of significant learning disability 6. Major psychiatric/neurologic/degenerative disorder, including a diagnosis of mild cognitive impairment or dementia 7. History of significant head trauma or recurrent concussions requiring hospitalization followed by persistent neurologic defaults or known structural brain abnormalities 8. Pain or sleep disorder that could interfere with cognitive testing 9. Major medical concerns that might interfere with cognitive testing 10. Recent history of substance/drug abuse 11. Known nickel allergy 12. Known cardiac implantable device 13. Known arrhythmias 14. Outside the included age range 15. Pregnant or breast feeding 16. Otherwise unable to use the ANNE sensors; for example, finger amputations. Healthy Volunteers: True Maximum Age: 85 Years Minimum Age: 55 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Healthy older adults between the ages of 55-85, with 8+ years of education and no frank cognitive impairment or dementia. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Alexander Nyman, BSc Phone: 416-480-6100 Role: CONTACT #### Locations Location 1: City: Toronto Contacts: *Contact 1:* - Email: [email protected] - Name: Silina Boshmaf, BSc - Phone: 416-480-6100 - Role: CONTACT *Contact 2:* - Name: Jennifer Rabin, PhD - Role: PRINCIPAL_INVESTIGATOR Country: Canada Facility: Sunnybrook Health Sciences Centre State: Ontario Status: RECRUITING Zip: M6G3T6 #### Overall Officials Official 1: Affiliation: Sunnybrook Research Institute Name: Jennifer Rabin, PhD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ### References Module #### References Citation: Foley DJ, Monjan AA, Brown SL, Simonsick EM, Wallace RB, Blazer DG. Sleep complaints among elderly persons: an epidemiologic study of three communities. Sleep. 1995 Jul;18(6):425-32. doi: 10.1093/sleep/18.6.425. PMID: 7481413 Citation: Senaratna CV, Perret JL, Lodge CJ, Lowe AJ, Campbell BE, Matheson MC, Hamilton GS, Dharmage SC. Prevalence of obstructive sleep apnea in the general population: A systematic review. Sleep Med Rev. 2017 Aug;34:70-81. doi: 10.1016/j.smrv.2016.07.002. Epub 2016 Jul 18. PMID: 27568340 Citation: Oosterman JM, van Someren EJ, Vogels RL, Van Harten B, Scherder EJ. Fragmentation of the rest-activity rhythm correlates with age-related cognitive deficits. J Sleep Res. 2009 Mar;18(1):129-35. doi: 10.1111/j.1365-2869.2008.00704.x. PMID: 19250179 Citation: Shi L, Chen SJ, Ma MY, Bao YP, Han Y, Wang YM, Shi J, Vitiello MV, Lu L. Sleep disturbances increase the risk of dementia: A systematic review and meta-analysis. Sleep Med Rev. 2018 Aug;40:4-16. doi: 10.1016/j.smrv.2017.06.010. Epub 2017 Jul 6. PMID: 28890168 Citation: Sindi S, Kareholt I, Johansson L, Skoog J, Sjoberg L, Wang HX, Johansson B, Fratiglioni L, Soininen H, Solomon A, Skoog I, Kivipelto M. Sleep disturbances and dementia risk: A multicenter study. Alzheimers Dement. 2018 Oct;14(10):1235-1242. doi: 10.1016/j.jalz.2018.05.012. Epub 2018 Jul 17. PMID: 30030112 Citation: Zhu X, Zhao Y. Sleep-disordered breathing and the risk of cognitive decline: a meta-analysis of 19,940 participants. Sleep Breath. 2018 Mar;22(1):165-173. doi: 10.1007/s11325-017-1562-x. Epub 2017 Sep 13. PMID: 28905231 Citation: Chung HU, Kim BH, Lee JY, Lee J, Xie Z, Ibler EM, Lee K, Banks A, Jeong JY, Kim J, Ogle C, Grande D, Yu Y, Jang H, Assem P, Ryu D, Kwak JW, Namkoong M, Park JB, Lee Y, Kim DH, Ryu A, Jeong J, You K, Ji B, Liu Z, Huo Q, Feng X, Deng Y, Xu Y, Jang KI, Kim J, Zhang Y, Ghaffari R, Rand CM, Schau M, Hamvas A, Weese-Mayer DE, Huang Y, Lee SM, Lee CH, Shanbhag NR, Paller AS, Xu S, Rogers JA. Binodal, wireless epidermal electronic systems with in-sensor analytics for neonatal intensive care. Science. 2019 Mar 1;363(6430):eaau0780. doi: 10.1126/science.aau0780. PMID: 30819934 ## Document Section ### Large Document Module #### Large Docs - Date: 2023-03-17 - Filename: ICF_000.pdf - Has ICF: True - Has Protocol: False - Has SAP: False - Label: Informed Consent Form - Size: 483122 - Type Abbrev: ICF - Upload Date: 2024-04-24T15:01 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001049 - Term: Apnea - ID: D000012120 - Term: Respiration Disorders - ID: D000012140 - Term: Respiratory Tract Diseases - ID: D000020919 - Term: Sleep Disorders, Intrinsic - ID: D000020920 - Term: Dyssomnias - ID: D000012893 - Term: Sleep Wake Disorders - ID: D000009422 - Term: Nervous System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M4361 - Name: Apnea - Relevance: LOW - As Found: Unknown - ID: M15694 - Name: Sleep Apnea Syndromes - Relevance: HIGH - As Found: Sleep Apnea - ID: M16355 - Name: Syndrome - Relevance: LOW - As Found: Unknown - ID: M14957 - Name: Respiration Disorders - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: M22242 - Name: Parasomnias - Relevance: LOW - As Found: Unknown - ID: M22654 - Name: Sleep Disorders, Intrinsic - Relevance: LOW - As Found: Unknown - ID: M22655 - Name: Dyssomnias - Relevance: LOW - As Found: Unknown - ID: M15696 - Name: Sleep Wake Disorders - Relevance: LOW - As Found: Unknown - ID: T4202 - Name: Oculocerebral Syndrome With Hypopigmentation - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000012891 - Term: Sleep Apnea Syndromes ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423105 Brief Title: Influencing Factors and Prediction Model of False-negative Central Lymph Nodes in Thyroid Cancer Patients Official Title: Influencing Factors and Prediction Model of False-negative Central Lymph Nodes in Thyroid Cancer Patients: a Cohort Study #### Organization Study ID Info ID: NO.SWYX2024-225 #### Organization Class: OTHER_GOV Full Name: Shandong Provincial Hospital ### Status Module #### Completion Date Date: 2024-04-01 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-23 Type: ACTUAL Last Update Submit Date: 2024-05-21 Overall Status: COMPLETED #### Primary Completion Date Date: 2023-12-31 Type: ACTUAL #### Start Date Date: 2013-01-01 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Shandong University #### Lead Sponsor Class: OTHER_GOV Name: Ningning Ren #### Responsible Party Investigator Affiliation: Shandong Provincial Hospital Investigator Full Name: Ningning Ren Investigator Title: Principal Investigator Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The problem of false-negative lymph nodes in the central region (CLN) refers to the inability to detect lymph nodes (LN) metastasis during preoperative ultrasound examination but is confirmed by surgical and postoperative pathological examination. According to this study, the false-negative rate of CLN of patients with TC was relatively high at approximately 71.7%. The high proportion of false-negatives indicates limitations in the sensitivity of ultrasound examination, especially for detecting small LN or small metastases. The presence of false-negative CLN directly affects clinical practice. First, it may lead to insufficient selection of treatment strategies for patients with TC, thereby affecting their prognosis. Second, such false-negative results may lead surgeons to overly trust ultrasound examination during preoperative evaluation, neglecting the importance of comprehensive clinical information, and thus affecting the formulation of treatment plans. This study aimed to explore the factors influencing false-negative CLN through a cohort study and to establish a predictive model. Detailed Description: Setting and Population This study collected 6369 patients admitted to the Breast and Thyroid Surgery Department of Shandong Provincial Hospital between January 2013 and December 2023, who were diagnosed with TC through postoperative pathology. (SDC, Figure 1) All patients included in the study signed a written informed consent form before surgery. Ethical approval for this study (NO.SWYX2024-225) was provided by the Ethical Committee of Shandong Provincial Hospital, Jinan, China on 15 April 2024. According to the relevant literature, the criteria for identifying abnormal cervical LN under ultrasound are: disappearance of the LN hilum structure or abnormalities in the skin and medulla, LN becoming round or having an increased aspect ratio, microcalcifications in the LN, cystic changes present in LN, and abnormal blood flow signals in LN.17 The inclusion and exclusion criteria are: all cases are newly diagnosed TC cases; all cases underwent preoperative thyroid and neck LN examinations by the Ultrasound Department of Shandong Provincial Hospital; all cases underwent thyroid surgery for the first time; all cases were diagnosed with TC through postoperative pathological examination; excluding cases of other combined tumors or major diseases. This study used the postoperative paraffin pathology results as the gold standard for diagnostic testing. All ultrasound examinations were performed by two ultrasound physicians. When two ultrasound physicians had different opinions, a third senior ultrasound physician was requested to assist in the evaluation. Data Collection After obtaining written consent, we recorded the patient\'s relevant information in detail and followed up on the patient\'s postoperative paraffin pathology results. The collected and organized items included: 1) sex, age, and past medical history; 2) preoperative ultrasound information; 3) preoperative fine-needle biopsy information; 4) surgical information; 5) postoperative pathological information; and 6) immunohistochemical information. Statistical Analysis This study first analyzed the baseline data of the included patients and obtained descriptive data on the current status of patients with TC. (Table 1) This study also analyzed the efficacy of ultrasound and fine-needle aspiration (FNA) for the evaluation of cervical LN. (Table 2) Subsequently, analysis was conducted on 52 factors that may cause false-negative CLN of TC. (Table 3) A total of 16 statistically significant influencing factors were identified. (Table 4) To construct a predictive model for the occurrence of false-negative CLN of the thyroid gland, we selected five preoperative influencing factors with predictive significance from eight preoperative influencing factors and drew a forest chart for data visualization and outcome prediction. This study was analyzed using IBM SPSS 29.0 software. Quantitative data are represented by mean ± standard deviation when it follows a normal distribution and homogeneity of variance, and an independent sample t-test is used for comparison between the two groups; the median (P25, P75) is used to represent non-normal distributions, and a non-parametric Mann-Whitney test is used for comparison between the two groups. Qualitative data were expressed as percentages (%), and intergroup comparisons were conducted using the chi-square or Fisher\'s exact test. Variables with statistical significance in the univariate analysis and those professionally considered to have an impact on the outcome were included in the logistic regression model to explore the independent factors influencing the outcome. The test level P was set at 0.05. A forest map was drawn using Graphpad Prism 10.12 software, and a column chart and credibility analysis were drawn using R Studio 4.3 software. ### Conditions Module Conditions: - Thyroid Cancer Keywords: - thyroid cancer - central lymph nodes - false negative ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 6369 Type: ACTUAL Patient Registry: True Study Type: OBSERVATIONAL Target Duration: 5 Years ### Arms Interventions Module #### Arm Group 1 Description: This article defines cases that preoperative ultrasound indicates no suspicious malignant enlargement of central lymph nodes and postoperative paraffin pathology indicates the presence of metastatic cancer in central lymph nodes as false-negative cases. Label: false negative ### Outcomes Module #### Primary Outcomes Description: This article defines cases that preoperative ultrasound indicates no suspicious malignant enlargement of central lymph nodes and postoperative paraffin pathology indicates the presence of metastatic cancer in central lymph nodes as false-negative cases. Measure: Pathological results Time Frame: From enrollment to the end of treatment at 5 years ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. All cases are new cases of thyroid cancer. 2. All clinical data and research materials of the cases are complete. 3. All cases underwent preoperative thyroid and neck lymph node examinations by the Ultrasound Department of Shandong Provincial Hospital. 4. All cases showed no swelling in the central lymph node status on preoperative ultrasound. 5. All cases underwent initial surgical treatment. 6. All cases were diagnosed with thyroid cancer through postoperative pathological examination. Exclusion Criteria: 1. Except for cases of recurrence. 2. Cases with incomplete clinical data and research materials are excluded. 3. Cases that have not undergone thyroid and neck lymph node examination by the ultrasound department of Shandong Provincial Hospital before surgery are excluded. 4. Cases with enlarged lymph nodes in the central thyroid region indicated by preoperative ultrasound are excluded. 5. Excluding cases of secondary surgery. 6. Cases with postoperative pathological diagnosis of benign thyroid tumors are excluded. Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT Study Population: This study collected 6369 patients admitted to the Breast and Thyroid Surgery Department of Shandong Provincial Hospital between January 2013 and December 2023, who were diagnosed with TC through postoperative pathology. ### IPD Sharing Statement Module Description: for privacy IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000004700 - Term: Endocrine System Diseases - ID: D000004701 - Term: Endocrine Gland Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000006258 - Term: Head and Neck Neoplasms ### Condition Browse Module - Browse Branches - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC04 - Name: Neoplasms ### Condition Browse Module - Browse Leaves - ID: M16718 - Name: Thyroid Diseases - Relevance: HIGH - As Found: Thyroid - ID: M16723 - Name: Thyroid Neoplasms - Relevance: HIGH - As Found: Thyroid Cancer - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown - ID: M7863 - Name: Endocrine Gland Neoplasms - Relevance: LOW - As Found: Unknown - ID: M9348 - Name: Head and Neck Neoplasms - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000013964 - Term: Thyroid Neoplasms - ID: D000013959 - Term: Thyroid Diseases ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423092 Brief Title: Music Therapy Songwriting and Mental Health in Neonatel Intensive Care Unit (NICU) Parents Official Title: Short-term Effectiveness of Music Therapy Songwriting on Mental Health Outcomes of At-risk Parents in the Neonatal Intensive Care Unit: an International Multicenter Mixed-methods Study. #### Organization Study ID Info ID: 166-23 UNV #### Organization Class: OTHER Full Name: Sanitas University ### Status Module #### Completion Date Date: 2026-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-01 Type: ESTIMATED #### Start Date Date: 2024-06 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: Sanitas University #### Lead Sponsor Class: OTHER Name: Claudia Aristizábal #### Responsible Party Investigator Affiliation: Sanitas University Investigator Full Name: Claudia Aristizábal Investigator Title: Director Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: The mental health of parents of preterm newborns (PTNB) is negatively affected by prolonged hospitalization of the PTNB in the intensive care unit. This produces changes in the role of the parents and the bond with the newborn, leading to states of depression, anxiety, and stress. Several strategies, including music therapy, have been implemented to mitigate the negative impact on the parents' mental health. The main objectives of the proposed trial are to determine whether Music Therapy (MT) songwriting combined with standard care (SC) during NICU stay is superior to SC alone in reducing the risk of postpartum depression in at-risk parents of preterm children at the end of treatment, and understand the lived experiences of participating parents who received music therapy for their mental health. Detailed Description: This study employs a multicenter, mixed-method approach, with a quantitative component that will be a pragmatic parallel controlled randomized clinical trial (RCT) and a qualitative component that will include phenomenological study. The quantitative component will assess depression and anxiety, which will be evaluated with the Edinburgh Postnatal Depression Scale (EPDS) and the Generalized Anxiety Disorder Scale (GAD-7), respectively. Secondary outcomes will be resilience, coping, stress, and mental well-being. These outcomes will be measured in the first week of hospitalization (baseline measure) and then in weeks 1, 2, and 3 of the intervention. Changes in scores will be assessed to identify the effect, and mediating variables will be determined by multivariate analysis. Semi-structured interviews will be conducted on the parents' experience of music therapy songwriting for the baby. The study will provide data on the effect of music therapy songwriting on the mental health of parents of neonates with brain injuries (PTNB) versus standard care and will document the lived experience of music therapy songs. The results may inform the standardization of this strategy in neonatal intensive care units (NICUs) to support and accompany parents and decrease the impact on their mental health. ### Conditions Module Conditions: - Mental Health Impairment ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Who Masked: - OUTCOMES_ASSESSOR Primary Purpose: OTHER #### Enrollment Info Count: 102 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: The music therapy songwriting is a method frequently employed in music therapy sessions. This method involves the collaborative creation of lyrics and/or music with the participants. The intervention will consist of nine sessions, each of which will last approximately 30 to 45 minutes. Three sessions will be conducted per week until a minimum of six and a maximum of nine sessions are achieved. Intervention Names: - Other: Music therapy songwriting Label: Music therapy songwriting + standard care Type: EXPERIMENTAL #### Arm Group 2 Description: Standard care is the usual care provided to parents of newborns hospitalized in a neonatal intensive care unit (NICU). This care includes providing information about the baby's health status and recommendations during contact with the baby. Additionally, when a health professional identifies symptoms of mental health disturbance in the parents, they are referred to a mental health professional for appropriate management. Label: Standard care Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Music therapy songwriting + standard care Description: Session 1: The goal of the first music therapy session is to know the parents musically and to provide information about song creation. This is achieved by exploring their favorite songs. Options for creating a song (original song or song parody) are presented and possibilities for creating lyrics are discussed. Sessions 2-7: The structure of the song will be created and discussed with the parents. Parents will also be invited to include written messages from other family members in the lyrics if they wish. In each session, the developing welcome song is sung together with the parents, accompanied by the music therapist, who provides vocal or instrumental support. The final sessions (Sessions 8-9) are dedicated to singing the final version of the song with the parents and their infant. Should the parents desire, a final recording of the song will also be made and the digital songbook will be created. Name: Music therapy songwriting Type: OTHER ### Outcomes Module #### Primary Outcomes Description: Postpartum depression will be assessed with the Edinburgh Postnatal Depression Scale (EPDS). Measure: Postpartum depression Time Frame: It will be measured during the first week of hospitalization (baseline measurement) and at weeks 1, 2, and 3 of the intervention. #### Secondary Outcomes Description: Anxiety will be assessed with the Generalized Anxiety Disorder Scale (GAD-7). Measure: Anxiety Time Frame: It will be measured during the first week of hospitalization (baseline measurement) and at weeks 2 and 3 of the intervention. Description: The Warwick Edinburgh Mental Well-Being Scale (WEMWBS) will be employed to assess well-being. Measure: Well-being Time Frame: It will be measured during the first week of hospitalization (baseline measurement) and at weeks 2 and 3 of the intervention. Description: Resilience will be assessed with the Brief Resilience Scale (BRS). Measure: Resilience Time Frame: It will be measured during the first week of hospitalization (baseline measurement) and at week 3 of the intervention. Description: Stress will be assessed with the 10-item Perceived Stress Scale (PSS-10). Measure: Stress Time Frame: It will be measured during the first week of hospitalization (baseline measurement) and at week 3 of the intervention. Description: Stress response will be assessed with the Brief COPE Inventory (Brief-COPE). Measure: Coping Time Frame: It will be measured during the first week of hospitalization (baseline measurement) and at week 3 of the intervention. ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * The study population consisted of parents/caregivers of newborns hospitalized in neonatal intensive care units (NICUs) with gestational ages of ≤32 weeks and expected hospitalizations of at least three weeks. In the case of a twin pregnancy, the firstborn infant was randomly assigned to one of the intervention groups, while both infants received the same treatment according to the outcome of randomization. * Mother a total score of ≥10 and/or father a total score of ≥7 on the EPDS (Edinburgh Postnatal Depression Scale) * Mother and/or father a total score of ≥8 on the GAD-7 (Generalized Anxiety Disorder Scale) Exclusion Criteria: * Parents/caregivers with known auditory problems that prevent participation in MT. Moreover parents/caregivers with a documented mental illness or cognitive impairment that prevents them from being able to complete the study intervention or outcome assessments. * Parents/caregivers of premature infants in palliative or end-of-life care, infants with known hearing impairment, or infants in the custody of social services. Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Mark Ettenberger, PhD Phone: +57 311 284 7635 Role: CONTACT #### Locations Location 1: City: Barranquilla Contacts: *Contact 1:* - Email: [email protected] - Name: Mark Ettenberger, PhD - Phone: +57 605 3319424 - Role: CONTACT Country: Colombia Facility: Clínica Iberoamérica en Colombia State: Atlántico Location 2: City: Bogotá Contacts: *Contact 1:* - Email: [email protected] - Name: Mark Ettenberger, PhD - Phone: (+57) 601 745 5100 - Role: CONTACT Country: Colombia Facility: Clinica Pediátrica State: Cundinamarca Location 3: City: Bogotá Contacts: *Contact 1:* - Email: [email protected] - Name: Mark Ettenberger - Phone: (+57) 6015948650 - Role: CONTACT *Contact 2:* - Name: Marcela Beltrán, MSc - Role: SUB_INVESTIGATOR *Contact 3:* - Name: Mark Ettenberger, PhD - Role: PRINCIPAL_INVESTIGATOR *Contact 4:* - Name: Angélica Hernández, MSc - Role: SUB_INVESTIGATOR *Contact 5:* - Name: Ana María Diaz, MSc - Role: SUB_INVESTIGATOR *Contact 6:* - Name: Johana Benavides, MSc - Role: SUB_INVESTIGATOR Country: Colombia Facility: Clínica Universitaria Colombia State: Cundinamarca Location 4: City: Ibagué Contacts: *Contact 1:* - Email: [email protected] - Name: Mark Ettenberger, PhD - Phone: +57 60 1 646 6060 - Role: CONTACT Country: Colombia Facility: Clínica Keralty Ibagué State: Tolima Location 5: City: Gdańsk Contacts: *Contact 1:* - Email: [email protected] - Name: Łucja Bieleninik, PhD - Phone: +48 58 523 30 00 - Role: CONTACT *Contact 2:* - Name: Łucja Bieleninik, PhD - Role: PRINCIPAL_INVESTIGATOR *Contact 3:* - Name: Ilona Poćwierz-Marciniak, PhD - Role: SUB_INVESTIGATOR Country: Poland Facility: University of Gdańsk ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423079 Brief Title: Scleral Fixation for Intraocular Lens-Bag Dislocation Official Title: Complex Intaocular Lens-Bag Fixation With Siepser's Scleral Sliding Knots #### Organization Study ID Info ID: Siep_001 #### Organization Class: OTHER Full Name: University of Naples ### Status Module #### Completion Date Date: 2022-05-10 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: COMPLETED #### Primary Completion Date Date: 2019-05-10 Type: ACTUAL #### Start Date Date: 2017-05-10 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: University of Naples #### Responsible Party Investigator Affiliation: University of Naples Investigator Full Name: Luca D'Andrea Investigator Title: Prinicipal investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: Novel introflective sutures offer a minimally invasive approach for stable fixation of dislocated bag-IOL complexes, preserving visual acuity and reducing corneal complications in patients with pseudoexfoliation syndrome. Detailed Description: To assess the one-month outcomes of visual performance and positional stability of capsule-fixated intraocular lenses (IOLs) in patients with IOL-Bag complex dislocation. Patients with intraoperative complications or prior posterior capsule Nd-YAG laser were excluded. Surgical intervention involved creating a superior service keratotomy and using introflective sutures for IOL fixation. Best Corrected Visual acuity (BCVA), endothelial cell counts, and tonometry were assessed at multiple postoperative time points. We also evaluated the mean spherical equivalent (SE), and the residual cylinder and sphere at each follow-up. ### Conditions Module Conditions: - Pseudoexfoliation Syndrome ### Design Module #### Design Info Observational Model: COHORT Time Perspective: RETROSPECTIVE #### Enrollment Info Count: 36 Type: ACTUAL Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Patients affected by pseudoexfoliation syndrome, with inferior dislocation of the bag-IOL complex. Intervention Names: - Procedure: Siepser knots Label: IOL-Bag Dislocation patients ### Interventions #### Intervention 1 Arm Group Labels: - IOL-Bag Dislocation patients Description: Surgical intervention involved creating a superior service keratotomy and using introflective sutures for IOL fixation Name: Siepser knots Type: PROCEDURE ### Outcomes Module #### Primary Outcomes Description: to evaluate the best corrected visual acuity after the surgery Measure: Best corrected visual acuity Time Frame: 1 year #### Secondary Outcomes Description: to evaluate the Endothelial cells count after the surgery Measure: Endothelial cells count Time Frame: 1 year ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * patients affected by pseudoexfoliation syndrome, with inferior dislocation of the bag-IOL complex Exclusion Criteria: * patients who underwent intraoperative complications, * dislocation in the vitreous chamber of the bag-IOL complex, * patients who had already undergone posterior capsule Nd-YAG laser Maximum Age: 90 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: patients affected by pseudoexfoliation syndrome, with inferior dislocation of the bag-IOL complex after cataract surgery. ### Contacts Locations Module #### Locations Location 1: City: NAples Country: Italy Facility: University of Naples Federico II Zip: 80131 ### IPD Sharing Statement Module Access Criteria: available on request Description: all collected IPD IPD Sharing: YES Time Frame: 5 years URL: https://guides.lib.umich.edu/datamanagement/clinicaltrials ## Derived Section ### Condition Browse Module - Ancestors - ID: D000007499 - Term: Iris Diseases - ID: D000014603 - Term: Uveal Diseases - ID: D000005128 - Term: Eye Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC11 - Name: Eye Diseases - Abbrev: BC05 - Name: Musculoskeletal Diseases - Abbrev: BC26 - Name: Wounds and Injuries - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M16355 - Name: Syndrome - Relevance: LOW - As Found: Unknown - ID: M20069 - Name: Exfoliation Syndrome - Relevance: HIGH - As Found: Pseudoexfoliation Syndrome - ID: M7385 - Name: Joint Dislocations - Relevance: LOW - As Found: Unknown - ID: M10531 - Name: Iris Diseases - Relevance: LOW - As Found: Unknown - ID: M17351 - Name: Uveal Diseases - Relevance: LOW - As Found: Unknown - ID: M8271 - Name: Eye Diseases - Relevance: LOW - As Found: Unknown - ID: T5824 - Name: Uveal Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000017889 - Term: Exfoliation Syndrome ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423066 Brief Title: Developing a Machine Learning Model to Predict Pleural Adhesion Preoperatively Using Pleural Ultrasound Official Title: Developing a Machine Learning Model to Predict Pleural Adhesion Preoperatively Using Pleural Ultrasound: a Prospective Observational Study #### Organization Study ID Info ID: USPDPA01 #### Organization Class: OTHER Full Name: Peking Union Medical College Hospital ### Status Module #### Completion Date Date: 2026-03-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-12-30 Type: ESTIMATED #### Start Date Date: 2024-06-01 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Peking Union Medical College Hospital #### Responsible Party Investigator Affiliation: Peking Union Medical College Hospital Investigator Full Name: Xuehan Gao Investigator Title: Research Investigator Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: This study aims to investigate the accuracy of using pleural ultrasound (USP) to identify pleural adhesions in patients who plan to receive video-assisted thoracoscopic surgery. It employs three-dimensional convolutional neural network (3D-CNN) technology to process USP-related images and video data for machine learning, and to establish a diagnostic model for identifying pleural adhesions using 3D-CNN-USP. The study will determine the sensitivity, specificity, positive predictive value, and negative predictive value of 3D-CNN-USP in identifying pleural adhesions. Additionally, it will explore the feasibility and effectiveness of using 3D-CNN-USP for preoperative identification of pleural adhesions in VATS, thereby supporting the implementation of day surgery in thoracic surgery and ultimately serving clinical practice. Detailed Description: Lung cancer is currently the leading cause of death from malignant tumors worldwide. Surgery is the primary treatment method for lung cancer, and breakthroughs in thoracic surgical techniques play a crucial role in the diagnosis and treatment of lung cancer. Medical ultrasound technology, due to its non-invasive, flexible, convenient, and economical characteristics, is widely used in clinical practice. With the advancement of ultrasound technology and the need to address clinical challenges, ultrasound imaging technology has seen new developments in the field of thoracoscopic surgery. In the era of minimally invasive surgery, intraoperative pleural adhesions are one of the main factors affecting the implementation of video-assisted thoracoscopic surgery (VATS). Especially under the concept of enhanced recovery after surgery (ERAS), the day surgery model for VATS has gradually taken shape. However, pleural adhesions significantly increase intraoperative trauma and prolong hospital stays. Additionally, pleural adhesions increase the risk of lung injury during VATS and, in severe cases, may hinder access to the pleural space, necessitating conversion to open thoracotomy. Pleural adhesions increase intraoperative time and morbidity in thoracic surgery due to poor visibility, bleeding, and lung and vascular injuries. The presence, location, and degree of pleural adhesions are useful for determining the initial port placement or choosing between open or VATS approaches. Therefore, accurately predicting the presence and specific location of pleural adhesions preoperatively is crucial for the development of day surgery under thoracic ERAS, ensuring the safety and efficiency of future VATS day surgeries. Previous studies have shown that chest CT is difficult to predict pleural adhesions, with a sensitivity of only 72% and a sensitivity of only 46% for determining adhesions at specific locations. In contrast, ultrasonography of the pleura (USP) can dynamically display pleural sliding and adhesions with surrounding lung tissue, and has real-time monitoring capabilities based on movement, providing unique advantages for detecting pleural adhesions. Preoperative prediction of pleural adhesions using USP has significant application value. Studies have already demonstrated the advantages of using transthoracic pleural ultrasound to identify pleural adhesions. Nicola et al. conducted 1,192 ultrasounds to predict pleural adhesions, confirming 1,124 positive cases and 68 negative cases, with a sensitivity of 80.6%, specificity of 96.1%, positive predictive value of 73.2%, and negative predictive value of 97.4%. However, there are still some issues with using USP to predict pleural adhesions. Physicians who can identify pleural adhesions need to be trained in lung ultrasound, and ultrasound examination and interpretation are skill-dependent techniques. The burden of training thoracic ultrasound physicians remains a clinical challenge. Three-dimensional convolutional neural network (3D-CNN) technology is an emerging technology in the field of artificial intelligence and machine learning. Unlike traditional convolutional neural networks (CNN), 3D-CNN can process three-dimensional data that includes a time dimension, making it suitable for analyzing the real-time dynamic image features of ultrasound images. This technology holds promise for developing a machine learning model to interpret USP images, potentially replacing physician interpretation and improving the accuracy of USP in identifying pleural adhesions. In summary, this study intends to use USP for preoperative identification of pleural adhesions in patients scheduled for VATS surgery. It aims to investigate the accuracy of USP in predicting intraoperative pleural adhesions and to develop a diagnostic model using 3D-CNN technology to process USP-related images and video data for machine learning. The study will explore the sensitivity, specificity, positive predictive value, and negative predictive value of the 3D-CNN-USP model in identifying pleural adhesions. Additionally, it will examine the feasibility and effectiveness of using 3D-CNN-USP for preoperative identification of pleural adhesions to support the implementation of day surgery in thoracic surgery. ### Conditions Module Conditions: - Pleural Diseases - Lung Cancer - Machine Learning Keywords: - pleural adhesion - 3D-CNN - machine learning - VATS ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 200 Type: ESTIMATED Study Type: OBSERVATIONAL ### Outcomes Module #### Primary Outcomes Description: Sensitivity of three-dimensional convolutional neural network (3D-CNN) in identifying pleural adhesions using pleural ultrasound (USP). The sensitivity value ranges from 0 to 100, with higher values indicating greater sensitivity. Measure: Sensitivity Time Frame: From enrollment to the end of surgery. #### Secondary Outcomes Description: Specificity off 3D-CNN in identifying pleural adhesions using USP. The specificity value ranges from 0 to 100, with higher values indicating greater specificity. Measure: Specificity Time Frame: From enrollment to the end of surgery. Description: Positive predictive value (PPV) of 3D-CNN in identifying pleural adhesions using USP. PPV is calculated by dividing the number of true positive results by the total number of positive test results. A higher PPV means that the test is more reliable in correctly identifying those with the condition. Measure: Positive predictive value Time Frame: From enrollment to the end of surgery. Description: Negative predictive value (NPV) of 3D-CNN in identifying pleural adhesions using USP. NPV is calculated by dividing the number of true negative results by the total number of negative test results. A higher NPV means that the test is more reliable in correctly identifying those without the condition. Measure: Negative predictive value Time Frame: From enrollment to the end of surgery. ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Patients who plan to accept VATS surgery. Exclusion Criteria: 1. Patients who can not obtain detailed clinical information; 2. Patients or their family members who can not understand the conditions and objectives of the study or refuse to participate in the study; 3. Patients with conditions affecting observation, such as skin lesions, infections, or scars in the area of the chest wall to be examined. Maximum Age: 80 Years Minimum Age: 12 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT Study Population: Patients who plan to accept VATS surgery in Peking Union Medical college Hospital, and agree to perform preoperative plerual ultrasound examination. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Xuehan Gao, MD Phone: 18801341299 Role: CONTACT Contact 2: Email: [email protected] Name: Yuanjing Gao, MD Phone: 16619765781 Role: CONTACT ### IPD Sharing Statement Module Description: The data of this study will be used in future analyses and be published in academic article. IPD Sharing: NO ### References Module #### References Citation: Mason AC, Miller BH, Krasna MJ, White CS. Accuracy of CT for the detection of pleural adhesions: correlation with video-assisted thoracoscopic surgery. Chest. 1999 Feb;115(2):423-7. doi: 10.1378/chest.115.2.423. PMID: 10027442 Citation: Cassanelli N, Caroli G, Dolci G, Dell'Amore A, Luciano G, Bini A, Stella F. Accuracy of transthoracic ultrasound for the detection of pleural adhesions. Eur J Cardiothorac Surg. 2012 Nov;42(5):813-8; discussion 818. doi: 10.1093/ejcts/ezs144. Epub 2012 Apr 19. PMID: 22518039 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000002921 - Term: Cicatrix - ID: D000005355 - Term: Fibrosis - ID: D000010335 - Term: Pathologic Processes - ID: D000012140 - Term: Respiratory Tract Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M11172 - Name: Lung Neoplasms - Relevance: LOW - As Found: Unknown - ID: M13885 - Name: Pleural Diseases - Relevance: HIGH - As Found: Pleural Diseases - ID: M3620 - Name: Tissue Adhesions - Relevance: HIGH - As Found: Adhesion - ID: M6160 - Name: Cicatrix - Relevance: LOW - As Found: Unknown - ID: M8485 - Name: Fibrosis - Relevance: LOW - As Found: Unknown - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000010995 - Term: Pleural Diseases - ID: D000000267 - Term: Tissue Adhesions ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423053 Brief Title: A Randomized Trial of a College Biology Course With Integrated Mindfulness Official Title: A Randomized Trial of a College Biology Course With Integrated Mindfulness Practice on Student Mindfulness, Learning-Related Anxiety, and Well-Being #### Organization Study ID Info ID: STUDY00032944 #### Organization Class: OTHER Full Name: Trustees of Dartmouth College ### Status Module #### Completion Date Date: 2024-09-01 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: ACTIVE_NOT_RECRUITING #### Primary Completion Date Date: 2024-07-01 Type: ESTIMATED #### Start Date Date: 2024-03-21 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-03-21 Study First Submit QC Date: 2024-05-20 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Trustees of Dartmouth College #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The proposed study aims to evaluate whether integrating mindfulness practice into an undergraduate biology course influences student levels of mindfulness, stress, positive academic emotions, and physical, mental, and social health outcomes. These outcomes will be evaluated for students who enroll in the biology course compared to students who attempted to register but were waitlisted. Detailed Description: The proposed study aims to evaluate whether integrating mindfulness practice into an undergraduate biology course influences student levels of mindfulness, learning-related anxiety and well-being. A two-arm design will look at students who receive the intervention (academic course) plus usual care and a control group of waitlisted students for the course who will only receive university wellness resources. Participants all attempted to register for the course during a set course selection period at the college and were randomly registered or waitlisted by the College Registrar. Students registered and waitlisted for the course will be recruited for the study and those that provide informed consent will be enrolled. Data relating to mindfulness, learning-related anxiety, and well-being will be collected at baseline, mid-intervention (\~5 weeks), at the conclusion of the intervention (\~10 weeks), and at \~20 weeks. The primary analyses will evaluate whether there is a greater 1. increase in mindfulness, 2. increase in composite well-being score, and 3. decrease in learning-related anxiety in the intervention arm compared to the control arm. The secondary analyses will evaluate whether there is a greater 1. increase in heart rate variability and 2. reduction in hair cortisol in the intervention arm compared to the control arm. Secondary analyses will also evaluate differential changes in individual well-being score components (including physical activity, sleep, diet, alcohol use, media use, perceived stress, overall mental well-being, and loneliness). The analytical approach will examine if changes in outcomes are greater in the intervention group than in the usual care group via linear mixed-effect or linear regression models, as appropriate, adjusting for covariates. Statistical analyses will follow an "intention-to-treat" approach and include all participants, regardless of intervention completion. A p-value of \<.05 will be used as the threshold for statistical significance for all tests. In addition, any outcomes with observed statically significant differences between the arms will be re-collected and analyzed for differences at \~10 weeks post-intervention. ### Conditions Module Conditions: - Mindfulness - Stress Psychological - Stress, Physiological ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Students who attempted to enroll in Biology 3: Mindful Physiology at Dartmouth College during the course selection period were randomly assigned to the class or waitlist by the college registrar. The intervention is participation in Biology 3, a college biology course with integrated mindfulness practices along with usual access to the College's wellness offerings. The control condition is the waitlist for Biology 3 along with usual access to the College's wellness offerings. ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 60 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: This arm consists of students enrolled in Dartmouth College's Biology 3 course during Spring 2024 term, who will have access to course offerings and usual university wellness resources (as described for the control arm). Intervention Names: - Behavioral: Biology Course with Integrated Mindfulness Label: Biology 3 students Type: EXPERIMENTAL #### Arm Group 2 Description: This arm consists of students waitlisted for Dartmouth College's Biology 3 course during Spring 2024 term. They will receive university wellness resources as usual. These include access to wellness counselors, mental health advisors, and psychiatrists at the university's counseling center, wellness advising at the student wellness center, and campus-wide wellness programs, such as weekly group yoga and meditation sessions and a free subscription to the Headspace app. The 4-hr mindfulness retreat will also be advertised to and open to all Dartmouth students. Label: Biology 3 waitlisted students Type: NO_INTERVENTION ### Interventions #### Intervention 1 Arm Group Labels: - Biology 3 students Description: This intervention is a college biology course with embedded mindfulness practice. There are 17 class sessions, each 1 hr and 50 min. long, over 9.5 weeks. Students will be taught human physiology through didactic lectures, laboratory activities, and written tests typical for a college course. Each class meeting will have \~20 min. of mindfulness practice in Thich Nhat Hanh's Plum Village tradition. Students are recommended to practice mindfulness for 15 minutes daily. Students are assigned a daily log of their mindfulness practice, and they are given full credit for each log completion regardless of the minutes of mindfulness practices. Students are assigned a weekly written reflection to reflect on the physiology course content and/or their mindfulness practice. All students in the class are required to attend a 4-hr mindfulness retreat Students in the intervention arm will also receive university wellness resources as usual as described for the control arm below. Name: Biology Course with Integrated Mindfulness Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: Trait mindfulness will be measured via the Five Facet Mindfulness Questionnaire (FFMQ; total possible score range: 1-5; higher scores indicate higher trait mindfulness). Measure: Trait Mindfulness Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) Description: Application of mindfulness in everyday life will be measured via the Applied Mindfulness Process Scale (AMPS; total possible score range: 0-60; higher scores indicate more application of mindfulness practice in daily life). Measure: Applied Mindfulness Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) Description: A well-being score assessing physical, emotional, and social health and behaviors, adapted from Loucks et al. (2021): sleep (5-day accelerometry and/or Pittsburg Sleep Quality Index, total possible score range: 0-21; higher scores indicate poorer sleep quality), physical activity (International Physical Activity Questionnaire and/or 5-day accelerometry), diet (short Health Eating Index; range: 0-100; higher scores indicate higher diet quality), alcohol intake (Quick Drinking Screen), media use (Bergen Social Media Addiction Scale; range: 6-30; higher scores indicate more problematic media use), stress (Perceived Stress Scale-10; range: 0-40; higher scores indicate more perceived stress), mental well-being (Warwick-Edinburgh Mental Well-being Scale; range: 14-70; higher scores show more mental well-being), and loneliness (UCLA-Loneliness Scale; range: 0-60; higher scores show more perceived loneliness). This composite score will be the mean z-score across the above-mentioned measures. Measure: Composite Well-Being Score Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) Description: Learning-related anxiety subscale from the Achievement Emotion Questionnaire-short version (AEQ-S; total possible score range: 1-5; higher scores indicate greater learning-related anxiety). Measure: Learning-Related Anxiety Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) #### Secondary Outcomes Description: Measured via a polar chest strap for 24 hours Measure: Physiologic Stress (HRV) Time Frame: Baseline and intervention completion(~10 weeks) Description: Measured via hair cortisol concentration Measure: Physiologic Stress (Cortisol) Time Frame: Baseline and intervention completion (~10 weeks) Description: Measured via Self-Compassion Scale (; total possible score range: 1-5; higher scores indicate higher levels of self-compassion) Measure: Self-Compassion Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) Description: Measured via Gratitude Questionnaire (GQ-6; total possible score range: 1-7; higher scores indicate higher levels of trait gratitude) Measure: Trait Gratitude Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) Description: Measured via Mindful Eating Questionnaire (MEQ; total possible score range: 1-4; higher scores indicate more mindful eating) Measure: Mindful Eating Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) Description: Each component of the composite well-being score described above will be assessed separately in secondary analyses. Measure: Components of Composite Well-Being Score Time Frame: Baseline, mid-intervention (~5 weeks), and intervention completion (~10 weeks) ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Current Dartmouth student who selected Biology 3: Mindful Physiology during 2024 Spring term course enrollment period. Exclusion Criteria: - Healthy Volunteers: True Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Hanover Country: United States Facility: Media and Health Behaviors Lab at Dartmouth State: New Hampshire Zip: 03755 #### Overall Officials Official 1: Affiliation: Dartmouth College Name: Diane I Gilbert-Diamond, ScD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module Access Criteria: Data Sharing Agreement Institutional Human Subjects Research Protocol Approval Description: De-identified participant data will be made available to other researchers upon request to the Principal Investigator with a data sharing agreement provided that the researchers have appropriate human subjects research approval. Info Types: - STUDY_PROTOCOL - SAP - ICF - CSR - ANALYTIC_CODE IPD Sharing: YES Time Frame: Data will become available October 1, 2026. ### References Module #### References Citation: Baer R. Assessment of mindfulness by self-report. Curr Opin Psychol. 2019 Aug;28:42-48. doi: 10.1016/j.copsyc.2018.10.015. Epub 2018 Nov 2. PMID: 30423507 Citation: Baer RA, Smith GT, Hopkins J, Krietemeyer J, Toney L. Using self-report assessment methods to explore facets of mindfulness. Assessment. 2006 Mar;13(1):27-45. doi: 10.1177/1073191105283504. PMID: 16443717 Citation: Bamber, M. D., & Schneider, J. K. (2022). College students' perceptions of mindfulness-based interventions: A narrative review of the qualitative research. Current Psychology, 41(2), 667-680. https://doi.org/10.1007/s12144-019-00592-4 Citation: Black, D. S. (2015). Mindfulness Training for Children and Adolsecents: A State-of-the-Science Review. In Handbook of Mindfulness: Theory, Research, and Practice (pp. 283-310). Guilford Publications. Citation: Buysse DJ, Reynolds CF 3rd, Monk TH, Berman SR, Kupfer DJ. The Pittsburgh Sleep Quality Index: a new instrument for psychiatric practice and research. Psychiatry Res. 1989 May;28(2):193-213. doi: 10.1016/0165-1781(89)90047-4. PMID: 2748771 Citation: Cohen S, Kamarck T, Mermelstein R. A global measure of perceived stress. J Health Soc Behav. 1983 Dec;24(4):385-96. No abstract available. PMID: 6668417 Citation: Colby S, Zhou W, Allison C, Mathews AE, Olfert MD, Morrell JS, Byrd-Bredbenner C, Greene G, Brown O, Kattelmann K, Shelnutt K. Development and Validation of the Short Healthy Eating Index Survey with a College Population to Assess Dietary Quality and Intake. Nutrients. 2020 Aug 27;12(9):2611. doi: 10.3390/nu12092611. PMID: 32867172 Citation: Craig CL, Marshall AL, Sjostrom M, Bauman AE, Booth ML, Ainsworth BE, Pratt M, Ekelund U, Yngve A, Sallis JF, Oja P. International physical activity questionnaire: 12-country reliability and validity. Med Sci Sports Exerc. 2003 Aug;35(8):1381-95. doi: 10.1249/01.MSS.0000078924.61453.FB. PMID: 12900694 Citation: Dawson AF, Brown WW, Anderson J, Datta B, Donald JN, Hong K, Allan S, Mole TB, Jones PB, Galante J. Mindfulness-Based Interventions for University Students: A Systematic Review and Meta-Analysis of Randomised Controlled Trials. Appl Psychol Health Well Being. 2020 Jul;12(2):384-410. doi: 10.1111/aphw.12188. Epub 2019 Nov 19. PMID: 31743957 Citation: Dum M, Sobell LC, Sobell MB, Heinecke N, Voluse A, Johnson K. A Quick Drinking Screen for identifying women at risk for an alcohol-exposed pregnancy. Addict Behav. 2009 Sep;34(9):714-6. doi: 10.1016/j.addbeh.2009.04.001. Epub 2009 Apr 8. PMID: 19406583 Citation: Framson C, Kristal AR, Schenk JM, Littman AJ, Zeliadt S, Benitez D. Development and validation of the mindful eating questionnaire. J Am Diet Assoc. 