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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT05056441
Other study ID # Vedolizumab-5066
Secondary ID
Status Completed
Phase
First received
Last updated
Start date December 1, 2021
Est. completion date September 30, 2022

Study information

Verified date October 2022
Source Takeda
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

The main aim of this study is to compare long-term remission in participants receiving vedolizumab (VDZ) and those receiving ustekinumab (UST). In this study, the study doctors will review each participant's past medical records. This study is about collecting existing information only; participants will not receive treatment or need to visit a study doctor during this study.


Description:

This is a non-interventional, retrospective study of participants with CD. The study will review the medical charts of participants who have initiated the treatment with vedolizumab and ustekinumab or another biologic agent (post- index). The study will aim to enroll approximately 700 participants, with 350 participants in each of the following cohorts: - Cohort 1: Vedolizumab - Cohort 2: Ustekinumab The data for participants will be collected in two main periods: - Pre-Index Event Period: From the date of diagnosis of CD until the date of index when vedolizumab or ustekinumab was initiated during the eligibility period. - Post-Index Event Period: From one day post-index when vedolizumab or ustekinumab was initiated during the eligibility period until chart abstraction initiation, unless the date of death or loss to follow-up is before the date of chart abstraction initiation. This multi-center study will be conducted in Belgium, Australia, and Switzerland. The overall time for data collection in the study will be approximately 12 months and the long-term duration of the study is approximately 36 months.


Recruitment information / eligibility

Status Completed
Enrollment 623
Est. completion date September 30, 2022
Est. primary completion date September 30, 2022
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: 1. Has a diagnosis of CD documented in the medical records. 2. Has received at least one dose of vedolizumab or ustekinumab at one of the participating study sites during the eligibility period. 3. Was biologic-naïve (no prior biologic use for any pathology, including CD) at the time of index event. 4. Has completed induction phase and has a minimum of a six-month duration between the date of the index event and the date of chart abstraction initiation and was still under active care at the site six months post-index date. Exclusion Criteria: 1. Has received vedolizumab or ustekinumab as part of a clinical trial in their lifetime (includes index event). 2. Has initiated index treatment as combination therapy with two biologic agents. 3. Has received previous treatment with biologic agents for CD or conditions other than CD ever in their lifetime. 4. Has medical chart empty or missing. 5. Part or all of the participant's index treatment was received at a different site, and the participant's medical chart pertaining to this care is not accessible. 6. Has received a subcutaneous formulation of ustekinumab for induction (that is, a subcutaneous induction dose of ustekinumab prior to ustekinumab's approval for CD in the study countries).

Study Design


Related Conditions & MeSH terms


Locations

Country Name City State
Australia Royal Adelaide Hospital Adelaide South Australia
Australia Monash Health, Monash Medical Centre Clayton Victoria
Australia Concord Repatriation General Hospital Concord New South Wales
Australia Royal Melbourne Hospital East Melbourne Victoria
Australia Lyell McEwin Hospital Elizabeth Vale South Australia
Australia Royal Brisbane & Women's Hospital Herston Queensland
Australia Liverpool Hospital Liverpool New South Wales
Australia The Alfred Hospital Melbourne Victoria
Australia Fiona Stanley Hospital Murdoch Western Australia
Australia John Hunter Hospital New Lambton New South Wales
Australia Mater Misericordiae Health Services South Brisbane Queensland
Australia St John of God Hospital Subiaco Subiaco Western Australia
Australia Integrated Gut Health Pty Ltd Taringa Queensland
Belgium Hopital Erasme Anderlecht Brussels
Belgium Imelda VZW Bonheiden Antwerpen
Belgium CHU St-Pierre Brussels
Belgium UZ Antwerpen Edegem Antwerpen
Belgium AZ Sint-Lucas Gent Oost-Vlaanderen
Belgium UZ Gent Gent Oost-Vlaanderen
Belgium AZ Groeninge Kortrijk West-Vlaanderen
Belgium UZ Leuven Leuven Vlaams Brabant
Belgium Centre Hospitalier Chretien MontLegia Liege
Belgium CHU de Liege Liege
Belgium Centre Hospitalier Universitaire Ambroise Pare Mons Hainaut
Belgium AZ Delta Roeselare West-Vlaanderen
Belgium CHWAPI Tournai Tournai Hainaut
Switzerland Clarunis Bauchzenturm Basel Basel-Stadt (de)
Switzerland Inselspital Bern Bern Bern (de)
Switzerland Intesto KLG Gastroenterologische Praxis Crohn-Colitis-Zentrum Bern Bern (de)
Switzerland Stadtspital Triemli Zurich Zurich Zurich (de)
Switzerland Universitatsspital Zurich Zurich Zurich (de)

Sponsors (1)

Lead Sponsor Collaborator
Takeda

Countries where clinical trial is conducted

Australia,  Belgium,  Switzerland, 

Outcome

Type Measure Description Time frame Safety issue
Primary Cumulative Rates of Clinical Remission Over 36 Months Compared Between VDZ and UST Cohorts Clinical remission will be defined as Crohn's Disease Activity Index (CDAI) score less than (<) 150 points, or if unknown, Harvey-Bradshaw Index (HBI) Overall score less than or equal to (<=) 4 points, or if unknown, Modified HBI (mHBI) score <=4 points, or if unknown, changes in biomarker assessments (C-reactive Protein, Fecal Calprotectin, and albumin) or remission status recorded in medical chart as 'in remission'. CDAI score <150 indicates quiescent disease and >450 indicates extremely severe disease. HBI consisted of 5 clinical parameters: general well-being, abdominal pain, number of liquid stools per day, abdominal mass, and complications. mHBI consisted of 4 clinical parameters- general well-being, abdominal pain, number of liquid stools per day and additional manifestation. HBI and mHBI total score will be sum of individual parameters, score ranges 0 to no pre-specified maximum score as it depends on number of liquid stools, where higher scores is more severe disease. Baseline up to 36 months post-index date
Secondary Cumulative Rates of Clinical Response Over 36 Months Compared Between VDZ and UST Cohorts Clinical response will be defined as CDAI positive change in score from baseline, or if unknown, HBI overall score decrease