2009 Aug;109(8):1439-44. doi: 10.1016/j.jada.2009.05.006. PMID: 19631053 Citation: Galante J, Dufour G, Vainre M, Wagner AP, Stochl J, Benton A, Lathia N, Howarth E, Jones PB. 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PMID: 26858469 Citation: Liu D, Kahathuduwa C, Vazsonyi AT. The Pittsburgh Sleep Quality Index (PSQI): Psychometric and clinical risk score applications among college students. Psychol Assess. 2021 Sep;33(9):816-826. doi: 10.1037/pas0001027. Epub 2021 May 20. PMID: 34014747 Citation: Shapiro, S. L., & Jazaieri, H. (2015). Mindfulness-Based Stress Reduction for Healthy Stressed Adults. In Handbook of mindfulness: Theory, research, and practice (pp. 269-282). The Guilford Press. Citation: Sobell LC, Agrawal S, Sobell MB, Leo GI, Young LJ, Cunningham JA, Simco ER. Comparison of a quick drinking screen with the timeline followback for individuals with alcohol problems. J Stud Alcohol. 2003 Nov;64(6):858-61. doi: 10.15288/jsa.2003.64.858. PMID: 14743950 Citation: Tennant R, Hiller L, Fishwick R, Platt S, Joseph S, Weich S, Parkinson J, Secker J, Stewart-Brown S. The Warwick-Edinburgh Mental Well-being Scale (WEMWBS): development and UK validation. 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An Open-Source Monitor-Independent Movement Summary for Accelerometer Data Processing. J Meas Phys Behav. 2019 Dec;2(4):268-281. doi: 10.1123/jmpb.2018-0068. PMID: 34308270 Citation: Wright KD, Hickman R, Laudenslager ML. Hair Cortisol Analysis: A Promising Biomarker of HPA Activation in Older Adults. Gerontologist. 2015 Jun;55 Suppl 1(Suppl 1):S140-5. doi: 10.1093/geront/gnu174. PMID: 26055775 Citation: Li K, Cardoso C, Moctezuma-Ramirez A, Elgalad A, Perin E. Heart Rate Variability Measurement through a Smart Wearable Device: Another Breakthrough for Personal Health Monitoring? Int J Environ Res Public Health. 2023 Dec 6;20(24):7146. doi: 10.3390/ijerph20247146. PMID: 38131698 Citation: Mccullough ME, Emmons RA, Tsang JA. The grateful disposition: a conceptual and empirical topography. J Pers Soc Psychol. 2002 Jan;82(1):112-27. doi: 10.1037//0022-3514.82.1.112. PMID: 11811629 Citation: Neff, K.D. The Self-Compassion Scale is a Valid and Theoretically Coherent Measure of Self-Compassion. Mindfulness 7, 264-274 (2016). https://doi.org/10.1007/s12671-015-0479-3 ## Derived Section ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M4324 - Name: Anxiety Disorders - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423040 Brief Title: Social Media Chatbot on Physical Activity Education for Older Adults Official Title: Exploring the Effectiveness of Applying Social Media Chatbot for Providing Real-Time Feedback on Physical Activity Education for Older Adults #### Organization Study ID Info ID: N202403043 #### Organization Class: OTHER Full Name: Taipei Medical University ### Status Module #### Completion Date Date: 2025-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-12 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-04 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-08 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Taipei Medical University #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: In this study, a social media chatbot was used to provide a continuous and real-time multimedia health education program on physical activity for the older adults, as well as supportive messages and feedbacks, to improve physical activity and exercise self-efficacy among the older adults. This study was a cluster randomized trial, and participants were recruited from community care stations and activity centers in Taipei City. The experimental group was involved in an 8-week, 5-day-a-week intervention with a total of 40 multimedia physical activity education programs, and users were provided with real-time feedback interactions and regular physical activity education guidelines, and self-administered questionnaires were used for data collection. The research instruments include basic personal information, International Physical Activity Questionnaire, Exercise Self-Efficacy Scale, Behavioral regulation in exercise questionnaire-2, Exercise Benefits/Barriers Scale, and the statistical methods will be descriptive statistics, independent sample t-test, paired sample t-test, and one-way analysis of covariance. ### Conditions Module Conditions: - Exercise - Self Efficacy - Behavioral Regulation - Healthy Aging ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: PREVENTION #### Enrollment Info Count: 104 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Label: Control Type: NO_INTERVENTION #### Arm Group 2 Intervention Names: - Other: Social Media Chatbot on Physical Activity Education Label: Experiment Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Experiment Description: a social media chatbot was used to provide a continuous and real-time multimedia health education program on physical activity for the older adults, as well as supportive messages and feedbacks. Name: Social Media Chatbot on Physical Activity Education Type: OTHER ### Outcomes Module #### Primary Outcomes Description: International Physical Activity Questionnaire Measure: Physical activity Time Frame: up to 8 weeks Description: Exercise Self-Efficacy Scale Measure: Self-Efficacy Time Frame: up to 8 weeks Description: Behavioral regulation in exercise questionnaire-2 Measure: Behavioral regulation Time Frame: up to 8 weeks Description: Exercise Benefits/Barriers Scale Measure: Benefits/Barriers Time Frame: up to 8 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Persons aged 60 to 85 years old living in Taipei City, healthy or with chronic conditions 2. Those who can listen, read and write Chinese 3. Those who have used smartphones in the past month and can use Line social software 4. Those who voluntarily participate in this study, can understand the research content after explanation and explanation, and sign the subject consent form Exclusion Criteria: 1. Those who are advised by a doctor not to exercise 2. Those who must exercise under the supervision of medical personnel 3. Patients with severe cardiovascular disease 4. Anyone with disability or cognitive impairment 5. Persons living in long-term care institutions Healthy Volunteers: True Maximum Age: 85 Years Minimum Age: 60 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423027 Brief Title: Nature-Oriented Chatbots on Older Adults' Mental Health Official Title: Exploring the Influence of Nature-Oriented Chatbots on the Mental Health of Older Adults Living Alone #### Organization Study ID Info ID: N202403042 #### Organization Class: OTHER Full Name: Taipei Medical University ### Status Module #### Completion Date Date: 2025-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2024-12 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-04 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-08 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Taipei Medical University #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: This study aims to explore the influence of nature-oriented chatbots on the mental health of older adults residing alone. Leveraging the therapeutic potential of nature exposure and the interactive capabilities of chatbot technology, our research seeks to investigate whether engaging with nature-oriented chatbots can mitigate feelings of depression, and loneliness while enhancing overall psychological well-being and quality of life. Through a combination of experimental interventions and psychological assessments, the investigators will assess the impact of nature-oriented chatbots on participants' mental health outcomes. ### Conditions Module Conditions: - Depression - Loneliness - Happiness - Connection With Nature - Anxiety ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: PREVENTION #### Enrollment Info Count: 60 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Label: Control Type: NO_INTERVENTION #### Arm Group 2 Intervention Names: - Behavioral: Nature-Oriented Chatbots Label: Experiment Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Experiment Description: Nature-oriented chatbots are an intervention with nature-based video delivered by self-developed chatbots Name: Nature-Oriented Chatbots Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: The Geriatric Depression Scale Measure: Depression Time Frame: up to 8 weeks Description: UCLA loneliness (ULS-8) Measure: loneliness Time Frame: up to 8 weeks Description: Well-being of Older People measure (WOOP) Measure: happiness Time Frame: up to 8 weeks Description: Connectedness with nature scale (CNS） Measure: connection with nature Time Frame: up to 8 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Individuals aged 60 years and above who live alone. 2. Regular users of smartphones, with internet access, and proficient in using LINE. 3. Individuals who consent to participate in the study and sign the consent form. 4. Capable of understanding interactive messages and the content of pre- and post-test questionnaires. Exclusion Criteria: 1. Individuals without smartphones, internet access, or not using LINE. 2. Diagnosed with sensory impairments. 3. Diagnosed with mental illnesses requiring continuous treatment. Healthy Volunteers: True Maximum Age: 90 Years Minimum Age: 60 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001526 - Term: Behavioral Symptoms ### Condition Browse Module - Browse Branches - Abbrev: BXM - Name: Behaviors and Mental Disorders - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M7058 - Name: Depression - Relevance: HIGH - As Found: Depression - ID: M4324 - Name: Anxiety Disorders - Relevance: LOW - As Found: Unknown - ID: M7061 - Name: Depressive Disorder - Relevance: LOW - As Found: Unknown - ID: M4818 - Name: Behavioral Symptoms - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000003863 - Term: Depression ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423014 Brief Title: Smart mHealth Strategy for Physical Activity and Health Promotion Official Title: Smart mHealth Strategy in the Delivery of Behavior Change Techniques for Physical Activity and Health Promotion #### Organization Study ID Info ID: N202303041 #### Organization Class: OTHER Full Name: Taipei Medical University ### Status Module #### Completion Date Date: 2026-12 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2026-07 Type: ESTIMATED #### Start Date Date: 2023-05-01 Type: ACTUAL Status Verified Date: 2024-03 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-08 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Taipei Medical University #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: The purpose of this study is to develop a Smart mHealth Strategy that delivers behavior change techniques through wearable physical activity trackers and social media chatbots, including self-monitoring, real-time feedback and reminders, goal-setting, competition and rewards, social support, and health coaching. This study also aims to explore the effect of the Smart mHealth Strategy on the behavioral outcomes and psychological factors of physical activity, and physical and mental health. The study design is a three-stage randomized controlled trial. In each stage, 120 are recruited and randomly assigned to control and experimental groups. Participants are adults with insufficient physical activity and a sedentary lifestyle. The Smart mHealth Strategy uses smartwatches and self-developed chatbots. The constrained dialogue content is designed to finally deliver the six behavior change techniques. Data are collected in the pre-, mid-, and post-tests. The measurement includes self-administered questionnaires, Actigraphy GT9X, Inbody 270S, OMRON HEM-7130, and heart rate variability monitors. ### Conditions Module Conditions: - Health Behavior Change - Wearable Technology - Chatbot - Social Media - Sedentary Lifestyle ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: PREVENTION #### Enrollment Info Count: 360 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Label: Control Type: NO_INTERVENTION #### Arm Group 2 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with the 1st behavior change technique - Behavioral: Wearable devices with the 2nd behavior change technique - Behavioral: Wearable devices with the 3rd behavior change technique - Behavioral: Wearable devices with the 4th behavior change technique - Behavioral: Wearable devices with the 5th behavior change technique - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices only Type: ACTIVE_COMPARATOR #### Arm Group 3 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices with the 1st behavior change technique Type: EXPERIMENTAL #### Arm Group 4 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices with the 2nd behavior change technique Type: EXPERIMENTAL #### Arm Group 5 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices with the 3rd behavior change technique Type: EXPERIMENTAL #### Arm Group 6 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices with the 4th behavior change technique Type: EXPERIMENTAL #### Arm Group 7 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices with the 5th behavior change technique Type: EXPERIMENTAL #### Arm Group 8 Intervention Names: - Behavioral: Wearable devices only - Behavioral: Wearable devices with all behavior change techniques Label: Wearable devices with all behavior change techniques Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Wearable devices only - Wearable devices with all behavior change techniques - Wearable devices with the 1st behavior change technique - Wearable devices with the 2nd behavior change technique - Wearable devices with the 3rd behavior change technique - Wearable devices with the 4th behavior change technique - Wearable devices with the 5th behavior change technique Description: self-monitoring Name: Wearable devices only Type: BEHAVIORAL #### Intervention 2 Arm Group Labels: - Wearable devices only Description: reminder Name: Wearable devices with the 1st behavior change technique Type: BEHAVIORAL #### Intervention 3 Arm Group Labels: - Wearable devices only Description: social support Name: Wearable devices with the 2nd behavior change technique Type: BEHAVIORAL #### Intervention 4 Arm Group Labels: - Wearable devices only Description: Competition Name: Wearable devices with the 3rd behavior change technique Type: BEHAVIORAL #### Intervention 5 Arm Group Labels: - Wearable devices only Description: Goal-setting Name: Wearable devices with the 4th behavior change technique Type: BEHAVIORAL #### Intervention 6 Arm Group Labels: - Wearable devices only Description: health coach Name: Wearable devices with the 5th behavior change technique Type: BEHAVIORAL #### Intervention 7 Arm Group Labels: - Wearable devices only - Wearable devices with all behavior change techniques - Wearable devices with the 1st behavior change technique - Wearable devices with the 2nd behavior change technique - Wearable devices with the 3rd behavior change technique - Wearable devices with the 4th behavior change technique - Wearable devices with the 5th behavior change technique Description: Self-monitoring, health coach, goal-setting, competition, social support, and reminder Name: Wearable devices with all behavior change techniques Type: BEHAVIORAL ### Outcomes Module #### Primary Outcomes Description: International Physical Activity Questionnaire (IPAQ-SF, MET-minute/week) Measure: Subjective physical activity Time Frame: up to 12 weeks Description: Actigraphy GT9X and GT3X (MET-minute/week) Measure: Objective physical activity Time Frame: up to 12 weeks Description: Higher score higher benefits and barriers Measure: Exercise Benefits/Barriers Scale-Concise (EBBS-C) Time Frame: up to 12 weeks Description: Higher score higher self-efficacy Measure: Exercise self-efficacy scale (EXSE) Time Frame: up to 12 weeks Description: Higher score higher Self-Regulation Measure: Physical Activity Self-Regulation Scale (PASR) Time Frame: up to 12 weeks Description: Higher score higher Behavioural Regulation Measure: Behavioural Regulation in Exercise Questionnaire (BREQ-3) Time Frame: up to 12 weeks #### Secondary Outcomes Description: Body mass index (BMI, kg/m\^2), skeletal muscle index (SMI, kg/m\^2), body fat percentage (%), body fat mass (kg), and fat-free mass (kg) Measure: body composition (Inbody) Time Frame: up to 12 weeks Description: Systolic and diastolic blood pressure (mmHg) Measure: blood pressure Time Frame: up to 12 weeks Description: Total power (TP, 0-0.5 Hz), low-frequency power (LF, 0.04-0.15 Hz), high-frequency power (HF, 0.15-0.40 Hz), the ratio of low frequency to high frequency (LF/HF), and the standard deviation of all normal-to-normal intervals (SDNN) Measure: heart rate variability Time Frame: up to 12 weeks Description: Higher score worse mental health Measure: Depression Anxiety Stress Scale (DASS) Time Frame: up to 12 weeks Description: Higher score higher Quality of Life Measure: World Health Organization Quality of Life Scale (WHOQOL-BREF) Time Frame: up to 12 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: Adults who is the age of majority, with insufficient physical activity, and a sedentary lifestyle who have smartphones Exclusion Criteria: * Individuals' health conditions may affect physical activity in daily living and the experiment, such as disability, serious health problems * There are unconventional life plans during the experiment, such as going abroad for vacation, pregnancy, and surgery. * Individuals have using experiences in any wearable physical activity trackers in the past six months ④ People who have ever had severe allergies to any wearable device ⑤ Professional athletes or student-athletes Healthy Volunteers: True Maximum Age: 70 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Hsin-Yen Yen, PhD Phone: 886-2-2736-1661 Phone Ext: 6326 Role: CONTACT #### Locations Location 1: City: Taipei City Contacts: *Contact 1:* - Email: [email protected] - Name: Hsin-Yen Yen, PhD - Phone: 886-2-2736-1661 - Phone Ext: 6326 - Role: CONTACT Country: Taiwan Facility: Taipei Medical University Status: RECRUITING Zip: 110 ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06423001 Acronym: prePO23 Brief Title: Efficacy and Safety of Oral Administration of Postibiotic by FOS Fermentation From Lactobacillus Paracasei in the Treatment of Irritable Bowel Syndrome. Official Title: A Randomized, Cross-over, Placebo-Controlled, Double-Blind Clinical Trial on the Efficacy and Safety of Oral Administration of Postibiotic by FOS Fermentation From Lactobacillus Paracasei in the Treatment of Irritable Bowel Syndrome. #### Organization Study ID Info ID: ID 2939 #### Organization Class: OTHER Full Name: Istituto Clinico Humanitas ### Status Module #### Completion Date Date: 2026-05-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-29 Type: ACTUAL Last Update Submit Date: 2024-05-28 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2025-05-15 Type: ESTIMATED #### Start Date Date: 2024-06-15 Type: ESTIMATED Status Verified Date: 2024-04 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-24 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Istituto Clinico Humanitas #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: Irritable bowel syndrome (IBS) is a highly prevalent functional pathology which currently has no real standardized and effective therapy, despite having a significant impact on quality of life and on social-health costs. Post-biotics have demonstrated in various in vitro and in vivo studies the ability to modulate the microbiota, the intestinal barrier function, the immune response as well as having systemic effects, with prospects for good efficacy in treatment of IBS. Detailed Description: PostbiotiX Slowing is a food supplement based on Fermented FOS from Lactobacillus paracasei CNCM I-5220, mallow and chamomile. The Fermented FOS from Lactobacillus paracasei CNCM I-5220 (postbiotic) is the result of a controlled fermentation. The fermentation process allows to eliminate all the individual variability that depends on the microbiota, the diet and the psycho-physical conditions of the single individual, offering a mixture of bacterial metabolites and fermented fiber (postbiotic), which has the functional activity. In addition, as FOS is already fermented it does not induce the formation of gas typical of fiber fermentation in IBS patients, thus providing all the beneficial effects of the fiber without its side effects. The fermented FOS from Lactobacillus paracasei CNCM I-5220 (postbiotic) is easily absorbed by the gut. Dosage and method of use: PostbiotiX Slowing 4 g sachets, administered at the dosage of one sachet a day. To pour the contents of the sachet in a glass, add 150 ml of water, mix until complete dissolution of the powder and taken immediately, preferably as soon as awakened, and away from meals. Ingredients: Maltodextrin, Aroma, Fermented FOS from Lactobacillus paracasei CNCM I-5220, mallow (Malva sylvestris L.) flowers and leaves d.e. tit. 20% polysaccharides, chamomile (Matricaria chamomilla L.) flowers d.e. tit. 0.3% apigenin, acidity regulator: citric acid; anti-caking agent: silicon dioxide; sweetener: sucralose. Conservation method: to be kept in a cool and dry place, away from light, humidity, and direct sources of heat. ### Conditions Module Conditions: - IBS - Irritable Bowel Syndrome ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: SEQUENTIAL ##### Masking Info Masking: SINGLE Who Masked: - PARTICIPANT Primary Purpose: OTHER #### Enrollment Info Count: 36 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Each patient will be supplied with the investigational product at Visit 0 (V0, Kit V0, PostibiotiX Slowing) and at visit 3 (V3, Kit V3, Placebo), based on the outcome of the randomization at V0 (Sequence AB, PostbiotiX Slowing/Placebo). Intervention Names: - Dietary Supplement: PostbiotiX Slowing 4 g sachets PostbiotiX Slowing is a food supplement based on Fermented FOS from Lactobacillus paracasei CNCM I-5220. Label: PostbiotiX Slowing (Treatment A) Sequence AB Type: EXPERIMENTAL #### Arm Group 2 Description: Each patient will be supplied with the investigational product at Visit 0 (V0, Kit V0, Placebo) and at visit 3 (V3, Kit V3, PostibiotiX Slowing), based on the outcome of the randomization at V0 (Sequence BA, Placebo/PostbiotiX Slowing). Intervention Names: - Dietary Supplement: PostbiotiX Slowing 4 g sachets PostbiotiX Slowing is a food supplement based on Fermented FOS from Lactobacillus paracasei CNCM I-5220. Label: Placebo (Tratment B) Sequence BA Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Placebo (Tratment B) Sequence BA - PostbiotiX Slowing (Treatment A) Sequence AB Description: Each patient will be supplied with the investigational product at Visit 0, PostibiotiX Slowing and at visit 3, based on the outcome of the randomization at V0 (Sequence AB, PostbiotiX Slowing/Placebo; Sequence BA, Placebo/PostbiotiX Slowing). Name: PostbiotiX Slowing 4 g sachets PostbiotiX Slowing is a food supplement based on Fermented FOS from Lactobacillus paracasei CNCM I-5220. Type: DIETARY_SUPPLEMENT ### Outcomes Module #### Primary Outcomes Description: Evaluated using a symptom measurement scale, at each visit, on a 4-point Likert scale (IBS symptom scale; 4 symptoms for a minimum sum score of 0, maximum 12). Measure: Reduction in symptom intensity Time Frame: 10 weeks #### Secondary Outcomes Description: IBS-SSS is a five-item questionnaire measuring frequency and intensity of abdominal pain, the severity of abdominal distension, dissatisfaction with bowel habits, and the interference of IBS with daily life, scoring from 0 to 500. Measure: Change from baseline in IBS-SSS (symptom severity score) Time Frame: up to 4 weeks Description: To assess adequate overall relief, patients will be asked weekly to answer the question "Compared to how you usually felt before taking the treatment, how would you rate your symptom relief (abdominal pain, bowel habits, and other symptoms of IBS) in the past 10 days?" Possible answers: 1, very relieved; 2, relieved; 3, somewhat relieved; 4, unchanged; 5, slightly worsened; 6, worsened; 7, much worsened. Measure: Adequate overall symptom relief after treatment, Time Frame: up to 10 days Description: Severity score of each of the individual symptoms included in the IBS-SSS (VAS sub-scores), assessed by numeric rating scale (NRS) from 0 to 100 Measure: Change from baseline after treatment in NRS: Time Frame: up to 10 days Description: Quality of life as assessed by IBS-QoL: The individual responses to the 34 items are summed and averaged for a total score and then transformed to a 0-100 scale for ease of interpretation with higher scores indicating better IBS specific quality of life Measure: Change from baseline after treatment in QqL: Time Frame: up to 10 days Description: Hospital anxiety and depression scale (HADS): HADS is a fourteen-item scale with seven items each for anxiety and depression subscales. Scoring for each item ranges from zero to three. A subscale score \>8 denotes anxiety or depression. Measure: Change from baseline after treatment in HADS: Time Frame: up to 10 days Description: Additional functional parameters in stool analysis differences before and after treatment (for example: digestive residues, bile acids, proteic composition) Measure: Fecal metagenomics: Time Frame: up to 10 days Description: Differences before and after treatment in the Sieric/plasma molecules such as for example Zonulin, soluble CD14, plasmatic inflammatory cytokines, bacterial DNA in the blood, and PBMCs analysis Measure: Analyses of metabolomic: Time Frame: up to 10 days ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * 18-75 years * IBS diagnosis according to ROME IV criteria * Mild-moderate disease defined by IBS-SSS questionnaire at the baseline visit and after the washout period * Signed Informed Consent * Patients' ability to comply with the study procedures * Stable diet within two months prior to the screening visit * Negative colonoscopy (only \> 50 years old patients) Exclusion Criteria: * Therapy with drugs or supplements included in the prohibited list * Malignancy or history of malignancy, except patients with a history of surgically removed extraintestinal malignancy and a 5-year disease-free interval * Unstable psychiatric pathology * Organic bowel disease * Major abdominal surgery, except appendectomy and cholecystectomy * Relevant organic, systemic, metabolic pathologies or significant laboratory test abnormalities * Pregnant or nursing women * Patients with known hypersensitivity to one or more components of the product Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Alessandro Repici, MD Phone: 0282247493 Role: CONTACT Contact 2: Email: [email protected] Name: Vincenzo Craviotto, MD Phone: 0282243113 Role: CONTACT #### Locations Location 1: City: Rozzano Country: Italy Facility: Department of Gastroenterology, Humanitas Research Hospital State: Milano Zip: 20089 ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ### References Module #### References Citation: Lacy BE, Pimentel M, Brenner DM, Chey WD, Keefer LA, Long MD, Moshiree B. ACG Clinical Guideline: Management of Irritable Bowel Syndrome. Am J Gastroenterol. 2021 Jan 1;116(1):17-44. doi: 10.14309/ajg.0000000000001036. PMID: 33315591 Citation: Oka P, Parr H, Barberio B, Black CJ, Savarino EV, Ford AC. Global prevalence of irritable bowel syndrome according to Rome III or IV criteria: a systematic review and meta-analysis. Lancet Gastroenterol Hepatol. 2020 Oct;5(10):908-917. doi: 10.1016/S2468-1253(20)30217-X. Epub 2020 Jul 20. Erratum In: Lancet Gastroenterol Hepatol. 2020 Dec;5(12):e8. PMID: 32702295 Citation: Inadomi JM, Fennerty MB, Bjorkman D. Systematic review: the economic impact of irritable bowel syndrome. Aliment Pharmacol Ther. 2003 Oct 1;18(7):671-82. doi: 10.1046/j.1365-2036.2003.t01-1-01736.x. PMID: 14510740 Citation: Camilleri M. Management Options for Irritable Bowel Syndrome. Mayo Clin Proc. 2018 Dec;93(12):1858-1872. doi: 10.1016/j.mayocp.2018.04.032. PMID: 30522596 Citation: Salminen S, Collado MC, Endo A, Hill C, Lebeer S, Quigley EMM, Sanders ME, Shamir R, Swann JR, Szajewska H, Vinderola G. The International Scientific Association of Probiotics and Prebiotics (ISAPP) consensus statement on the definition and scope of postbiotics. Nat Rev Gastroenterol Hepatol. 2021 Sep;18(9):649-667. doi: 10.1038/s41575-021-00440-6. Epub 2021 May 4. Erratum In: Nat Rev Gastroenterol Hepatol. 2021 Jun 15;: Nat Rev Gastroenterol Hepatol. 2022 Aug;19(8):551. PMID: 33948025 Citation: Tsilingiri K, Barbosa T, Penna G, Caprioli F, Sonzogni A, Viale G, Rescigno M. Probiotic and postbiotic activity in health and disease: comparison on a novel polarised ex-vivo organ culture model. Gut. 2012 Jul;61(7):1007-15. doi: 10.1136/gutjnl-2011-300971. Epub 2012 Feb 1. PMID: 22301383 Citation: Tsilingiri K, Rescigno M. Postbiotics: what else? Benef Microbes. 2013 Mar 1;4(1):101-7. doi: 10.3920/BM2012.0046. PMID: 23271068 Citation: Aguilar-Toala JE, Arioli S, Behare P, Belzer C, Berni Canani R, Chatel JM, D'Auria E, de Freitas MQ, Elinav E, Esmerino EA, Garcia HS, da Cruz AG, Gonzalez-Cordova AF, Guglielmetti S, de Toledo Guimaraes J, Hernandez-Mendoza A, Langella P, Liceaga AM, Magnani M, Martin R, Mohamad Lal MT, Mora D, Moradi M, Morelli L, Mosca F, Nazzaro F, Pimentel TC, Ran C, Ranadheera CS, Rescigno M, Salas A, Sant'Ana AS, Sivieri K, Sokol H, Taverniti V, Vallejo-Cordoba B, Zelenka J, Zhou Z. Postbiotics - when simplification fails to clarify. Nat Rev Gastroenterol Hepatol. 2021 Nov;18(11):825-826. doi: 10.1038/s41575-021-00521-6. No abstract available. PMID: 34556825 Citation: Ma L, Tu H, Chen T. Postbiotics in Human Health: A Narrative Review. Nutrients. 2023 Jan 6;15(2):291. doi: 10.3390/nu15020291. PMID: 36678162 Citation: Adams CA. The probiotic paradox: live and dead cells are biological response modifiers. Nutr Res Rev. 2010 Jun;23(1):37-46. doi: 10.1017/S0954422410000090. Epub 2010 Apr 20. PMID: 20403231 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000004194 - Term: Disease - ID: D000010335 - Term: Pathologic Processes - ID: D000003109 - Term: Colonic Diseases, Functional - ID: D000003108 - Term: Colonic Diseases - ID: D000007410 - Term: Intestinal Diseases - ID: D000005767 - Term: Gastrointestinal Diseases - ID: D000004066 - Term: Digestive System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M16355 - Name: Syndrome - Relevance: HIGH - As Found: Syndrome - ID: M25118 - Name: Irritable Bowel Syndrome - Relevance: HIGH - As Found: Irritable Bowel Syndrome - ID: M6336 - Name: Colonic Diseases - Relevance: LOW - As Found: Unknown - ID: M6337 - Name: Colonic Diseases, Functional - Relevance: LOW - As Found: Unknown - ID: M10444 - Name: Intestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: T4202 - Name: Oculocerebral Syndrome With Hypopigmentation - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000043183 - Term: Irritable Bowel Syndrome - ID: D000013577 - Term: Syndrome ### Intervention Browse Module - Browse Branches - Abbrev: Ot - Name: Other Dietary Supplements - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: T355 - Name: Acidophilus - Relevance: HIGH - As Found: Students ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422988 Brief Title: Do Probiotics Reduce The Risk Of Severe Necrotising Enterocolitis (NEC) In Infants Born Before 32 Weeks Gestation? Official Title: Do Probiotics Reduce The Risk Of Severe Necrotising Enterocolitis (NEC) In Infants Born Before 32 Weeks Gestation? An Observational Study Using Routinely Collected Data. #### Organization Study ID Info ID: IRAS323099 #### Organization Class: OTHER Full Name: Imperial College London ### Status Module #### Completion Date Date: 2024-12-30 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-18 Overall Status: ENROLLING_BY_INVITATION #### Primary Completion Date Date: 2024-07-30 Type: ESTIMATED #### Start Date Date: 2024-05-30 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-24 Study First Submit QC Date: 2024-05-18 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: University of Nottingham Class: OTHER Name: Newcastle University Class: OTHER Name: Queen Mary University of London #### Lead Sponsor Class: OTHER Name: Imperial College London #### Responsible Party Investigator Affiliation: Imperial College London Investigator Full Name: Cheryl Battersby Investigator Title: Clinical Senior Lecturer Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Necrotising enterocolitis (NEC) is one of the leading causes of mortality and morbidity in very preterm infants. This study aims to determine whether NEC rates are different between infants who receive probiotics versus infants who do not receive probiotics. The study has a retrospective cohort design and will utilise routinely collected data from the UK National Neonatal Research Database (NNRD). The cohort will comprise all infants born before 32 weeks gestation and cared for in neonatal units in England and Wales between 2016 and 2022. A propensity score matched approach will be used to conduct two comparisons: i) the risk of necrotising enterocolitis (NEC) between who do and those who do not receive probiotics in the first 14 days of life ii) the risk of NEC between babies who receive the two most common probiotic products used in UK units, (Labinic and Proprems). ### Conditions Module Conditions: - Enterocolitis, Necrotizing Keywords: - Probiotics ### Design Module #### Design Info Observational Model: COHORT Time Perspective: RETROSPECTIVE #### Enrollment Info Count: 48000 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Receipt of any probiotic in the first 14 days of life. Probiotics to include: Labinic, Proprems probiotic, Acidophillus, Bifidobacterium, Bio-kult, Infloran, LB2. To address potential recording error, infants whose NNRD records show minimal (one day) of probiotic exposure will only be classed as exposed if they are cared for in a probiotic unit. Probiotic units are defined as: * units who have confirmed that a guideline was in place to provide probiotics to infants born before 32 weeks gestation and that the guideline was in place at any point in the year that the infant was born OR * units where more than 50% of the infants eligible to be part of the cohort received probiotics in the six months after the infant was born. Intervention Names: - Dietary Supplement: Probiotics Label: Exposed to probiotics #### Arm Group 2 Description: Did not receive any probiotic in the first 14 days of life. Intervention Names: - Dietary Supplement: Probiotics Label: No probiotic exposure ### Interventions #### Intervention 1 Arm Group Labels: - Exposed to probiotics - No probiotic exposure Description: Any exposure to probiotics in first 14 days of life Name: Probiotics Other Names: - Labinic - Proprems - Acidophillus - Bifidobacterium - Bio-kult - Infloran - LB2 Type: DIETARY_SUPPLEMENT ### Outcomes Module #### Primary Outcomes Description: NEC confirmed at surgery or postmortem or listed as a cause of death Measure: Severe necrotising enterocolitis (NEC) Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months #### Secondary Outcomes Description: NEC diagnosed at postmortem or NEC diagnosed during surgery or NEC diagnosed using clinical and radiographic features (where the infant has at least one clinical feature (bilious gastric aspirate or emesis, abdominal distension, occult, gross blood in stool) and at least one radiographic feature (pneumatosis, hepato-biliary gas, pneumoperitoneum)). Measure: Necrotising enterocolitis (NNAP definition) Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: Infants who had a recorded diagnosis of necrotising enterocolitis and received at least 5 consecutive days of antibiotics whilst also nil by mouth Measure: Pragmatically defined NEC Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: HQIP NNAP case definition Measure: Late onset sepsis Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: Growth of any organisms that appear in the NNAP lists of "Clearly pathogenic organisms" and "Other organisms" Measure: Pragmatically defined late onset sepsis Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Measure: Survival to discharge home Time Frame: On date of discharge from final neonatal unit, assessed up to 24 months Description: LOS is defined according to the Healthcare Quality Improvement Partnership (HQIP) National Neonatal Audit Programme (NNAP) case definition i.e. blood stream or cerebrospinal fluid confirmed pure growth in culture after first three days of life Measure: Survival without severe NEC or late onset sepsis (LOS) Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: NEC is defined as per the NNAP definition Measure: Survival without any NEC Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: Either left or right grade 3 or higher intra-ventricular haemorrhage or cystic periventricular leukomalacia Measure: Brain injury Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: Defined as cryotherapy, laser therapy or injection of anti-vascular endothelial growth factor therapy for ROP in either or both eyes Measure: Treated retinopathy of prematurity Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Measure: Stage of retinopathy of prematurity Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: Defined as any respiratory or ventilatory support or supplemental oxygen at 36 weeks postmenstrual age Measure: Bronchopulmonary dysplasia Time Frame: 36 weeks postmenstrual age Description: Defined as ventilation via endotracheal tube or trachestomy, and excluding non-invasive support or CPAP, at 36 weeks postmenstrual age Measure: Severe bronchopulmonary dysplasia Time Frame: 36 weeks postmenstrual age Description: Number of days between first neonatal unit admission and final neonatal unit discharge for surviving infants Measure: Length of stay Time Frame: From date of birth until the date of discharge from final neonatal unit, assessed up to 24 months Description: Defined as the number of days until an infant is recorded as not requiring any parenteral nutrition or fluid (i.e. no parenteral nutrition or intravenous dextrose) Measure: Time to full feeds Time Frame: Before discharge from final neonatal unit Description: Weight for post-menstrual age standard deviation score Measure: Growth Time Frame: 36 weeks corrected gestational age ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Eligible infants must have been born at less than 32 weeks gestation and be cared for in a English or Welsh unit which contributes data to the National Neonatal Research Database (this includes all NHS neonatal units in England and Wales). * Infants born in the period January 1st, 2016, to December 31st, 2022 (7 years) will be included. Exclusion Criteria: * They have missing data for any of: gestational age at birth, birth weight, year of birth and date of death (for those that died). * Their NNRD record does not include details of their first admission or begins after Day 3 of life. * The absolute value of their recorded birthweight for gestational age z score exceeds 4 or is missing. * They die in the first two postnatal days of life. * They have a major congenital abnormality Maximum Age: 32 Weeks Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - CHILD Study Population: Infants born very preterm i.e. before 32 weeks gestation ### Contacts Locations Module #### Locations Location 1: City: London Country: United Kingdom Facility: Imperial College Zip: SW10 9NH ### IPD Sharing Statement Module Description: Study protocol available now. Analysis code will be available after publication of results. IPD Sharing: UNDECIDED ## Document Section ### Large Document Module #### Large Docs - Date: 2024-04-12 - Filename: Prot_SAP_000.pdf - Has ICF: False - Has Protocol: True - Has SAP: True - Label: Study Protocol and Statistical Analysis Plan - Size: 1459636 - Type Abbrev: Prot_SAP - Upload Date: 2024-04-23T05:17 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000005759 - Term: Gastroenteritis - ID: D000005767 - Term: Gastrointestinal Diseases - ID: D000004066 - Term: Digestive System Diseases - ID: D000007410 - Term: Intestinal Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: All - Name: All Conditions - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M7922 - Name: Enterocolitis - Relevance: HIGH - As Found: Enterocolitis - ID: M22151 - Name: Enterocolitis, Necrotizing - Relevance: HIGH - As Found: Enterocolitis, Necrotizing - ID: M8875 - Name: Gastroenteritis - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M10444 - Name: Intestinal Diseases - Relevance: LOW - As Found: Unknown - ID: T4055 - Name: Necrotizing Enterocolitis - Relevance: HIGH - As Found: Enterocolitis, Necrotizing ### Condition Browse Module - Meshes - ID: D000004760 - Term: Enterocolitis - ID: D000020345 - Term: Enterocolitis, Necrotizing ### Intervention Browse Module - Browse Branches - Abbrev: Ot - Name: Other Dietary Supplements - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: T367 - Name: Bifidobacterium - Relevance: HIGH - As Found: Neonates ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422975 Brief Title: Registry of Patients in Shock Treated With Vasopressin Official Title: Prospective Multicentre Observational Study of Patients Treated With Vasopressin in Critical Care Units #### Organization Study ID Info ID: VASOPRES REGISTRY #### Organization Class: OTHER Full Name: Hospital Universitario 12 de Octubre ### Status Module #### Completion Date Date: 2026-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-24 Type: ACTUAL Last Update Submit Date: 2024-05-23 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-06 Type: ESTIMATED #### Start Date Date: 2024-06 Type: ESTIMATED Status Verified Date: 2024-04 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-04-29 Study First Submit QC Date: 2024-05-17 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Hospital Universitario 12 de Octubre #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Is US Export: False Oversight Has DMC: False ### Description Module Brief Summary: Arginine-vasopressin (AVP) is a non-catecholaminergic hormone produced in the hypothalamus and released into the circulation via the neurohypophysis. It has different actions depending on the receptors through which it acts: V1 (vasoconstriction, platelet aggregation, efferent arteriole constriction of the renal glomerulus, glycogenolysis); V2 (water reabsorption, release of von Willebrand factor and factor VIII); V3 (increased cortisol and insulin). Septic shock is the most common cause of vasoplegic shock and its management includes control of the focus, early antibiotic therapy, volume resuscitation, vasopressor therapy, support of various organ dysfunctions, as well as monitoring and follow-up. The Surviving Sepsis Campaign (a global initiative to improve sepsis management) recommends noradrenaline as the first line of vasopressor therapy and early addition of AVP as a second line rather than further up-titration of noradrenaline when signs of hypoperfusion persist, through its action primarily on V1. The rationale for its use in septic shock would be: * endogenous vasopressin deficiency present in septic shock; * as a catecholamine-sparing strategy, reducing the side effects of catecholamines; * its potential nephroprotective effect; * its use should be early. The uncertainties surrounding the use of AVP in septic shock and other types of shock are many, hence the need for this registry. Detailed Description: The main objective is to characterise the routine clinical practice of vasopressin use in the context of shock in a multicentre observational study. By collecting clinical, analytical and echocardiographic data in a uniform manner, describing the time sequence of vasopressin and/or noradrenaline use; how long vasopressin is used; and which vasoconstrictor is more frequently withdrawn earlier: vasopressin or noradrenaline. The secondary objectives are: * to assess what motivated the decision to initiate AVP: type of shock, perfusion parameters, noradrenaline dose; * to define the impact of initiating AVP on noradrenaline dose (whether the dose can be reduced or not), on cardiac function (whether echocardiographic data improve or worsen) and on perfusion data (whether laboratory and clinical data such as lactate, capillary refill time, mottling score or diuresis improve or worsen); * estimate what is the dose range of AVP used and what is the maximum dose used in routine clinical practice; * observe when AVP is stopped, how (abruptly or progressively); * describe the incidence of side effects of AVP, whether it is related to the dose of AVP and the comorbidities of the patients; * assess medium/long-term outcomes: 28- and 90-day mortality, ICU and hospital stay, days of vasopressor support, days of mechanical ventilation, days of renal replacement. ### Conditions Module Conditions: - Vasopressin Causing Adverse Effects in Therapeutic Use - Shock - Vasopressor Adverse Reaction - Vasopressin Deficiency Keywords: - Vasopressin - Shock ### Design Module #### Design Info Observational Model: OTHER Time Perspective: PROSPECTIVE #### Enrollment Info Count: 500 Type: ESTIMATED Patient Registry: True Study Type: OBSERVATIONAL Target Duration: 90 Days ### Arms Interventions Module ### Interventions #### Intervention 1 Description: Patients treated with vasopressin Name: Vasopressin Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Describing the time sequence of vasopressin and/or noradrenaline use (what is initiated first) during shock Measure: Characterise the clinical practice of vasopressin use in the context of shock in a multicentre observational study. Time Frame: 90 days #### Secondary Outcomes Description: Assess what prompted the decision to initiate AVP: type of shock (vasoplegic, hypovolemic,...), perfusion parameters (as lactate) or noradrenaline dose (microgram/kg/minute) Measure: Assess what prompted the decision to initiate AVP Time Frame: Up to 7 days Description: Define the impact of starting AVP on noradrenaline dose (microgram/kg/minute) Measure: Define the impact of starting AVP on noradrenaline dose Time Frame: Up to 7 days Description: Define the impact of starting AVP on lactate level (mmol/L) Measure: Define the impact of starting AVP on lactate level Time Frame: Up to 7 days Description: Describe number of participants what AVP is discontinued first and how (abruptly or progressively) Measure: Observe when AVP is discontinued and how Time Frame: Up to 7 days Description: Estimate the range of doses of AVP used and the maximum dose used in routine clinical practice. Measure: Estimate the range of doses of AVP used Time Frame: Up to 7 days Description: Describe the incidence of side effects, whether it is related to AVP dose and patients' comorbidities. Measure: Incidence of side effects Time Frame: Up to 7 days Description: Death on or before study day 28 Measure: 28-day all-cause mortality Time Frame: 28 days Description: Death on or before study day 90 Measure: 90-day all-cause mortality Time Frame: 90 days Description: New receipt of renal replacement therapy after onset of shock Measure: Incidence of new renal replacement therapy Time Frame: From onset of shock until hospital discharge, an average of 2 weeks Description: Number of days between day 28 and the end of the last period of vasopressor therapy prior to day 28 Measure: Vasopressor-free days to day 28 Time Frame: 28 days Description: Number of days between day 28 and the end of the last period of intensive care unit admission prior to day 28. Measure: Intensive care unit-free days to day 28 Time Frame: 28 days Description: Number of days between day 28 and the end of the last period of hospital admission prior to day 28 Measure: Hospital-free days to day 28 Time Frame: 28 days ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Any patient over 18 years of age who is in shock and requires the administration of vasoconstrictors, to whom vasopressin is administered in the operating theatre and/or critical care unit, according to best clinical practice. Exclusion Criteria: * Non-consent by patient/legal representatives Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: Patients in shock receiving vasopressin ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Raquel García Álvarez, MD Phone: +34913908243 Role: CONTACT #### Locations Location 1: City: A Coruña Contacts: *Contact 1:* - Name: Pablo Rama Maceiras - Role: CONTACT Country: Spain Facility: Hospital Universitario de A Coruña Location 2: City: Baracaldo Contacts: *Contact 1:* - Name: Gontzal Tamayo - Role: CONTACT Country: Spain Facility: Hospital Universitario de Cruces Location 3: City: Barcelona Contacts: *Contact 1:* - Name: Marta Giné Servén - Role: CONTACT Country: Spain Facility: Hospital de Sant Pau Location 4: City: Barcelona Contacts: *Contact 1:* - Name: Ramón Adalia - Role: CONTACT Country: Spain Facility: Hospital del Mar Location 5: City: Barcelona Country: Spain Facility: Hospital Universitario Valle de Hebrón Location 6: City: Bilbao Contacts: *Contact 1:* - Name: Felipe Ortega Palacios - Role: CONTACT Country: Spain Facility: Hospital Universitario de Basurto Location 7: City: Donostia Contacts: *Contact 1:* - Name: Cristina García Fernández - Role: CONTACT Country: Spain Facility: Hospital de Donostia Location 8: City: Elche Contacts: *Contact 1:* - Name: Ana Pérez Carbonell - Role: CONTACT Country: Spain Facility: Hospital General Universitario de Elche Location 9: City: Gijón Country: Spain Facility: Hospital Universitario de Cabueñes Location 10: City: León Contacts: *Contact 1:* - Name: Rafael González de Castro - Role: CONTACT Country: Spain Facility: Complejo Asistencial Universitario de León Location 11: City: Lugo Contacts: *Contact 1:* - Name: Lorena Mouritz - Role: CONTACT Country: Spain Facility: Hospital Lucus Augustus Location 12: City: Madrid Contacts: *Contact 1:* - Name: Carlos Alberto Calvo García - Role: CONTACT Country: Spain Facility: Hospital General Universitario Gregorio Marañón Location 13: City: Madrid Contacts: *Contact 1:* - Email: [email protected] - Name: Raquel García Álvarez - Role: CONTACT Country: Spain Facility: Hospital Universitario 12 de Octubre Location 14: City: Madrid Contacts: *Contact 1:* - Name: Fernando Ramasco Rueda - Role: CONTACT *Contact 2:* - Name: Jesús Nieves Alonso - Role: CONTACT Country: Spain Facility: Hospital Universitario La Princesa Location 15: City: Madrid Country: Spain Facility: Hospital Universitario Ramón y Cajal Location 16: City: Majadahonda Contacts: *Contact 1:* - Name: Reyes Iranzo - Role: CONTACT Country: Spain Facility: Hospital Universitario Puerta de Hierro Majadahonda Location 17: City: Ourense Contacts: *Contact 1:* - Name: Concepción Alonso - Role: CONTACT Country: Spain Facility: Complexo Hospitalario Universitario de Ourense Location 18: City: Oviedo Contacts: *Contact 1:* - Name: Beatriz Mancha Getino - Role: CONTACT Country: Spain Facility: Hospital Universitario Central de Asturias Location 19: City: Santa Cruz De Tenerife Contacts: *Contact 1:* - Name: David Domínguez - Role: CONTACT Country: Spain Facility: Hospital Universitario Nuestra Señora de Candelaria Location 20: City: Santander Contacts: *Contact 1:* - Name: Adriana Ixquic Reyes Echeverria - Role: CONTACT Country: Spain Facility: Hospital Universitario Marqués de Valdecilla Location 21: City: Santiago De Compostela Contacts: *Contact 1:* - Name: Manuel Taboada - Role: CONTACT Country: Spain Facility: Hospital Clínico Universitario de Santiago Location 22: City: Tarragona Contacts: *Contact 1:* - Name: Diego Prendes Fernández - Role: CONTACT Country: Spain Facility: Hospital Universitario Joan XXIII Location 23: City: Valencia Contacts: *Contact 1:* - Name: Gerardo Aguilar - Role: CONTACT Country: Spain Facility: Hospital Clínico Universitario de Valencia Location 24: City: Valencia Contacts: *Contact 1:* - Name: Miguel Ángel Rodenas - Role: CONTACT Country: Spain Facility: Hospital Universitari i Politècnic La Fe #### Overall Officials Official 1: Affiliation: Hospital Universitario 12 de Octubre Name: Raquel García Álvarez Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ### References Module #### References Citation: Garcia-Alvarez R, Arboleda-Salazar R. Vasopressin in Sepsis and Other Shock States: State of the Art. J Pers Med. 2023 Oct 29;13(11):1548. doi: 10.3390/jpm13111548. PMID: 38003863 Citation: Treschan TA, Peters J. The vasopressin system: physiology and clinical strategies. Anesthesiology. 2006 Sep;105(3):599-612; quiz 639-40. doi: 10.1097/00000542-200609000-00026. PMID: 16931995 Citation: Dunser MW, Lindner KH, Wenzel V. A century of arginine vasopressin research leading to new therapeutic strategies. Anesthesiology. 2006 Sep;105(3):444-5. doi: 10.1097/00000542-200609000-00004. No abstract available. PMID: 16931974 Citation: Ramasco F, Nieves-Alonso J, Garcia-Villabona E, Vallejo C, Kattan E, Mendez R. Challenges in Septic Shock: From New Hemodynamics to Blood Purification Therapies. J Pers Med. 2024 Feb 3;14(2):176. doi: 10.3390/jpm14020176. PMID: 38392609 Citation: Evans L, Rhodes A, Alhazzani W, Antonelli M, Coopersmith CM, French C, Machado FR, Mcintyre L, Ostermann M, Prescott HC, Schorr C, Simpson S, Wiersinga WJ, Alshamsi F, Angus DC, Arabi Y, Azevedo L, Beale R, Beilman G, Belley-Cote E, Burry L, Cecconi M, Centofanti J, Coz Yataco A, De Waele J, Dellinger RP, Doi K, Du B, Estenssoro E, Ferrer R, Gomersall C, Hodgson C, Moller MH, Iwashyna T, Jacob S, Kleinpell R, Klompas M, Koh Y, Kumar A, Kwizera A, Lobo S, Masur H, McGloughlin S, Mehta S, Mehta Y, Mer M, Nunnally M, Oczkowski S, Osborn T, Papathanassoglou E, Perner A, Puskarich M, Roberts J, Schweickert W, Seckel M, Sevransky J, Sprung CL, Welte T, Zimmerman J, Levy M. Surviving sepsis campaign: international guidelines for management of sepsis and septic shock 2021. Intensive Care Med. 2021 Nov;47(11):1181-1247. doi: 10.1007/s00134-021-06506-y. Epub 2021 Oct 2. No abstract available. PMID: 34599691 Citation: Sharshar T, Blanchard A, Paillard M, Raphael JC, Gajdos P, Annane D. Circulating vasopressin levels in septic shock. Crit Care Med. 2003 Jun;31(6):1752-8. doi: 10.1097/01.CCM.0000063046.82359.4A. PMID: 12794416 Citation: Holmes CL, Patel BM, Russell JA, Walley KR. Physiology of vasopressin relevant to management of septic shock. Chest. 2001 Sep;120(3):989-1002. doi: 10.1378/chest.120.3.989. PMID: 11555538 Citation: Martin C, Medam S, Antonini F, Alingrin J, Haddam M, Hammad E, Meyssignac B, Vigne C, Zieleskiewicz L, Leone M. NOREPINEPHRINE: NOT TOO MUCH, TOO LONG. Shock. 2015 Oct;44(4):305-9. doi: 10.1097/SHK.0000000000000426. PMID: 26125087 Citation: Russell JA, Walley KR, Singer J, Gordon AC, Hebert PC, Cooper DJ, Holmes CL, Mehta S, Granton JT, Storms MM, Cook DJ, Presneill JJ, Ayers D; VASST Investigators. Vasopressin versus norepinephrine infusion in patients with septic shock. N Engl J Med. 2008 Feb 28;358(9):877-87. doi: 10.1056/NEJMoa067373. PMID: 18305265 Citation: Demiselle J, Fage N, Radermacher P, Asfar P. Vasopressin and its analogues in shock states: a review. Ann Intensive Care. 2020 Jan 22;10(1):9. doi: 10.1186/s13613-020-0628-2. PMID: 31970567 Citation: Gordon AC, Russell JA, Walley KR, Singer J, Ayers D, Storms MM, Holmes CL, Hebert PC, Cooper DJ, Mehta S, Granton JT, Cook DJ, Presneill JJ. The effects of vasopressin on acute kidney injury in septic shock. Intensive Care Med. 2010 Jan;36(1):83-91. doi: 10.1007/s00134-009-1687-x. Epub 2009 Oct 20. PMID: 19841897 Citation: Hamzaoui O, Goury A, Teboul JL. The Eight Unanswered and Answered Questions about the Use of Vasopressors in Septic Shock. J Clin Med. 2023 Jul 10;12(14):4589. doi: 10.3390/jcm12144589. PMID: 37510705 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000010335 - Term: Pathologic Processes - ID: D000003919 - Term: Diabetes Insipidus - ID: D000007674 - Term: Kidney Diseases - ID: D000014570 - Term: Urologic Diseases - ID: D000052776 - Term: Female Urogenital Diseases - ID: D000005261 - Term: Female Urogenital Diseases and Pregnancy Complications - ID: D000091642 - Term: Urogenital Diseases - ID: D000052801 - Term: Male Urogenital Diseases - ID: D000010900 - Term: Pituitary Diseases - ID: D000004700 - Term: Endocrine System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BXS - Name: Urinary Tract, Sexual Organs, and Pregnancy Conditions - Abbrev: BC19 - Name: Gland and Hormone Related Diseases - Abbrev: BC18 - Name: Nutritional and Metabolic Diseases - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M15577 - Name: Shock - Relevance: HIGH - As Found: Shock - ID: M22545 - Name: Diabetes Insipidus, Neurogenic - Relevance: HIGH - As Found: Vasopressin Deficiency - ID: M7115 - Name: Diabetes Mellitus - Relevance: LOW - As Found: Unknown - ID: M7114 - Name: Diabetes Insipidus - Relevance: LOW - As Found: Unknown - ID: M10698 - Name: Kidney Diseases - Relevance: LOW - As Found: Unknown - ID: M17319 - Name: Urologic Diseases - Relevance: LOW - As Found: Unknown - ID: M2875 - Name: Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M27093 - Name: Female Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M14127 - Name: Pregnancy Complications - Relevance: LOW - As Found: Unknown - ID: M8399 - Name: Female Urogenital Diseases and Pregnancy Complications - Relevance: LOW - As Found: Unknown - ID: M27095 - Name: Male Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M13791 - Name: Pituitary Diseases - Relevance: LOW - As Found: Unknown - ID: M7862 - Name: Endocrine System Diseases - Relevance: LOW - As Found: Unknown - ID: T1030 - Name: Central Diabetes Insipidus - Relevance: HIGH - As Found: Vasopressin Deficiency ### Condition Browse Module - Meshes - ID: D000020790 - Term: Diabetes Insipidus, Neurogenic - ID: D000012769 - Term: Shock ### Intervention Browse Module - Ancestors - ID: D000006490 - Term: Hemostatics - ID: D000003029 - Term: Coagulants - ID: D000014662 - Term: Vasoconstrictor Agents - ID: D000050034 - Term: Antidiuretic Agents - ID: D000045283 - Term: Natriuretic Agents - ID: D000045505 - Term: Physiological Effects of Drugs ### Intervention Browse Module - Browse Branches - Abbrev: NaAg - Name: Natriuretic Agents - Abbrev: VaCoAg - Name: Vasoconstrictor Agents - Abbrev: Coag - Name: Coagulants - Abbrev: All - Name: All Drugs and Chemicals - Abbrev: AA - Name: Amino Acids ### Intervention Browse Module - Browse Leaves - ID: M17414 - Name: Vasopressins - Relevance: HIGH - As Found: Contained - ID: M4437 - Name: Arginine Vasopressin - Relevance: HIGH - As Found: Contained - ID: M9576 - Name: Hemostatics - Relevance: LOW - As Found: Unknown - ID: M6259 - Name: Coagulants - Relevance: LOW - As Found: Unknown - ID: M17409 - Name: Vasoconstrictor Agents - Relevance: LOW - As Found: Unknown - ID: T1 - Name: Arginine - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000014667 - Term: Vasopressins - ID: D000001127 - Term: Arginine Vasopressin ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422962 Brief Title: [Trial of device that is not approved or cleared by the U.S. FDA] Official Title: [Trial of device that is not approved or cleared by the U.S. FDA] #### Organization Study ID Info ID: OTO-03 #### Organization Full Name: [Redacted] ### Status Module Delayed Posting: True #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: WITHHELD #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Name: [Redacted] #### Responsible Party Old Name Title: [Redacted] Old Organization: [Redacted] ## Derived Section ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422949 Brief Title: Efficacy and Safety of HILOTERM® Device for the Prevention of Peripheral Neuropathy Official Title: A Study on the Efficacy and Safety of HILOTERM® Device for the Prevention of Chemotherapy-induced Peripheral Neuropathy in Early Breast Cancer Patients #### Organization Study ID Info ID: IEO 1974 #### Organization Class: OTHER Full Name: European Institute of Oncology ### Status Module #### Completion Date Date: 2027-08-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-31 Type: ESTIMATED Last Update Submit Date: 2024-05-30 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2027-08-15 Type: ESTIMATED #### Start Date Date: 2024-06-15 Type: ESTIMATED Status Verified Date: 2024-04 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: European Institute of Oncology #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Taxol is a very effective drug in breast cancer, but it can cause peripheral neuropathy (PN). This toxicity is often dose-limiting. Symptoms of PN usually improve after taxol discontinuation, but \>80% of affected women experience symptoms 1-3 years after treatment stop. The intensity, the duration and the type of symptoms related to PN are very different and they can strongly interfere with patients' quality of life. The application of cold to the hands and feet seems to be able to reduce the incidence of PN. Hilotherm® is a machine that allows to cool hands and feet. The aim of this study is to verify whether the use of Hilotherm® is able to reduce the incidence of moderate and severe PN and to evaluate the tolerability of Hilotherm® and its impact on quality of life. Detailed Description: Taxol is a very effective drug in breast cancer, but it can cause peripheral neuropathy (PN), that is damage to the nerves of the hands and feet. This toxicity can begin a few days to months after starting taxol treatment and is often dose-limiting. Symptoms of chemotherapy-induced peripheral neuropathy (CIPN) usually improve after taxol discontinuation, but \>80% of affected women experience symptoms 1-3 years after treatment stop. The intensity, the duration and the type of symptoms related to PN are very different and they range from mild and transient symptoms to more severe and persistent symptoms. These symptoms can strongly interfere with patients' quality of life and can create difficulties in carrying out activities of daily living. Despite numerous pharmacological approaches, no substance has proven capable of counteracting the onset of PN in patients eligible to receive chemotherapy with taxol. Some clinical studies have shown that the application of cold to the hands and feet is able to reduce the incidence of PN because the cold-induced constriction of the vessels leads to a reduction of blood flow and consequently to a reduced inflow of drug at the level of the hands and feet. Hilotherm® is a machine that allows to keep hands and feet at a constant temperature of 10°C. The aim of this study is to verify whether the use of Hilotherm® is able to reduce the incidence of moderate and severe PN and to evaluate the tolerability of Hilotherm® and its impact on quality of life. ### Conditions Module Conditions: - Breast Cancer - Neuropathy;Peripheral Keywords: - Early stage breast cancer - Paclitaxel - Chemotherapy-induced peripheral neuropathy ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 120 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Cooling treatment with Hilotherm® at hands and feet level Intervention Names: - Device: Hilotherm® Cooling treatment Label: Hilotherm® Cooling treatment Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Hilotherm® Cooling treatment Description: Patient will receive cooling treatment with Hilotherm® at hands and feet level from half an hour before taxol treatment start until half an hour after treatment end Name: Hilotherm® Cooling treatment Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: Severity of PN evaluated using the CTCAE scale, version 5 Measure: Overall incidence of grade 2 or 3 CIPN Time Frame: 12 months #### Secondary Outcomes Description: Number of patients withdrawing Hilotherapy due to cold intolerance Measure: Incidence of withdrawal from Hilotherapy Time Frame: 12 weeks Description: Collection of EORTC QLQ-C30 \[European Organization for Research and Treatment of Cancer - Quality of Life Questionnaire\] (minimum value: 1, maximum value: 4 - higher scores mean a worse outcome) Measure: Patients' physical, psychological and social functions evaluation Time Frame: 12 months Description: Collection of EORTC-BR23 \[European Organization for Research and Treatment of Cancer - Breast Cancer specific Module\] (minimum value: 1, maximum value: 4 - higher scores mean a worse outcome) Measure: Side effects impact evaluation Time Frame: 12 months Description: Collection of Brief Pain Inventory (BPI) questionnaire (minimum value: 0, maximum value: 10 - higher scores mean a worse outcome) Measure: Pain assessment Time Frame: 12 months Description: Collection of Technology Acceptance Model Questionnaire (minimum value: 1, maximum value: 7 - higher scores mean a lower agreement with the statement) Measure: Technology acceptance and perception evaluation Time Frame: 12 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Women \> 18 years of age * Eastern Cooperative Oncology Group (ECOG) Performance Status 0-1 * Radically operated infiltrating breast cancer, pT1-T3, pN0-2, M0 * Candidate to adjuvant chemotherapy that includes weekly paclitaxel 80 mg/m2 intravenous for 12 weeks \[either following anthracyclines and/or in association with trastuzumab\] * Negative pregnancy test at baseline (in fertile women) * Willing and able to sign informed consent for protocol treatment Exclusion Criteria: * Evidence of metastatic disease (M1) * pT4 and/or pN3 * Previous or concomitant malignancy of any other type * Previous treatment with chemotherapy, hormonal therapy or an investigational drug for any type of malignancy * Plans to use a chemotherapy regimen other than those specified in the inclusion criteria * Any serious concurrent infection or any clinically significant medical illness (in particular clinically significant liver disease, clinically significant renal dysfunction, clinically significant cardiovascular disease, uncontrolled infections) which would jeopardize the ability of the patient to complete the planned therapy and follow-up * Pre-existing motor or sensory neuropathy of any grade, for any reason * Participation in any other clinical investigation or exposure to other investigational agents, drugs, device or procedure that may cause PN * History of Raynaud phenomenon, either primary or secondary to autoimmune or connective tissue diseases such as systemic lupus erythematous, scleroderma, Buerger disease, Sjögren syndrome, rheumatoid arthritis, occlusive vascular disease, such as atherosclerosis, polymyositis, cold agglutinin disease or cryoglobulinemia, thyroid disorders, pulmonary hypertension * Cold urticaria / cold contact urticaria * Severe arterial disease * Trophic tissue lesions * Diabetes mellitus * Alcohol abuse * History of severe allergic, anaphylactic, or other hypersensitivity reactions to the components of Hilotherm Chemo care device * Simultaneous use of Dignicap system to prevent hair loss from chemotherapy Minimum Age: 18 Years Sex: FEMALE Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Silvia Dellapasqua, MD Phone: +39 0257489970 Role: CONTACT #### Locations Location 1: City: Milan Contacts: *Contact 1:* - Email: [email protected] - Name: Silvia Dellapasqua, MD - Phone: +39 0257489970 - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Mara Negri - Phone: +39 0257489536 - Role: CONTACT Country: Italy Facility: European Institute of Oncology Zip: 20141 #### Overall Officials Official 1: Affiliation: European Istitute of Oncology Name: Silvia Dellapasqua, MD Role: PRINCIPAL_INVESTIGATOR ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009371 - Term: Neoplasms by Site - ID: D000009369 - Term: Neoplasms - ID: D000001941 - Term: Breast Diseases - ID: D000012871 - Term: Skin Diseases - ID: D000009468 - Term: Neuromuscular Diseases - ID: D000009422 - Term: Nervous System Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: BC17 - Name: Skin and Connective Tissue Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC10 - Name: Nervous System Diseases ### Condition Browse Module - Browse Leaves - ID: M5220 - Name: Breast Neoplasms - Relevance: HIGH - As Found: Breast Cancer - ID: M13432 - Name: Peripheral Nervous System Diseases - Relevance: HIGH - As Found: Peripheral Neuropathy - ID: M5218 - Name: Breast Diseases - Relevance: LOW - As Found: Unknown - ID: M15674 - Name: Skin Diseases - Relevance: LOW - As Found: Unknown - ID: M12411 - Name: Neuromuscular Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000001943 - Term: Breast Neoplasms - ID: D000010523 - Term: Peripheral Nervous System Diseases ### Intervention Browse Module - Browse Branches - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M19537 - Name: Paclitaxel - Relevance: LOW - As Found: Unknown - ID: M231 - Name: Albumin-Bound Paclitaxel - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422936 Acronym: SPOTLIGHT204 Brief Title: Clinical Trial to Evaluate BO-112 in Patients With Basal Cell Carcinoma (BCC) Official Title: SPOTLIGHT 204: A Multicenter, Phase 2b, Open-label, Non-randomized, Clinical Trial to Evaluate Safety, Tolerability and Preliminary Efficacy of Intra-lesional BO-112 in Patients With Resectable Primary Low and High Risk Basal Cell Carcinoma #### Organization Study ID Info ID: BOT-112-204 #### Organization Class: INDUSTRY Full Name: Highlight Therapeutics ### Status Module #### Completion Date Date: 2028-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-31 Type: ESTIMATED Last Update Submit Date: 2024-05-29 Overall Status: RECRUITING #### Primary Completion Date Date: 2026-06 Type: ESTIMATED #### Start Date Date: 2024-05-27 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-13 Study First Submit QC Date: 2024-05-16 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Highlight Therapeutics #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Oversight Has DMC: False ### Description Module Brief Summary: This is a multicenter, phase 2b, open-label, non-randomized, clinical trial to evaluate safety, tolerability, pharmacodynamics and preliminary efficacy of intra-lesional BO-112 in patients with resectable primary low and high risk basal cell carcinoma. * primary endpoint is complete visual and pathological response \[at surgery\] on patient level assessed by central review * secondary endpoints are 1. Occurrence of adverse events (AEs), serious adverse events (SAEs), and AEs leading to discontinuation or death on patient level. 2. Pathological response \[at surgery\] on patient level assessed by the investigator and central review, respectively, and visual response \[during the study and at surgery\] on patient level assessed by the investigator and central review, respectively. 3. Recurrence \[at 12 and 24 months\] after surgery on patient level assessed by the investigator. ### Conditions Module Conditions: - Basal Cell Carcinoma ### Design Module #### Design Info Allocation: NON_RANDOMIZED Intervention Model: PARALLEL Intervention Model Description: Parallel group design with same treatment and study procedures ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 60 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: patients with low risk nodular BCC Intervention Names: - Drug: BO-112 Label: Cohort I Type: EXPERIMENTAL #### Arm Group 2 Description: patients with high risk BCC Intervention Names: - Drug: BO-112 Label: Cohort II Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Cohort I - Cohort II Description: Noncoding double-stranded (ds) RNA based on polyinosinic-polycytidylic acid (Poly I:C), formulated with polyethylenimine (PEI) for intra-lesional injection Name: BO-112 Type: DRUG ### Outcomes Module #### Primary Outcomes Description: Complete visual and pathological response of all treated BCC lesions on participant level assessed by central review Measure: Number of Participants with Complete Visual and Pathological Response Time Frame: at 24 weeks #### Secondary Outcomes Description: Occurrence of adverse events (AEs), serious adverse events (SAEs), and AEs leading to discontinuation or death on participant level. Measure: Number of Participants with Treatment-Related Adverse Events assessed by CTCAE 5.0 Time Frame: through study completion, average 7 months Description: Pathological response on participant level assessed by the investigator and central review, respectively, using a 4-point scale 1. Pathologic Complete Response (pCR): No Residual Viable Tumor (RVT) 2. Major Pathologic Response (MPR)/ "near-pCR": \<= 10% RVT 3. Pathologic Partial Response (pPR): 10% \< RVT \<= 50% " 4. Pathologic Non-Response" (pNR): \>50% RVT Measure: Extent of Pathological Response Time Frame: at 24 weeks Description: Visual response \[during the study and at surgery\] on participant level assessed by the investigator and central review, respectively. Measure: Change of Visual Lesion Appearance Time Frame: at baseline and at 24 weeks Description: Recurrence after surgery on participant level assessed by the investigator Measure: Number of Participants with BCC Recurrence Time Frame: at 12 and 24 months after surgery ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Participant must be ≥ 18 years old \[or the legal age of consent in the jurisdiction in which the study is taking place\], at the time of signing the informed consent. Type of Participant and Disease Condition 2. Has primary resectable low or high risk basal cell carcinoma according to the protocol definition 3. Has diagnostic punch biopsy of all lesions intended for injection available prior to the first dose of BO-112. 4. Has adequate organ function defined as defined per protocol 5. Women of childbearing potential (WOCBP) must have a negative serum or urine pregnancy test (minimum sensitivity 25 IU/L or equivalent units of human chorionic gonadotropin \[HCG\]) within 24 hours prior to the start of study drug. 6. Women of childbearing potential must be willing to use two effective methods of birth control while treated with BO-112 and for 4 weeks after the last treatment. The two forms of birth control authorized are defined as the use of a barrier method of contraception (condom with spermicide) in association with one of the following methods of birth control: bilateral tubal ligation; combined oral contraceptives (estrogens and progesterone) or implanted or injectable contraceptives from the time of informed consent. 7. Male patients with female partners of childbearing potential must be willing to use two adequate contraception methods while treated with BO-112 and for 4 weeks after treatment completion. Informed Consent 8. Capable of giving signed informed consent as described in Appendix 1 which includes compliance with the requirements and restrictions listed in the informed consent form (ICF) and in this protocol. 9. Able and willing to comply with all study requirements, including surgical removal of lesion/lesion site at completion of study. Exclusion Criteria: 1. Has history of hypersensitivity to BO-112 or its excipients/vehicle. 2. Has any BCC lesion(s) in site of prior radiation and/or any BCC lesion(s) within 2 cm of the open eyelid margins 4. Has Gorlin's syndrome 5. Has clinically active or uncontrolled skin disease or tattoos that would interfere with evaluation of the area surrounding the target lesion 6. Has another malignant disease requiring treatment 7. Has a history of immunological disorder, severe allergic reaction, moderate or severe asthma or known history of anaphylaxis or any other serious adverse reactions to the investigational products. 8. Female participants: lactating or pregnant. 9. Has received a live vaccine or messenger ribonucleic acid (mRNA) Corona virus disease (COVID) vaccine within 7 days prior to the first dose of study drug or has a vaccination planned during treatment with BO-112 and within 7 days after the last study drug administration. 10. Is immunocompromised. Systemic corticosteroids at \>10 mg/day prednisone or equivalent within 1 week prior to the first dose of BO-112. 11. Has any prior systemic anti-lesion therapy or local treatment for study lesions prior to first dose; any chemotherapy or immunotherapy for any other malignancy within 24 months prior to the first dose of BO-112. 12. Has any experimental or investigational agents within one month of first BO-112 injection. 13. Has received or is expected to receive treatment with psoralen plus ultraviolet A (UVA) or ultraviolet B (UVB) therapy within 6 months prior to the first dose of BO-112. 14. Requires / or has used topical products within 5 cm of a treatment-targeted BCC lesion or systemic therapies that might interfere with the evaluation of the study medication during the study. 15. Has any other concurrent anti-cancer therapy (chemotherapy, immunotherapy, radiotherapy, or any ancillary therapy considered investigational \[used for a not approved indication and in the context of a research investigation\]) within 28 days of first study drug administration; or plans to participate in an experimental drug study while enrolled in this study. 16. Has any medical contraindications to surgery Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Marisol Quintero, PhD Phone: +34 682 544 814 Role: CONTACT Contact 2: Email: [email protected] Name: Zuzana Jirakova Trnkova, MD, PhD Phone: +34 682 544 814 Role: CONTACT #### Locations Location 1: City: Be'er Sheva Contacts: *Contact 1:* - Name: Adi Saadia, MD - Role: CONTACT Country: Israel Facility: Soroka Medical Center Status: RECRUITING Location 2: City: Haifa Contacts: *Contact 1:* - Name: Michal Ramon, MD - Role: CONTACT Country: Israel Facility: Rambam Medical Center Status: NOT_YET_RECRUITING Location 3: City: Jerusalem Contacts: *Contact 1:* - Name: Sharon Merims, MD - Role: CONTACT Country: Israel Facility: Hadassah Ein Kerem Medical Center Status: NOT_YET_RECRUITING Location 4: City: Tel Aviv Contacts: *Contact 1:* - Name: Gila Isman-Nelkenbaum, MD - Role: CONTACT Country: Israel Facility: Sourasky Medical Center Status: NOT_YET_RECRUITING ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009375 - Term: Neoplasms, Glandular and Epithelial - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000018295 - Term: Neoplasms, Basal Cell ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: All - Name: All Conditions ### Condition Browse Module - Browse Leaves - ID: M5534 - Name: Carcinoma - Relevance: HIGH - As Found: Carcinoma - ID: M5537 - Name: Carcinoma, Basal Cell - Relevance: HIGH - As Found: Basal Cell Carcinoma - ID: M12320 - Name: Neoplasms, Glandular and Epithelial - Relevance: LOW - As Found: Unknown - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M20439 - Name: Neoplasms, Basal Cell - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000002277 - Term: Carcinoma - ID: D000002280 - Term: Carcinoma, Basal Cell ### Intervention Browse Module - Browse Branches - Abbrev: Infe - Name: Anti-Infective Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M13957 - Name: Poly I-C - Relevance: LOW - As Found: Unknown ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422923 Brief Title: Effect of NRTX-1001, a Cellular Therapy Product, for the Treatment of Refractory Bilateral TLE Official Title: A Study of Inhibitory Interneurons (NRTX-1001) for the Treatment of Drug-resistant Bilateral Temporal Lobe Focal Seizures #### Organization Study ID Info ID: NTE002 #### Organization Class: INDUSTRY Full Name: Neurona Therapeutics ### Status Module #### Completion Date Date: 2040-07-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-31 Type: ESTIMATED Last Update Submit Date: 2024-05-29 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-07-15 Type: ESTIMATED #### Start Date Date: 2024-07-15 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Neurona Therapeutics #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Oversight Has DMC: True ### Description Module Brief Summary: This study is designed to obtain open-label feasibility, safety, and seizure frequency data in patients with drug-resistant bilateral mesial temporal lobe epilepsy (MTLE) administered NRTX-1001. Detailed Description: This is an open-label study of the bilateral intrahippocampal administration of NRTX1001, with the primary endpoint to evaluate safety and a secondary endpoint to evaluate seizure metrics. ### Conditions Module Conditions: - Epilepsy, Temporal Lobe Keywords: - Bilateral Temporal Lobe Epilepsy - Bilateral MTLE - Refractory Bilateral MTLE ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 10 Type: ESTIMATED Phases: - PHASE1 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: This is an open-label study of the bilateral intrahippocampal administration of NRTX-1001 in a single dose cohort of up to 10 subjects. Subjects will be temporarily immunosuppressed after surgery. Intervention Names: - Biological: NRTX-1001 Label: Treatment Arm Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Treatment Arm Description: Cellular therapy consisting of GABAergic Inhibitory Interneurons Name: NRTX-1001 Type: BIOLOGICAL ### Outcomes Module #### Primary Outcomes Description: Safety Measure: Incidence of Serious Adverse Events at end of month 12 Time Frame: 12 months after treatment #### Secondary Outcomes Description: Seizure frequency change during months 7-12, compared to frequency of clinical seizures in the 6-month baseline period. Measure: Change in frequency of clinical seizures Time Frame: 12 months after treatment ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Male or female, age 18-75 years. 2. Subjects of childbearing potential will use highly effective contraception (defined as documented failure rate ≤1%) while taking immunosuppressants. For females using enzyme-inducing anti-seizure medications (EI-ASM), hormonal contraception will not be considered as effective (EI-ASM determined from US Prescribing Information). 3. Proven history of focal seizures of hippocampal origin with bilateral seizure foci confirmed by scalp or intracranial ictal EEG (including confirmation by recordings from responsive neurostimulation \[RNS\] electrodes when applicable). 4. Either 1. bilateral hippocampal sclerosis on MRI (evidenced by increased FLAIR signal intensity in both hippocampi or by visual assessment showing reduced volume compared to normal) or 2. bilateral temporal hypometabolism on 18-Flourodeoxyglucose Positron Emission Tomography (FDG PET) (assessed by visual assessment, comparing temporal regions to frontal/parietal lobe neocortex). In this case, ictal EEG recordings must also include intracranial confirmation. or 3. a combination of unilateral instances of the evidence described in a. and b. (e.g., one side can be evidenced by criterion a. and the other side by criterion b.) MRI or PET scans used for assessment must have been acquired within 3 years of screening. 5. For subjects with unilateral RNS, the contralateral side must meet one of the descriptions listed in inclusion criterion 4. 6. For subjects with RNS, the electrodes are in (or near) hippocampi and have been in place for ≥12 months prior to screening. 7. For subjects with RNS, the RNS device is MRI-conditional (RNS Neurostimulator model 320). Subjects with RNS® Neurostimulator, model RNS-300 devices are not eligible. Patients with other RNS model devices may be eligible depending on confirmation of MRI compatibility. 8. For subjects with RNS, RNS system batteries are not expected to need replacement during year 1 of this trial. 9. For subjects with RNS, settings for ES detection and stimulation have not changed in the past 6 months and should be held constant over the first 2 years after NRTX-1001 administration. 10. Subject has maintained a diary (written or electronic) recording clinical seizure frequency for at least 1 month prior to surgery. 11. Subject has had at least four clinical focal seizures, including at least two clinical focal seizures with objective manifestations, on average, per month for the 6 months prior to screening. 12. Subject has previously had adequate (in opinion of investigator) therapeutic trials of at least two Anti-Seizure Medicines (ASMs). 13. Current ASM regimen, and doses of other drugs known to affect seizure frequency (e.g., antidepressants), have been stable for at least three months prior to enrollment. 14. Subject has received Shingrix vaccine (first dose by at least 7 days prior to start of immunosuppression). 15. Subject can converse and read in English or Spanish. Able to participate in required study procedures and provide signed informed consent. 16. Subject has either 10th grade education or equivalent or full-scale intelligence quotient (IQ) ≥70, assessed either within 1 year of screening, or during the screening period. 17. Subject can comply with study visits \& procedures (may have caregiver assist). Exclusion Criteria: 1. Evidence of seizure focus outside hippocampus (either by seizure semiology or EEG findings). 2. MRI indicating potential malignant lesion (low-grade glioma of any type is excluded) in any location or non-malignant potentially epileptogenic lesion outside the hippocampus. Small (\<2 cm) non invasive meningioma, remote from the affected temporal lobe, is not exclusionary. 3. Seizures of non-focal origin. 4. History of status epilepticus in the year prior to screening, as guided by ILAE criteria (Trinka 2015) in the judgement of the PI. A history of cluster seizures is permitted. 5. Clinical diagnosis of autoimmune epilepsy, supported by the presence of serum antibodies detected on a standard test panel (Labcorp Autoimmune Epilepsy Evaluation Profile test 505490, or Mayo Clinic Laboratories Epilepsy, Autoimmune/Paraneoplastic Evaluation test EPS2, or similar with approval from Sponsor), either within 3 years of screening or during the baseline period. 6. Psychogenic Non-Epileptic Seizures (PNES) within the past 3 years. 7. Severe psychiatric disorders. 8. Primary or secondary immunodeficiency. 9. Evidence of active cytomegalovirus (CMV) or Epstein-Barr virus (EBV) infection (symptomatic or asymptomatic as demonstrated by positive plasma polymerase chain reaction \[PCR\] or plasma Nucleic Acid Amplification Test \[NAAT\] and immunoglobulin M \[IgM\] tests). Subjects may re-screen after infection is resolved. 10. Substance use disorder (including alcohol) per the Diagnostic and Statistical Manual of Mental Illnesses (DSM-5) criteria. 11. Planned surgery within one year of enrollment. 12. Current pregnancy, or lactation. 13. Prior exposure to NRTX-1001 product, or other cell or gene therapy treatments (of any kind). 14. Participation in another investigational trial within past 30 days, excepting non-interventional studies. 15. Detection of clinically relevant donor-specific allo-HLA reactive antibodies. Maximum Age: 75 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Holly Finefrock, BSHS Phone: 650-436-3045 Role: CONTACT Contact 2: Email: [email protected] Name: Sheri Madrid, BS, BA Phone: 949-500-0027 Role: CONTACT #### Overall Officials Official 1: Affiliation: Neurona Therapeutics Name: John Hixson, MD Role: STUDY_DIRECTOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001927 - Term: Brain Diseases - ID: D000002493 - Term: Central Nervous System Diseases - ID: D000009422 - Term: Nervous System Diseases - ID: D000004828 - Term: Epilepsies, Partial - ID: D000073376 - Term: Epileptic Syndromes ### Condition Browse Module - Browse Branches - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M7983 - Name: Epilepsy - Relevance: HIGH - As Found: Epilepsy - ID: M7989 - Name: Epilepsy, Temporal Lobe - Relevance: HIGH - As Found: Epilepsy, Temporal Lobe - ID: M15452 - Name: Seizures - Relevance: LOW - As Found: Unknown - ID: M5204 - Name: Brain Diseases - Relevance: LOW - As Found: Unknown - ID: M5742 - Name: Central Nervous System Diseases - Relevance: LOW - As Found: Unknown - ID: M7984 - Name: Epilepsies, Partial - Relevance: LOW - As Found: Unknown - ID: M16355 - Name: Syndrome - Relevance: LOW - As Found: Unknown - ID: M1165 - Name: Epileptic Syndromes - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000004827 - Term: Epilepsy - ID: D000004833 - Term: Epilepsy, Temporal Lobe ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422910 Brief Title: Video Exercise Mobile Application for People With Knee Osteoarthritis Official Title: Development and Investigation of the Effectiveness of Video Exercise Mobile Application for People With Knee Osteoarthritis #### Organization Study ID Info ID: Tubitak diz OA #### Organization Class: OTHER Full Name: Muğla Sıtkı Koçman University ### Status Module #### Completion Date Date: 2024-05-15 Type: ACTUAL #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: COMPLETED #### Primary Completion Date Date: 2024-04-30 Type: ACTUAL #### Start Date Date: 2023-05-02 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Collaborators Class: OTHER Name: The Scientific and Technological Research Council of Turkey #### Lead Sponsor Class: OTHER Name: Fatih Ozden #### Responsible Party Investigator Affiliation: Muğla Sıtkı Koçman University Investigator Full Name: Fatih Ozden Investigator Title: Assistant Professor Type: SPONSOR_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: The aim of our study is to realize an exercise training and follow-up system that individuals with knee OA can easily adapt. ### Conditions Module Conditions: - Telerehabilitation - Osteoarthritis, Knee ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 52 Type: ACTUAL Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Other: Telerehabilitation Label: Intervention Group Type: EXPERIMENTAL #### Arm Group 2 Intervention Names: - Other: Telerehabilitation Label: Control Group Type: ACTIVE_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - Control Group - Intervention Group Description: Home exercises will be delivered through a video mobile application. In this application, exercises for knee osteoarthritis will be presented according to their types (stretching, strengthening, etc.). Videos deemed appropriate by the physiotherapist will be added to the exercise prescription and sent to the patients via message. Patients will have the opportunity to remotely access their own exercise prescription with visual, auditory and written commands. Translated with DeepL.com (free version) Name: Telerehabilitation Type: OTHER ### Outcomes Module #### Primary Outcomes Description: On a 0 cm straight line or numeric scale, the patient is asked to mark the pain they feel (0: no pain, 10: excruciating pain). Measure: Visual Analog Scale (VAS) Time Frame: Change from Baseline VAS at 8 weeks Description: WOMAC consists of 3 main headings: pain intensity, stiffness and physical function. The total score ranges from 0 (no disability) to 96 (complete disability). Measure: The Western Ontario and McMaster Universities Osteoarthritis Index (WOMAC) Time Frame: Change from Baseline WOMAC at 8 weeks Description: On a 0 cm straight line or numeric scale, the patient will be asked to mark their pre-treatment expectation and post-treatment satisfaction level. 0 will represent the lowest expectation and satisfaction and 10 the highest expectation or satisfaction. Measure: Satisfaction and expectation assessment Time Frame: Change from Baseline Satisfaction and expectation assessment at 8 weeks ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Diagnosis of primary knee osteoarthritis (OA) according to the American College of Rheumatology (ACR) criteria * Be qualified to use the mobile application and agree to use the application Exclusion Criteria: * Individuals with poor cognitive function or inadequate reading skills * Individuals with neurological disorders that may affect mobility skills * Individuals who have undergone knee joint surgery and individuals with traumatic injuries Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Locations Location 1: City: Muğla Country: Turkey Facility: Fethiye State Hospital State: Fethiye #### Overall Officials Official 1: Affiliation: Muğla Sıtkı Koçman University Name: Fatih Özden, PhD Role: STUDY_CHAIR Official 2: Affiliation: Muğla Sıtkı Koçman University Name: Baki Umut Tuğay, PhD Role: STUDY_DIRECTOR Official 3: Affiliation: Muğla Sıtkı Koçman University Name: Barış Ethem Süzek, PhD Role: PRINCIPAL_INVESTIGATOR Official 4: Affiliation: Sanko University Name: Nazan Tuğay, PhD Role: PRINCIPAL_INVESTIGATOR Official 5: Affiliation: Marmara University Name: Zübeyir Sarı, PhD Role: PRINCIPAL_INVESTIGATOR Official 6: Affiliation: Haliç University Name: İrem Çetinkaya, MSc Role: PRINCIPAL_INVESTIGATOR Official 7: Affiliation: İstanbul Medeniyet University Name: Gülser Cinbaz, MSc Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000001168 - Term: Arthritis - ID: D000007592 - Term: Joint Diseases - ID: D000009140 - Term: Musculoskeletal Diseases - ID: D000012216 - Term: Rheumatic Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC05 - Name: Musculoskeletal Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC17 - Name: Skin and Connective Tissue Diseases ### Condition Browse Module - Browse Leaves - ID: M12926 - Name: Osteoarthritis - Relevance: HIGH - As Found: Osteoarthritis - ID: M22168 - Name: Osteoarthritis, Knee - Relevance: HIGH - As Found: Osteoarthritis, Knee - ID: M4476 - Name: Arthritis - Relevance: LOW - As Found: Unknown - ID: M10621 - Name: Joint Diseases - Relevance: LOW - As Found: Unknown - ID: M12097 - Name: Musculoskeletal Diseases - Relevance: LOW - As Found: Unknown - ID: M15045 - Name: Rheumatic Diseases - Relevance: LOW - As Found: Unknown - ID: M6323 - Name: Collagen Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000010003 - Term: Osteoarthritis - ID: D000020370 - Term: Osteoarthritis, Knee ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422897 Acronym: OCT Brief Title: Role of AS-OCT in Assessment of Corneal Perforation Official Title: Role of Anterior Segment Optical Coherence Tomography in Assessment of Healing of Thin or Perforated Cornea Treated by Amniotic Membrane Graft and Platelet Rich Plasma Clot #### Organization Study ID Info ID: 1133/04/2024 #### Organization Class: OTHER Full Name: Minia University ### Status Module #### Completion Date Date: 2024-06-05 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: RECRUITING #### Primary Completion Date Date: 2024-05-30 Type: ESTIMATED #### Start Date Date: 2024-04-15 Type: ACTUAL Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Minia University #### Responsible Party Investigator Affiliation: Minia University Investigator Full Name: Ahemd Abdelghany Investigator Title: Associate professor Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: False ### Description Module Brief Summary: Assessment of healing of thin and perforated cornea after surgical treatment by anterior segment optical coherence tomography Detailed Description: * thin and perforated cornea (small perforation) is surgically treated by amniotic membrane graft and platelet rich plasma clot * anterior segment optical coherence tomography is performed preoperative and 1 month postoperative to assess healing ### Conditions Module Conditions: - Corneal Perforation ### Design Module #### Design Info Observational Model: CASE_ONLY Time Perspective: PROSPECTIVE #### Enrollment Info Count: 15 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: cases are assessed by Anterior segment optical coherence tomography 1 month after surgical managemnt Intervention Names: - Other: anterior segment optical coherence tomography Label: cases after surgical management ### Interventions #### Intervention 1 Arm Group Labels: - cases after surgical management Description: surgically treated corneal perforation by amniotic membrane graft and platelet rich plasma clot is assessed by anterior segment optical coherence tomography 1 month postoperative Name: anterior segment optical coherence tomography Type: OTHER ### Outcomes Module #### Primary Outcomes Description: complete corneal healing Measure: healing Time Frame: 1 month ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * thin cornea about to perforate * small corneal perforation Exclusion Criteria: * active infection Maximum Age: 80 Years Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: patients from both sexes was thin cornea or small corneal perforation surgically treated by amniotic membrane graft and platelet rich plasma clot ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Ahmed A Abdelghany, professor Phone: 00201020009630 Role: CONTACT #### Locations Location 1: City: Minya Contacts: *Contact 1:* - Name: Ahmed Abdelghany, Ass prof - Role: CONTACT Country: Egypt Facility: Faculty of Medicine Status: RECRUITING #### Overall Officials Official 1: Affiliation: professor Name: Ahmed A Abdelghany, professor Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: UNDECIDED ### References Module #### References Citation: Abdelghany AA, Bahrawy ME, Alio JL. Combined Platelet Rich Plasma and Amniotic membrane in the treatment of Perforated Corneal Ulcers. Eur J Ophthalmol. 2022 Jul;32(4):2148-2152. doi: 10.1177/11206721211049100. Epub 2021 Oct 8. PMID: 34623187 ## Derived Section ### Condition Browse Module - Ancestors - ID: D000065306 - Term: Corneal Injuries - ID: D000005131 - Term: Eye Injuries - ID: D000005151 - Term: Facial Injuries - ID: D000006259 - Term: Craniocerebral Trauma - ID: D000020196 - Term: Trauma, Nervous System - ID: D000009422 - Term: Nervous System Diseases - ID: D000003316 - Term: Corneal Diseases - ID: D000005128 - Term: Eye Diseases - ID: D000014947 - Term: Wounds and Injuries ### Condition Browse Module - Browse Branches - Abbrev: BC10 - Name: Nervous System Diseases - Abbrev: BC11 - Name: Eye Diseases - Abbrev: BC26 - Name: Wounds and Injuries - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology ### Condition Browse Module - Browse Leaves - ID: M28724 - Name: Corneal Perforation - Relevance: HIGH - As Found: Corneal Perforation - ID: M6539 - Name: Corneal Diseases - Relevance: LOW - As Found: Unknown - ID: M30499 - Name: Corneal Injuries - Relevance: LOW - As Found: Unknown - ID: M8274 - Name: Eye Injuries - Relevance: LOW - As Found: Unknown - ID: M21089 - Name: Facies - Relevance: LOW - As Found: Unknown - ID: M8294 - Name: Facial Injuries - Relevance: LOW - As Found: Unknown - ID: M17685 - Name: Wounds and Injuries - Relevance: LOW - As Found: Unknown - ID: M9349 - Name: Craniocerebral Trauma - Relevance: LOW - As Found: Unknown - ID: M22023 - Name: Trauma, Nervous System - Relevance: LOW - As Found: Unknown - ID: M8271 - Name: Eye Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000057112 - Term: Corneal Perforation ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422884 Brief Title: A Phase 2 Trial of ENV-101 in Patients With Lung Fibrosis (WHISTLE-PF Trial) Official Title: A Phase 2, Multi-Center, Randomized, Double-Blind, Controlled Trial Evaluating the Safety and Efficacy of ENV-101 in Patients With Lung Fibrosis (WHISTLE-PF Trial) #### Organization Study ID Info ID: ENV-IPF-103 #### Organization Class: INDUSTRY Full Name: Endeavor Biomedicines, Inc. ### Status Module #### Completion Date Date: 2026-06 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2026-06 Type: ESTIMATED #### Start Date Date: 2024-09 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Endeavor Biomedicines, Inc. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: True Is US Export: True Oversight Has DMC: True ### Description Module Brief Summary: The goal of this clinical trial is to evaluate the impact that ENV-101 has on lung function and key measures of fibrosis in adult patients with idiopathic pulmonary fibrosis (IPF) and progressive pulmonary fibrosis (PPF). Another goal of this study is to better understand the safety and tolerability of ENV-101 in these patient populations. Detailed Description: This trial is a 6-month, randomized, double-blind, controlled, dose-ranging trial of ENV-101 in two parallel cohorts of adult patients with lung fibrosis: idiopathic pulmonary fibrosis (IPF) and progressive pulmonary fibrosis (PPF). Patients are allowed to continue treatment with approved standard of care (e.g., nintedanib, pirfenidone) during the trial. Patients will be randomized to one of 3 dose levels of ENV-101 or placebo at baseline. The objectives of this trial are to characterize the efficacy, antifibrotic activity, and safety of ENV-101 to select the Phase 3 dose of ENV-101 in each indication. ### Conditions Module Conditions: - Idiopathic Pulmonary Fibrosis - Progressive Pulmonary Fibrosis - Progressive Fibrosing Interstitial Lung Disease ### Design Module #### Design Info Allocation: RANDOMIZED Intervention Model: PARALLEL ##### Masking Info Masking: TRIPLE Who Masked: - PARTICIPANT - INVESTIGATOR - OUTCOMES_ASSESSOR Primary Purpose: TREATMENT #### Enrollment Info Count: 320 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Drug: ENV-101 Label: ENV-101 Low Dose (IPF Population) Type: EXPERIMENTAL #### Arm Group 2 Intervention Names: - Drug: ENV-101 Label: ENV-101 Mid Dose (IPF Population) Type: EXPERIMENTAL #### Arm Group 3 Intervention Names: - Drug: ENV-101 Label: ENV-101 High Dose (IPF Population) Type: EXPERIMENTAL #### Arm Group 4 Intervention Names: - Drug: Placebo Label: Placebo (IPF Population) Type: PLACEBO_COMPARATOR #### Arm Group 5 Intervention Names: - Drug: ENV-101 Label: ENV-101 Low Dose (PPF Population) Type: EXPERIMENTAL #### Arm Group 6 Intervention Names: - Drug: ENV-101 Label: ENV-101 Mid Dose (PPF Population) Type: EXPERIMENTAL #### Arm Group 7 Intervention Names: - Drug: ENV-101 Label: ENV-101 High Dose (PPF Population) Type: EXPERIMENTAL #### Arm Group 8 Intervention Names: - Drug: Placebo Label: Placebo (PPF Population) Type: PLACEBO_COMPARATOR ### Interventions #### Intervention 1 Arm Group Labels: - ENV-101 High Dose (IPF Population) - ENV-101 High Dose (PPF Population) - ENV-101 Low Dose (IPF Population) - ENV-101 Low Dose (PPF Population) - ENV-101 Mid Dose (IPF Population) - ENV-101 Mid Dose (PPF Population) Description: oral tablet, dosed once a day Name: ENV-101 Other Names: - taladegib Type: DRUG #### Intervention 2 Arm Group Labels: - Placebo (IPF Population) - Placebo (PPF Population) Description: oral tablet, dosed once a day Name: Placebo Type: DRUG ### Outcomes Module #### Primary Outcomes Description: ppFVC is a measure of lung function Measure: IPF Population Primary Endpoint: Rate of change in percent predicted forced vital capacity (ppFVC) compared to placebo Time Frame: Baseline and Week 24 Description: The incidence, severity, and relationship of treatment-emergent adverse events (TEAEs), and treatment-emergent and clinically significant changes in lab parameters, vital signs, electrocardiogram (ECG), and oxygen saturation Measure: PPF Population Primary Endpoint: Safety Time Frame: Baseline and Week 24 #### Secondary Outcomes Measure: PPF Population: Rate of change in ppFVC compared to placebo Time Frame: Baseline and Week 24 Description: FVC is a measure of lung function Measure: Absolute change in FVC (mL) compared to placebo Time Frame: Baseline and Week 24 Measure: Time to disease progression (absolute decline in ppFVC >10%, IPF-related hospitalization, or death) compared to placebo Time Frame: Baseline and Week 24 Description: The L-PF Symptoms Questionnaire Cough domain consists of 6 questions regarding a subject's experience with cough over the prior 24 hours. Questions have response options on a five-point numeric rating scale with an anchor of 0 ("Not at all") to 4 ("Extremely"). Total score for the Cough domain is normalized to the range 0 to 100, with higher scores indicating greater impairment. Measure: Absolute change in the Living with Pulmonary Fibrosis Symptoms (L-PF Symptoms) Questionnaire Cough domain score compared to placebo Time Frame: Baseline and Week 24 Description: The L-PF Symptoms Questionnaire Dyspnea domain consists of 12 questions regarding a subject's experience with dyspnea (shortness of breath) over the prior 24 hours. Questions have response options on a five-point numeric rating scale with an anchor of 0 ("Not at all") to 4 ("Extremely"). Total score for the Dyspnea domain is normalized to the range 0 to 100, with higher scores indicating greater impairment. Measure: Absolute change in the L-PF Symptoms Questionnaire Dyspnea domain score compared to placebo Time Frame: Baseline and Week 24 Description: The L-PF Symptoms Questionnaire Fatigue domain consists of 5 questions regarding a subject's experience with fatigue over the prior 24 hours. Questions have response options on a five-point numeric rating scale with an anchor of 0 ("Not at all") to 4 ("Extremely"). Total score for the Fatigue domain is normalized to the range 0 to 100, with higher scores indicating greater impairment. Measure: Absolute change in the L-PF Symptoms Questionnaire Fatigue domain score compared to placebo Time Frame: Baseline and Week 24 Description: HRCT is a method of imaging which is more precise than chest x-ray in the diagnosis and monitoring of diseases of the lung tissue and the airways. Measure: Absolute change in total lung capacity (TLC) by chest high-resolution computed tomography (HRCT) imaging compared to placebo Time Frame: Baseline and Week 24 Measure: Absolute change in % quantitative interstitial lung disease (QILD) by chest HRCT imaging compared to placebo compared to placebo Time Frame: Baseline and Week 24 Measure: Absolute change in % quantitative ground glass opacity (QGG) by chest HRCT imaging compared to placebo Time Frame: Baseline and Week 24 Measure: Absolute change in % quantitative lung fibrosis (QLF) by chest HRCT imaging compared to placebo Time Frame: Baseline and Week 24 ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * IPF Population: Patients ≥ 40 years old with an IPF diagnosis as confirmed by the Investigator. * PPF Population: Patients ≥ 18 years old (or the minimum legal adult age, whichever is greater) with a diagnosis of PPF, as confirmed by the Investigator. * Percent predicted FVC of ≥ 45% at study start. * Percent predicted diffusing capacity of lung for carbon monoxide (DLCO) ≥ 25%, adjusted for hemoglobin (Hgb) at study start. * Ability to perform spirometry tests. * Either stable treatment with standard of care (SoC) \[i.e., antifibrotics, immunosuppressants (PPF only)\] for at least 3 months prior to study start or not treated with SoC for at least 8 weeks prior to study start. Exclusion Criteria: * IPF Population: Evidence of other known causes of interstitial lung disease (ILD) * Forced expiratory volume in one second (FEV1)/FVC ratio \<0.7 at study start. * History of malignancy, including carcinoma during the preceding 5 years from study start, with the following exceptions: 1. Prior history of in situ melanoma, basal or squamous cell skin cancer if treated with curative therapy. 2. Patients with prostate cancer that are managed by surveillance. 3. Patients with ductal carcinoma in situ, treated surgically with curative intent. * Patients with moderate to severe hepatic impairment (Child-Pugh B and C). * Smoking (including vaping) within 6 months of study start; current smoker, or unwillingness to refrain from smoking during the clinical trial duration. * Active or suspected alcohol or drug abuse in the opinion of the Investigator. * Currently enrolled in another investigational device or drug trial, or less than 3 months from study start since ending another investigational device or drug trial(s) or receiving other investigational treatment(s). * Presence of active infection at study start or confirmed active human immunodeficiency virus (HIV), Hepatitis B virus (HBV) or Hepatitis C virus (HCV). * Major surgery requiring hospitalization (according to the Investigator) performed within 3 months prior to study start or planned during the course of the trial. Being on a transplant list is allowed. * Occurrence of serious illness requiring hospitalization within 90 days prior to study start. * Current or previous use (within 28 days prior to study start) of the following: 1. Endothelin receptor antagonist 2. Riociguat 3. Prostacyclin or prostacyclin analogue 4. Radiation to the lungs 5. Oral corticosteroids \>15 mg/day * Use of cyclophosphamide or tocilizumab within 8 weeks, or rituximab within 6 months, prior to study start. * Use of drugs that are known moderate or stronger CYP3A4 inhibitors or inducers within 14 days prior to study start. Patients must also agree not to eat fruits that inhibit CYP3A4 such as grapefruit, Seville oranges, pomelo and star fruit. * Patients of reproductive potential who are sexually active and unwilling to use birth control for the duration of the study and for 3 months after their final dose of study drug. * Females that are pregnant or nursing. * Patients that are unwilling to refrain from blood or blood product donation for the duration of the study and for 30 days after their final dose of study drug. * Males who are unwilling to refrain from sperm donation and females who are unwilling to refrain from egg donation for the duration of the study and for 3 months after their final dose of study drug. * Patients with a history of a severe allergic reaction or anaphylactic reaction or known hypersensitivity to any component of ENV-101. * Patients who have previously taken ENV-101. Sex: ALL Standard Ages: - CHILD - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Endeavor Clinical Trials Phone: 1-858-727-3199 Role: CONTACT #### Locations Location 1: City: Birmingham Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Alabama Zip: 35233 Location 2: City: Phoenix Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Arizona Zip: 85013 Location 3: City: Gainesville Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Florida Zip: 32608 Location 4: City: Maywood Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Illinois Zip: 60153 Location 5: City: Kansas City Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Kansas Zip: 66160 Location 6: City: Ann Arbor Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Michigan Zip: 48109 Location 7: City: Royal Oak Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Michigan Zip: 48073 Location 8: City: Portland Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Studies - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Oregon Zip: 97220 Location 9: City: Philadelphia Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Pennsylvania Zip: 19107 Location 10: City: Philadelphia Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Pennsylvania Zip: 19140 Location 11: City: Dallas Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Texas Zip: 75246 Location 12: City: San Antonio Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 858-727-3199 - Role: CONTACT Country: United States Facility: Research Site State: Texas Zip: 78229 Location 13: City: South Brisbane Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Australia Facility: Research Site State: Queensland Zip: 4101 Location 14: City: Adelaide Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Australia Facility: Research Site State: South Australia Zip: 5000 Location 15: City: Box Hill Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Australia Facility: Research Site State: Victoria Zip: 3128 Location 16: City: Melbourne Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Australia Facility: Research Site State: Victoria Zip: 3004 Location 17: City: Nedlands Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Australia Facility: Research Site State: Western Australia Zip: 6009 Location 18: City: Vienna Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Austria Facility: Research Site Zip: 1090 Location 19: City: Vancouver Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Canada Facility: Research Site State: British Columbia Zip: V6Z 2K5 Location 20: City: Sherbrooke Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Canada Facility: Research Site State: Quebec Zip: J1H 5N4 Location 21: City: Munich Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Germany Facility: Research Site Zip: 81377 Location 22: City: Dublin Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Ireland Facility: Research Site Zip: D04 T6F4 Location 23: City: Ulsan Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Korea, Republic of Facility: Research Site State: (Dong District) Zip: 44033 Location 24: City: Seoul Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Korea, Republic of Facility: Research Site State: (Gangnam District) Zip: 135-710 Location 25: City: Busan Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Korea, Republic of Facility: Research Site State: (Haeundae District) Location 26: City: Seoul Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Korea, Republic of Facility: Research Site State: (Seongbuk District) Zip: 02841 Location 27: City: Seoul Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Korea, Republic of Facility: Research Site State: (Songpa District) Zip: 05505 Location 28: City: Seoul Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Korea, Republic of Facility: Research Site State: (Yongsan District) Zip: 04401 Location 29: City: Kuala Lumpur Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Malaysia Facility: Research Site Zip: 50590 Location 30: City: Selayang Baru Utara Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Malaysia Facility: Research Site Location 31: City: Monterrey Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site State: Nuevo Leon Zip: 64060 Location 32: City: Monterrey Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site State: Nuevo Leon Zip: 64718 Location 33: City: San Nicolás De Los Garza Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site State: Nuevo Leon Zip: 66465 Location 34: City: San Juan Del Río Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site State: Queretaro Zip: 76800 Location 35: City: Chihuahua Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site Zip: 31203 Location 36: City: Mexico City Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site Zip: 14080 Location 37: City: Oaxaca Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site Zip: 68000 Location 38: City: Puebla Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Mexico Facility: Research Site Zip: 72180 Location 39: City: Bern Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: Switzerland Facility: Research Site Zip: 3010 Location 40: City: Edinburgh Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: United Kingdom Facility: Research Site Zip: EH1 3EG Location 41: City: Exeter Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: United Kingdom Facility: Research Site Zip: EX2 5DW Location 42: City: London Contacts: *Contact 1:* - Email: [email protected] - Name: Endeavor Clinical Trials - Phone: 1-858-727-3199 - Role: CONTACT Country: United Kingdom Facility: Research Site Zip: SW3 6NP #### Overall Officials Official 1: Affiliation: Endeavor Biomedicines Name: Paul Frohna, M.D., Ph.D., Pharm.D. Role: STUDY_DIRECTOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000010335 - Term: Pathologic Processes - ID: D000012140 - Term: Respiratory Tract Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC08 - Name: Respiratory Tract (Lung and Bronchial) Diseases - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M11168 - Name: Lung Diseases - Relevance: HIGH - As Found: Lung Disease - ID: M8485 - Name: Fibrosis - Relevance: HIGH - As Found: Fibrosis - ID: M14512 - Name: Pulmonary Fibrosis - Relevance: HIGH - As Found: Pulmonary Fibrosis - ID: M27989 - Name: Idiopathic Pulmonary Fibrosis - Relevance: HIGH - As Found: Idiopathic Pulmonary Fibrosis - ID: M19813 - Name: Lung Diseases, Interstitial - Relevance: HIGH - As Found: Interstitial Lung Disease - ID: M14977 - Name: Respiratory Tract Diseases - Relevance: LOW - As Found: Unknown - ID: T3003 - Name: Idiopathic Pulmonary Fibrosis - Relevance: HIGH - As Found: Idiopathic Pulmonary Fibrosis ### Condition Browse Module - Meshes - ID: D000008171 - Term: Lung Diseases - ID: D000011658 - Term: Pulmonary Fibrosis - ID: D000054990 - Term: Idiopathic Pulmonary Fibrosis - ID: D000017563 - Term: Lung Diseases, Interstitial - ID: D000005355 - Term: Fibrosis ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422871 Acronym: PReSeRVE-HD Brief Title: Observational Study of the Merit HeRO® Graft and Super HeRO® in Patients on Hemodialysis Official Title: PReSeRVE-HD: PRospective, Multicenter, Observational Study of the Merit HeRO® Graft and Super HeRO® EValuated in End-Stage Renal Disease Patients on HemoDialysis #### Organization Study ID Info ID: CVO-P4-23-02 #### Organization Class: INDUSTRY Full Name: Merit Medical Systems, Inc. ### Status Module #### Completion Date Date: 2028-07-15 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2027-01-15 Type: ESTIMATED #### Start Date Date: 2025-02-15 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: Merit Medical Systems, Inc. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: True Is FDA Regulated Drug: False Is US Export: True Oversight Has DMC: False ### Description Module Brief Summary: The goal of this observational study is to increase the understanding of the safety and performance of Merit Medical's HeRO Graft System (HeRO) and Super HeRO Adaptor and Support Seal System (Super HeRO) devices. This study includes adults that are being treated with one of these devices as part of their regular medical care for maintaining long-term dialysis access when all other dialysis access options have failed. Patients in the study will return to their study center 4 times over 2 years for follow-up visits to check their current health and dialysis status. ### Conditions Module Conditions: - End Stage Renal Disease - Hemodialysis Access Failure ### Design Module #### Design Info Observational Model: COHORT Time Perspective: PROSPECTIVE #### Enrollment Info Count: 175 Type: ESTIMATED Study Type: OBSERVATIONAL ### Arms Interventions Module #### Arm Group 1 Description: Subjects who meet all inclusion criteria and none of the exclusion criteria and treatment is attempted with the HeRO® Graft or Super HeRO® device. Intervention Names: - Device: HeRO® Graft System or Super HeRO® System Label: HeRO® / Super HeRO® ### Interventions #### Intervention 1 Arm Group Labels: - HeRO® / Super HeRO® Description: Treatment attempted with the HeRO® or Super HeRO® device. Name: HeRO® Graft System or Super HeRO® System Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: Proportion of subjects with cumulative patency Measure: Effectiveness Endpoint Time Frame: 6 months Description: Proportion of subjects with device-related infection-free survival Measure: Safety Endpoint Time Frame: 6 months #### Secondary Outcomes Measure: Proportion of subjects with primary patency Time Frame: 12 and 24 months Measure: Proportion of subjects with cumulative patency Time Frame: 12 and 24 months Measure: Device-related safety events Time Frame: 24 months ### Eligibility Module Eligibility Criteria: Key Inclusion Criteria: * Subject provides written informed consent * Subject is ≥ 18 years * Subject is end-stage renal disease patient on hemodialysis. * Subject is treated with HeRO Graft or Super HeRO System in accordance with device instructions for use (IFU) Key Exclusion Criteria: * Subject has a previously placed HeRO or Super HeRO device that is undergoing revision or replacement * Subject has a topical or subcutaneous infection associated with the implantation site * Subject has known or suspected systemic infection, bacteremia or septicemia Minimum Age: 18 Years Sampling Method: NON_PROBABILITY_SAMPLE Sex: ALL Standard Ages: - ADULT - OLDER_ADULT Study Population: End-stage renal disease patients on hemodialysis who have exhausted all other access options. ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: PReSeRVE-HD Clinical Affairs Team Phone: 978-758-6166 Role: CONTACT #### Overall Officials Official 1: Affiliation: Baylor Scott and White Health Name: Stephen Hohmann, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000014570 - Term: Urologic Diseases - ID: D000052776 - Term: Female Urogenital Diseases - ID: D000005261 - Term: Female Urogenital Diseases and Pregnancy Complications - ID: D000091642 - Term: Urogenital Diseases - ID: D000052801 - Term: Male Urogenital Diseases - ID: D000051436 - Term: Renal Insufficiency, Chronic - ID: D000051437 - Term: Renal Insufficiency - ID: D000002908 - Term: Chronic Disease - ID: D000020969 - Term: Disease Attributes - ID: D000010335 - Term: Pathologic Processes ### Condition Browse Module - Browse Branches - Abbrev: BXS - Name: Urinary Tract, Sexual Organs, and Pregnancy Conditions - Abbrev: All - Name: All Conditions - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M10698 - Name: Kidney Diseases - Relevance: HIGH - As Found: Renal Disease - ID: M10699 - Name: Kidney Failure, Chronic - Relevance: HIGH - As Found: End Stage Renal Disease - ID: M26718 - Name: Renal Insufficiency - Relevance: LOW - As Found: Unknown - ID: M17319 - Name: Urologic Diseases - Relevance: LOW - As Found: Unknown - ID: M2875 - Name: Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M27093 - Name: Female Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M14127 - Name: Pregnancy Complications - Relevance: LOW - As Found: Unknown - ID: M8399 - Name: Female Urogenital Diseases and Pregnancy Complications - Relevance: LOW - As Found: Unknown - ID: M27095 - Name: Male Urogenital Diseases - Relevance: LOW - As Found: Unknown - ID: M26717 - Name: Renal Insufficiency, Chronic - Relevance: LOW - As Found: Unknown - ID: M6147 - Name: Chronic Disease - Relevance: LOW - As Found: Unknown - ID: M22700 - Name: Disease Attributes - Relevance: LOW - As Found: Unknown - ID: T1303 - Name: Chronic Graft Versus Host Disease - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000007674 - Term: Kidney Diseases - ID: D000007676 - Term: Kidney Failure, Chronic ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422858 Acronym: Stars Brief Title: Sequential Tegafur-gimeracil-oteracil Potassium Capsule (s-1) and Serplulimab Following Concurrent Chemoradiotherapy for Esophageal Squamous Cell Carcinoma Official Title: Sequential Tegafur-gimeracil-oteracil Potassium Capsule (s-1) and Serplulimab Following Concurrent Chemoradiotherapy in the Treatment of Locally Advanced Inoperable Esophageal Squamous Cell Carcinoma: A Single-Arm Phase II Clinical Trial #### Organization Study ID Info ID: STARS-CCRT-ESCC #### Organization Class: OTHER Full Name: Zhejiang Cancer Hospital ### Status Module #### Completion Date Date: 2026-04 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-20 Overall Status: RECRUITING #### Primary Completion Date Date: 2025-04 Type: ESTIMATED #### Start Date Date: 2024-05 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-09 Study First Submit QC Date: 2024-05-20 ### Sponsor Collaborators Module #### Lead Sponsor Class: OTHER Name: Zhejiang Cancer Hospital #### Responsible Party Investigator Affiliation: Zhejiang Cancer Hospital Investigator Full Name: Ji Yongling Investigator Title: Dr Type: PRINCIPAL_INVESTIGATOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False Oversight Has DMC: True ### Description Module Brief Summary: This Phase II trial evaluates the efficacy and safety of Serplulimab combined with S1 chemotherapy in patients with inoperable, locally advanced esophageal squamous cell carcinoma after concurrent chemoradiation. The primary endpoint is the one-year progression-free survival rate. Secondary measures include clinical response rates, overall survival, duration of response, and safety profiles. Exploratory goals focus on the potential of biomarkers like PD-L1 and ctDNA to predict treatment outcomes. Treatment involves initial chemoradiation followed by consolidation with Serplulimab and S1, continuing for up to 12 months or until disease progression or unacceptable toxicity. Detailed Description: Detailed Description: This single-arm, Phase II study is designed to assess the efficacy and safety of the combination of Serplulimab (an anti-PD-1 antibody) and S1 (an oral fluoropyrimidine derivative) in patients with locally advanced, inoperable esophageal squamous cell carcinoma (ESCC), following concurrent chemoradiation therapy. Study Treatment Regimen: Patients enrolled in the study will first undergo concurrent chemoradiation, which includes a total radiation dose of 50.4 Gy delivered in 28 fractions over six weeks. Radiation will be administered using modern techniques such as image-guided radiation therapy (IGRT), intensity-modulated radiation therapy (IMRT), volumetric modulated arc therapy (VMAT), or helical tomotherapy (TOMO), ensuring precise targeting of the tumor and surrounding lymph nodes. Concurrent chemotherapy consists of cisplatin (75 mg/m2 on day 1) and S1 (60 mg/m2 per day, given in two divided doses from day 1 to day 14, repeated every 28 days). Following chemoradiation, patients will receive consolidation therapy with Serplulimab administered at a fixed dose of 300 mg every three weeks via intravenous infusion, alongside S1 (60 mg/m2 per day, on days 1-14 of a 21-day cycle). This consolidation phase will continue for up to 12 months or 17 cycles, unless there is disease progression, patient withdrawal, onset of unacceptable toxicity, or initiation of new anti-cancer treatment. ### Conditions Module Conditions: - Locally Advanced Inoperable Esophageal Squamous Cell Carcinoma ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: PREVENTION #### Enrollment Info Count: 37 Type: ESTIMATED Phases: - PHASE2 Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Intervention Names: - Drug: Serplulimab - Drug: Tegafur-gimeracil-oteracil potassium capsule(S1) - Radiation: Radiotherapy - Drug: Cisplatin Label: Serplulimab and S1 Chemotherapy Post-Concurrent Chemoradiation Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Serplulimab and S1 Chemotherapy Post-Concurrent Chemoradiation Description: Serplulimab will be administered as a fixed dose of 300 mg via intravenous infusion every three weeks, continuing for up to 12 months or until disease progression, unacceptable toxicity, or withdrawal of consent Name: Serplulimab Type: DRUG #### Intervention 2 Arm Group Labels: - Serplulimab and S1 Chemotherapy Post-Concurrent Chemoradiation Description: S1 will be administered at a dose of 60 mg/m2 per day, taken orally in two divided doses on day 1 concurrent with radiotherapy, repeated every 28 days; and from day 1 to day 14 of each 21-day cycle, for up to 12 months or until disease progression, unacceptable toxicity, or withdrawal of consent Name: Tegafur-gimeracil-oteracil potassium capsule(S1) Type: DRUG #### Intervention 3 Arm Group Labels: - Serplulimab and S1 Chemotherapy Post-Concurrent Chemoradiation Description: Radiotherapy will be delivered as a total dose of 50.4 Gy in 28 fractions over six weeks using techniques such as IGRT, IMRT, VMAT, or TOMO, targeting the primary tumor and associated lymph nodes Name: Radiotherapy Type: RADIATION #### Intervention 4 Arm Group Labels: - Serplulimab and S1 Chemotherapy Post-Concurrent Chemoradiation Description: Cisplatin will be administered at a dose of 75 mg/m\^2 on day 1 concurrent with radiotherapy, repeated every 28 days Name: Cisplatin Type: DRUG ### Outcomes Module #### Other Outcomes Description: The study will implement a pre-specified safety threshold where if the incidence of Grade 3 pneumonia, as categorized by the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE), exceeds 15% of participants, the trial may be modified or halted to assess and mitigate risks to patient safety. Measure: Grade 3 Pneumonia Incidence [Safety and Tolerability] Time Frame: through study completion, an average of 1 year #### Primary Outcomes Description: The primary outcome measure is the proportion of participants who are alive and free from disease progression at one year after initiating treatment. Progression is defined according to RECIST v1.1 criteria as a 20% increase in the sum of diameters of target lesions, the appearance of new lesions, or the worsening of non-target disease Measure: One-Year Progression-Free Survival (PFS) Time Frame: 1 year #### Secondary Outcomes Description: The rate of participants achieving a clinical complete response assessed by RECIST v1.1 criteria. A clinical complete response is defined as the disappearance of all target lesions and normalization of tumor marker levels. Measure: Incidence of Clinical Complete Response Rate (cCR) at 3 months after treatment initiation Time Frame: Assessed at 3 months after treatment initiation Description: Overall survival is defined as the time from the start of treatment to the date of death from any cause. If a patient is not known to have died, survival time will be censored at the date of the last known follow-up. Measure: Overall Survival (OS) Time Frame: From the start of treatment up to 3 years Description: Duration of response is measured from the time measurement criteria are first met for Complete Response or Partial Response (whichever is first recorded) until the first date that recurrent or progressive disease is objectively documented. Measure: Duration of Response (DoR) Time Frame: From the first documented response up to 2 years Description: The incidence and severity of adverse events categorized by the National Cancer Institute Common Terminology Criteria for Adverse Events (NCI CTCAE) version 5.0. Measure: Incidence of Treatment-Emergent Adverse Events Time Frame: Throughout the study, estimated at 12 months Description: Qualitasured using validated instruments such as the European Organization for Research and Treatment of Cancer Quality of Life Questionnaire (EORTC-QLQ-C30). The quality of life score is calculated based on the rules set by EORTC (range 0-100). A lower score indicates better quality of life on the symptom scales, while a higher score indicates better quality of life scores on the overall health and functional scales. Measure: EORTC-QoL-C30 Score(Quality of Life) Time Frame: At baseline, 6 months, and 12 months ### Eligibility Module Eligibility Criteria: Inclusion Criteria: * Able to understand and voluntarily sign a written informed consent form, which must be signed before initiating any study-specific procedures. * Male or female participants aged between 18 and 70 years at the time of informed consent. * Eastern Cooperative Oncology Group (ECOG) performance status of 0-1. Histologically or cytologically confirmed diagnosis of locally advanced esophageal squamous cell carcinoma (ESCC); or patients who refuse surgery; staged as T1-4bN1-3M0 (according to AJCC 8th edition). * Medically inoperable or refusal of surgery. * No prior anti-tumor treatment. * Expected survival of at least 6 months. * At least one measurable lesion as defined by RECIST v1.1. * Participants must provide either archived (within the last 2 years) or freshly obtained tumor tissue samples, with at least three unstained FFPE pathology slides. * Adequate organ function defined as follows: a. Hematology (no blood transfusions or growth factor support within 7 days before starting study treatment): i. Absolute Neutrophil Count (ANC) ≥1.5×10\^9/L (1500/mm³); ii. Platelet count ≥100×10\^9/L (100000/mm³); iii. Hemoglobin ≥90 g/L. b. Renal: i. Calculated creatinine clearance (CrCl) ≥50 mL/min using the Cockcroft-Gault formula: CrCl (mL/min) = {(140-age) × weight (kg) × F} / (SCr (mg/dL) × 72), where F=1 for males and 0.85 for females; SCr=serum creatinine. ii. Urinary protein \<2+ or 24-hour urinary protein quantification \<1.0 g. c. Liver: i. Total bilirubin (TBiL) ≤1.5×ULN; ii. AST and ALT ≤2.5×ULN (≤5×ULN for participants with liver metastases); iii. Serum albumin (ALB) ≥28 g/L. d. Coagulation: International Normalized Ratio (INR) and Activated Partial Thromboplastin Time (APTT) ≤1.5×ULN, unless the participant is receiving anticoagulant therapy and INR and APTT are within the expected range of their therapeutic use. e. Cardiac: Left Ventricular Ejection Fraction (LVEF) ≥50%. * Female participants of childbearing potential must have a negative urine or serum pregnancy test within 3 days prior to the first dose of study medication. If urine test is not conclusive, a serum test will be administered. If sexually active with a non-sterilized male partner, the participant must agree to use effective contraception during the study and for 120 days after the last dose of study medication. Discussion with the researcher is required regarding cessation of contraception after this point. * Male participants with female partners of childbearing potential must agree to use effective contraception from screening to 120 days after the last dose of study medication. Discussion with the researcher is required regarding cessation of contraception after this point. * Willing and able to comply with scheduled visits, treatment plans, laboratory tests, and other study procedures. Exclusion Criteria: * Previous anti-tumor treatment (including chemotherapy, radiation therapy, surgery, or immunotherapy). * Initial diagnosis with metastases to vital organs such as the liver, bones, lungs, brain, adrenal glands, etc. (stage IVb esophageal cancer). * History of thoracic radiotherapy. * Presence of an esophageal mediastinal fistula and/or esophageal tracheal fistula before treatment. * Known or suspected allergy to any component of S1, serplulimab, or cisplatin. * Pregnant or breastfeeding women. * Inability to provide informed consent due to psychological, familial, or social reasons. * History of any malignancy other than esophageal cancer within the past 5 years, except for adequately treated non-melanoma skin cancer, in-situ cervical cancer, or cured early-stage prostate cancer. * Unable to tolerate chemoradiation due to severe cardiac, pulmonary, hepatic, renal dysfunctions, hematological diseases, or cachexia. * Active autoimmune diseases, history of autoimmune diseases (including but not limited to colitis, hepatitis, hyperthyroidism, or syndromes), history of immunodeficiency (including positive HIV test), or other acquired or congenital immunodeficiency diseases, history of organ transplant or allogeneic bone marrow transplant. * Active hepatitis B (HBV DNA ≥ 2000IU/mL or 10×10\^4 copies/mL), positive hepatitis C antibody with elevated HCV RNA levels above the lower limit of detection. History of immunodeficiency; positive HIV antibody; current long-term use of systemic corticosteroids or other immunosuppressants. * Serious infection within 4 weeks before the first administration of study medication, including but not limited to complications requiring hospitalization, sepsis, or severe pneumonia; active infection requiring systemic anti-infective treatment within 2 weeks before the first dose (excluding antiviral treatment for hepatitis B or C). Known active tuberculosis (TB), suspected active TB requiring clinical exclusion; known active syphilis infection. * Vaccination with live or attenuated live vaccines within 30 days before the first dose of study medication or planning to receive such vaccines during the study period; inactivated vaccines are permitted. * History of interstitial lung disease or non-infectious pneumonia. * History of myocarditis, cardiomyopathy, malignant arrhythmias, unstable angina, myocardial infarction within the past 12 months, congestive heart failure as determined by NYHA Class II or higher, or vascular diseases such as aortic aneurysm at risk of rupture, or other cardiac damage that could compromise the safety evaluation of the study medication (such as poorly controlled arrhythmia or myocardial ischemia). * Known history of mental illness, drug abuse, alcoholism, or drug addiction. * Non-malignant systemic diseases or symptoms secondary to tumors that could pose a higher medical risk or confound the assessment of survival, such as leukemic reaction (white cell count \>20×10\^9/L) or cachexia manifestations (known weight loss exceeding 10% in the 3 months prior to screening). * Any condition that, in the opinion of the investigator, might pose a risk to the participant, interfere with the evaluation of the study medication, or confound the interpretation of study results. Maximum Age: 70 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Jin Wang, Dr Phone: 86-571-88122564 Role: CONTACT #### Locations Location 1: City: Hangzhou Contacts: *Contact 1:* - Email: [email protected] - Name: Jin Wang, MD - Phone: 0086-571-88122088 - Role: CONTACT *Contact 2:* - Email: [email protected] - Name: Yongling JI, MD - Phone: 0086-571-88122088 - Role: CONTACT *Contact 3:* - Name: Yongling JI, MD - Role: PRINCIPAL_INVESTIGATOR Country: China Facility: Zhejiang Cancer Hospital State: Zhejiang Status: RECRUITING Zip: 310022 #### Overall Officials Official 1: Affiliation: Zhejiang Cancer Hospital Name: Yongling Ji Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000009375 - Term: Neoplasms, Glandular and Epithelial - ID: D000009370 - Term: Neoplasms by Histologic Type - ID: D000009369 - Term: Neoplasms - ID: D000018307 - Term: Neoplasms, Squamous Cell - ID: D000004938 - Term: Esophageal Neoplasms - ID: D000005770 - Term: Gastrointestinal Neoplasms - ID: D000004067 - Term: Digestive System Neoplasms - ID: D000009371 - Term: Neoplasms by Site - ID: D000006258 - Term: Head and Neck Neoplasms - ID: D000004066 - Term: Digestive System Diseases - ID: D000004935 - Term: Esophageal Diseases - ID: D000005767 - Term: Gastrointestinal Diseases ### Condition Browse Module - Browse Branches - Abbrev: BC04 - Name: Neoplasms - Abbrev: All - Name: All Conditions - Abbrev: BC06 - Name: Digestive System Diseases - Abbrev: Rare - Name: Rare Diseases ### Condition Browse Module - Browse Leaves - ID: M5534 - Name: Carcinoma - Relevance: HIGH - As Found: Carcinoma - ID: M5550 - Name: Carcinoma, Squamous Cell - Relevance: HIGH - As Found: Squamous Cell Carcinoma - ID: M1733 - Name: Esophageal Squamous Cell Carcinoma - Relevance: HIGH - As Found: Esophageal Squamous Cell Carcinoma - ID: M12320 - Name: Neoplasms, Glandular and Epithelial - Relevance: LOW - As Found: Unknown - ID: M12315 - Name: Neoplasms by Histologic Type - Relevance: LOW - As Found: Unknown - ID: M20451 - Name: Neoplasms, Squamous Cell - Relevance: LOW - As Found: Unknown - ID: M8088 - Name: Esophageal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8886 - Name: Gastrointestinal Neoplasms - Relevance: LOW - As Found: Unknown - ID: M7256 - Name: Digestive System Neoplasms - Relevance: LOW - As Found: Unknown - ID: M9348 - Name: Head and Neck Neoplasms - Relevance: LOW - As Found: Unknown - ID: M8883 - Name: Gastrointestinal Diseases - Relevance: LOW - As Found: Unknown - ID: M7255 - Name: Digestive System Diseases - Relevance: LOW - As Found: Unknown - ID: M8085 - Name: Esophageal Diseases - Relevance: LOW - As Found: Unknown - ID: T2141 - Name: Esophageal Cancer - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000002277 - Term: Carcinoma - ID: D000002294 - Term: Carcinoma, Squamous Cell - ID: D000077277 - Term: Esophageal Squamous Cell Carcinoma ### Intervention Browse Module - Ancestors - ID: D000000970 - Term: Antineoplastic Agents - ID: D000000964 - Term: Antimetabolites, Antineoplastic - ID: D000000963 - Term: Antimetabolites - ID: D000045504 - Term: Molecular Mechanisms of Pharmacological Action ### Intervention Browse Module - Browse Branches - Abbrev: ANeo - Name: Antineoplastic Agents - Abbrev: All - Name: All Drugs and Chemicals ### Intervention Browse Module - Browse Leaves - ID: M8760 - Name: Tegafur - Relevance: HIGH - As Found: Carrier - ID: M6182 - Name: Cisplatin - Relevance: LOW - As Found: Unknown - ID: M4281 - Name: Antimetabolites - Relevance: LOW - As Found: Unknown ### Intervention Browse Module - Meshes - ID: D000005641 - Term: Tegafur ### Misc Info Module - Version Holder: 2024-05-31
## Protocol Section ### Identification Module NCT ID: NCT06422845 Acronym: SCDB Brief Title: Peripheral Scoring Drug-coated Balloon in the Treatment of Hemodialysis Arteriovenous Fistula Stenosis Official Title: A Prospective, Multicenter, Single-Arm Target Value Clinical Study to Evaluate the Safety and Effectiveness of Peripheral Scoring Drug-coated Balloon Dilation Catheter in the Treatment of Hemodialysis Arteriovenous Fistula Stenosis #### Organization Study ID Info ID: VP-P-24-012 #### Organization Class: INDUSTRY Full Name: DK Medical Technology (Suzhou) Co., Ltd. ### Status Module #### Completion Date Date: 2027-07 Type: ESTIMATED #### Expanded Access Info #### Last Update Post Date Date: 2024-05-21 Type: ACTUAL Last Update Submit Date: 2024-05-15 Overall Status: NOT_YET_RECRUITING #### Primary Completion Date Date: 2027-07 Type: ESTIMATED #### Start Date Date: 2024-06 Type: ESTIMATED Status Verified Date: 2024-05 #### Study First Post Date Date: 2024-05-21 Type: ACTUAL Study First Submit Date: 2024-05-15 Study First Submit QC Date: 2024-05-15 ### Sponsor Collaborators Module #### Lead Sponsor Class: INDUSTRY Name: DK Medical Technology (Suzhou) Co., Ltd. #### Responsible Party Type: SPONSOR ### Oversight Module Is FDA Regulated Device: False Is FDA Regulated Drug: False ### Description Module Brief Summary: This is a prospective, multi-center, single-arm target value clinical study to study the safety and effectiveness of Peripheral Scoring Drug-coated Balloon dilatation catheters in the treatment of hemodialysis arteriovenous fistula stenosis. Detailed Description: This is a prospective, multi-center, single-arm target value clinical study to study the safety and effectiveness of Peripheral Scoring Drug-coated Balloon dilatation catheters (SDCB) in the treatment of hemodialysis arteriovenous fistula stenosis. A total of 328 participants will be enrolled across multiple clinical trial sites. Participants will undergo a surgical procedure using a peripheral scoring drug-coated balloon dilation catheter, with follow-up within 5 days, at 1 month, and 6 months after the procedure, then at 12, 18, and 24 months post-procedure. The target lesion primary patency (TLPP) at 6 months post-procedure is the defined primary endpoint to evaluate the safety and effectiveness of the peripheral scoring drug balloon dilatation catheter. ### Conditions Module Conditions: - Arteriovenous Fistula Stenosis Keywords: - arteriovenous fistula stenosis - scoring - hemodialysis - drug-coated balloon ### Design Module #### Design Info Allocation: NA Intervention Model: SINGLE_GROUP ##### Masking Info Masking: NONE Primary Purpose: TREATMENT #### Enrollment Info Count: 328 Type: ESTIMATED Phases: - NA Study Type: INTERVENTIONAL ### Arms Interventions Module #### Arm Group 1 Description: Subjects in this group are treated with Dissolve AV Peripheral Scoring Drug-coated Balloon dilatation catheter Intervention Names: - Device: Dissolve AV Peripheral Scoring Drug-coated Balloon Label: Dissolve AV Peripheral Scoring Drug-coated Balloon Type: EXPERIMENTAL ### Interventions #### Intervention 1 Arm Group Labels: - Dissolve AV Peripheral Scoring Drug-coated Balloon Description: Subjects in the test group are treated with Dissolve AV Peripheral Scoring Drug-coated Balloon Name: Dissolve AV Peripheral Scoring Drug-coated Balloon Other Names: - Scoring Drug-coated Balloon Type: DEVICE ### Outcomes Module #### Primary Outcomes Description: Target Lesion Primary Patency is defined as freedom from clinically driven Target Lesion Failure (TLF) (including +/-5mm proximal or distal of the target lesion) or Vascular Access Thrombosis. TLF is defined as the presence of at least one clinical symptom, sign or indicator (defined according to the NKF-K/DOQI guideline) due to target lesion stenosis (≥ 50% stenosis of the target lesion assessed by contrast angiography or ultrasound), including a significant increase in venous pressure during dialysis, high blood pressure, abnormal physical examination, decreased pump-controlled blood flow, decreased dialysis adequacy, brachial artery blood flow \< 600 ml/min or decreased by 25% compared with the previous follow-up, etc. Measure: Target Lesion Primary Patency (TLPP) at 6 months post-procedure Time Frame: 6 months post-procedure #### Secondary Outcomes Description: TLF is defined as the presence of at least one clinical symptom, sign or indicator (defined according to the NKF-K/DOQI guideline) due to target lesion stenosis (≥ 50% stenosis of the target lesion assessed by contrast angiography or ultrasound), including a significant increase in venous pressure during dialysis, high blood pressure, abnormal physical examination, decreased pump-controlled blood flow, decreased dialysis adequacy, brachial artery blood flow \< 600 ml/min or decreased by 25% compared with the previous follow-up, etc. Measure: Target Lesion Primary Patency (TLPP) Time Frame: 12, 24 months post-procedure Description: Proportion of patients whose peak systolic flow velocity ratio (PSVR) ≤ 2.0, as determined by Doppler ultrasound (DUS), at 6, 12, and 24 months post-procedure, so as to confirm the absence of restenosis. Measure: Proportion of patients whose peak systolic flow velocity ratio (PSVR) ≤ 2.0, as determined by Doppler ultrasound (DUS), so as to confirm the absence of restenosis Time Frame: 6, 12, 24 months post-procedure Description: Any reintervention of a target lesion (including +/-5 mm proximal or distal to the target lesion) as determined by clinical symptoms or dialysis indicators indicating that it is unable to perform dialysis. Measure: Clinically-driven Target Lesion Revascularization (CD-TLR) Time Frame: 1, 6, 12, 18, and 24 months post-procedure Measure: Clinically-driven Target Shunt Revascularization (CD-TSR) Time Frame: 1, 6, 12, 18, and 24 months post-procedure Description: Defined as the ability of the balloon to reach the target lesion, be successfully expanded without rupture, and be successfully withdrawn. Evaluation is based on single balloon dilation catheter. Measure: Device Success Time Frame: During the procedure Description: Defined as residual stenosis of the target lesion post-procedure is ≤ 30%, and no serious adverse events related to the trial device occurred during the perioperative period. Measure: Technical Success Time Frame: 0-5 days post-procedure Description: Defined as ability to complete at least one successful hemodialysis session post-procedure. Measure: Clinical Success Time Frame: 0-5 days post-procedure ### Eligibility Module Eligibility Criteria: Inclusion Criteria: 1. Age ≥ 18 and ≤ 80 years old; 2. The patient's AVF/AVG is mature and has successfully completed hemodialysis at least once; 3. The target lesion is located at the AVF/AVG return vein and venous side anastomosis; 4. Hemodynamically significant AVF/AVG return vein stenosis ≥ 50% as assessed by ultrasound or contrast imaging, and any of the following clinical symptoms, signs or indicators are present, including significant increase in venous pressure during dialysis, abnormal physical examination, decreased pump-controlled blood flow, decreased adequacy of dialysis, brachial artery blood flow \< 600 ml/min or decreased by 25% compared with the previous follow-up visit, etc.; 5. The target lesion is a primary or restenotic lesion, consisting of one or more tandem lesions (if the total length of adjacent tandem lesions is ≤ 60 mm, it can be considered a single target lesion); 6. Visual inspection of the reference blood vessel diameter of the target lesion is between 4.0-8.0mm, and the total length of the target lesion is ≤ 60mm; 7. The patient voluntarily signs the informed consent form. Exclusion Criteria: 1. Women of childbearing age whose preoperative pregnancy test is not negative, and women who are breastfeeding; 2. Patients who have undergone major surgical treatment within 30 days before inclusion in the study; 3. Calcified lesions that are not expected to be expandable with balloons; 4. Patients with thrombosis at the access stenosis site; 5. The target lesion is located at the blood supply artery and arterial anastomosis; 6. Patients known to be allergic to or intolerant to contrast media and paclitaxel; 7. The patient's life expectancy is less than 2 years; 8. Patients with systemic lupus erythematosus and antineutrophil cytoplasmic antibody (ANCA)-associated small vessel vasculitis; 9. Patients with kidney transplantation or those who planned to undergo kidney transplantation or switch to peritoneal dialysis; 10. Vascular access infection or systemic active infection; 11. Those who have participated in unfinished clinical trials of other drugs or devices; 12. Patients with other medical conditions that the investigator believes are not suitable to participate in this study. Maximum Age: 80 Years Minimum Age: 18 Years Sex: ALL Standard Ages: - ADULT - OLDER_ADULT ### Contacts Locations Module #### Central Contacts Contact 1: Email: [email protected] Name: Yuzhu Wang, MD Phone: 18701387950 Role: CONTACT #### Locations Location 1: City: Hefei Contacts: *Contact 1:* - Name: Liang Yuan - Role: CONTACT Country: China Facility: The Second Hospital of Anhui Medical University State: Anhui Location 2: City: Beijing Contacts: *Contact 1:* - Email: [email protected] - Name: Yuzhu Wang, MD - Phone: 18701387950 - Role: CONTACT Country: China Facility: Beijing Haidian Hospital State: Beijing Location 3: City: Chongqing Contacts: *Contact 1:* - Name: Qining Fu - Role: CONTACT Country: China Facility: The First Affiliated Hospital of Chongqing Medical University State: Chongqing Location 4: City: Guanzhou Contacts: *Contact 1:* - Name: Riguang Liu - Role: CONTACT Country: China Facility: Guangzhou First People's Hospital State: Guangdong Location 5: City: Huizhou Contacts: *Contact 1:* - Name: Qiming Chen - Role: CONTACT Country: China Facility: Huizhou Central People's Hospital State: Guangdong Location 6: City: Shenzhen Contacts: *Contact 1:* - Name: Wei Liang - Role: CONTACT Country: China Facility: Peking University Shenzhen Hospital State: Guangdong Location 7: City: Shenzhen Contacts: *Contact 1:* - Name: Tiecheng Yang - Role: CONTACT Country: China Facility: The Eighth Affiliated Hospital, Sun Yat-sen University State: Guangdong Location 8: City: Liuzhou Contacts: *Contact 1:* - Name: Yuhong Chen - Role: CONTACT Country: China Facility: Liuzhou Traditional Chinese Medical Hospital State: Guangxi Location 9: City: Nanning Contacts: *Contact 1:* - Name: Xiaomei Peng - Role: CONTACT Country: China Facility: Foresea Life Insurance Guangxi Hospital State: Guangxi Location 10: City: Guiyang Contacts: *Contact 1:* - Name: Zongyang Liu - Role: CONTACT Country: China Facility: The Affiliated Cancer Hospital of Guizhou Medical University State: Guizhou Location 11: City: Zhengzhou Contacts: *Contact 1:* - Name: Hongtao Zhang - Role: CONTACT Country: China Facility: Henan Provincial People's Hospital State: Henan Location 12: City: Wuhan Contacts: *Contact 1:* - Name: Fan He - Role: CONTACT Country: China Facility: Tongji Hospital Affiliated To Tongji Medical College HUST State: Hubei Location 13: City: Changsha Contacts: *Contact 1:* - Name: Yong Xu - Role: CONTACT Country: China Facility: Changsha Jieao Kidney Disease Hospital State: Hunan Location 14: City: Changsha Contacts: *Contact 1:* - Name: Xun Luo - Role: CONTACT Country: China Facility: Hunan Provincial People's Hospital State: Hunan Location 15: City: Changsha Contacts: *Contact 1:* - Name: Hong Wu - Role: CONTACT Country: China Facility: The Second Xiangya Hospital of Central South University State: Hunan Location 16: City: Nanchang Contacts: *Contact 1:* - Name: Yan Yan - Role: CONTACT Country: China Facility: The First Affiliated Hospital of Nanchang University State: Jiangxi Location 17: City: Changchun Contacts: *Contact 1:* - Name: Mingxin Chang - Role: CONTACT Country: China Facility: The Affiliated Hospital To Changchun University of Chinese Medicine State: Jilin Location 18: City: Xi'an Contacts: *Contact 1:* - Name: Shifeng Yang - Role: CONTACT Country: China Facility: The First Affiliated Hospital of Xi'an Jiaotong University State: Shaanxi Location 19: City: Dezhou Contacts: *Contact 1:* - Name: Jing Sun - Role: CONTACT Country: China Facility: Qilu Hospital of Shandong University Dezhou Hospital State: Shandong Location 20: City: Jinan Contacts: *Contact 1:* - Name: Xiaoping Wang - Role: CONTACT Country: China Facility: Central Hospital Affiliated To Shandong First Medical University State: Shandong Location 21: City: Jinan Contacts: *Contact 1:* - Name: Zunsong Wang - Role: CONTACT Country: China Facility: The First Affiliated Hospital of Shandong First Medical University State: Shandong Location 22: City: Qingdao Contacts: *Contact 1:* - Name: Jian Sun - Role: CONTACT Country: China Facility: Qingdao Municipal Hospital State: Shandong Location 23: City: Rizhao Contacts: *Contact 1:* - Name: Hong Zhang - Role: CONTACT Country: China Facility: People's Hospital of Rizhao State: Shandong Location 24: City: Taiyuan Contacts: *Contact 1:* - Name: Hua Chen - Role: CONTACT Country: China Facility: Shanxi Bethune Hospital State: Shanxi Location 25: City: Chengdu Contacts: *Contact 1:* - Name: Qiang He - Role: CONTACT Country: China Facility: Sichuan Academy of Medical Sciences Sichuan Provincial People's Hospital State: Sichuan Location 26: City: Chengdu Contacts: *Contact 1:* - Name: Ping Fu - Role: CONTACT Country: China Facility: West China Hospital Sichuan University State: Sichuan Location 27: City: Mianyang Contacts: *Contact 1:* - Name: Dan Liao - Role: CONTACT Country: China Facility: Mianyang Central Hospital State: Sichuan Location 28: City: Nanchong Contacts: *Contact 1:* - Name: Heping Zhang - Role: CONTACT Country: China Facility: Affiliated Hospital of North Sichuan Medical College State: Sichuan Location 29: City: Hangzhou Contacts: *Contact 1:* - Name: Hua Li - Role: CONTACT Country: China Facility: Sir Run Run Shaw Hospital Zhejiang University School of medicine State: Zhejiang Location 30: City: Hangzhou Contacts: *Contact 1:* - Name: Hua Jiang - Role: CONTACT Country: China Facility: The First Affiliated Hospital, Zhejiang University School of Medicine State: Zhejiang Location 31: City: Jinhua Contacts: *Contact 1:* - Name: Yangbiao He - Role: CONTACT Country: China Facility: Jinhua Hospital of TCM State: Zhejiang Location 32: City: Taizhou Contacts: *Contact 1:* - Name: Liyun Xu - Role: CONTACT Country: China Facility: Taizhou Hospital of Zhejiang Province State: Zhejiang Location 33: City: Ürümqi Contacts: *Contact 1:* - Name: Alpati - Role: CONTACT Country: China Facility: The First Affiliated Hospital of Xinjiang Medical University State: Ürümqi #### Overall Officials Official 1: Affiliation: Beijing Haidian Hospital Name: Yuzhu Wang, MD Role: PRINCIPAL_INVESTIGATOR ### IPD Sharing Statement Module IPD Sharing: NO ## Derived Section ### Condition Browse Module - Ancestors - ID: D000020763 - Term: Pathological Conditions, Anatomical - ID: D000001165 - Term: Arteriovenous Malformations - ID: D000054079 - Term: Vascular Malformations - ID: D000018376 - Term: Cardiovascular Abnormalities - ID: D000002318 - Term: Cardiovascular Diseases - ID: D000016157 - Term: Vascular Fistula - ID: D000014652 - Term: Vascular Diseases - ID: D000000013 - Term: Congenital Abnormalities ### Condition Browse Module - Browse Branches - Abbrev: BC23 - Name: Symptoms and General Pathology - Abbrev: All - Name: All Conditions - Abbrev: BC14 - Name: Heart and Blood Diseases - Abbrev: BC16 - Name: Diseases and Abnormalities at or Before Birth ### Condition Browse Module - Browse Leaves - ID: M8532 - Name: Fistula - Relevance: HIGH - As Found: Fistula - ID: M4472 - Name: Arteriovenous Fistula - Relevance: HIGH - As Found: Arteriovenous Fistula - ID: M6475 - Name: Constriction, Pathologic - Relevance: HIGH - As Found: Stenosis - ID: M7292 - Name: Dilatation, Pathologic - Relevance: LOW - As Found: Unknown - ID: M22519 - Name: Pathological Conditions, Anatomical - Relevance: LOW - As Found: Unknown - ID: M4473 - Name: Arteriovenous Malformations - Relevance: LOW - As Found: Unknown - ID: M12 - Name: Congenital Abnormalities - Relevance: LOW - As Found: Unknown - ID: M27558 - Name: Vascular Malformations - Relevance: LOW - As Found: Unknown - ID: M20503 - Name: Cardiovascular Abnormalities - Relevance: LOW - As Found: Unknown - ID: M18619 - Name: Vascular Fistula - Relevance: LOW - As Found: Unknown - ID: M17400 - Name: Vascular Diseases - Relevance: LOW - As Found: Unknown ### Condition Browse Module - Meshes - ID: D000001164 - Term: Arteriovenous Fistula - ID: D000003251 - Term: Constriction, Pathologic - ID: D000005402 - Term: Fistula ### Misc Info Module - Version Holder: 2024-05-31

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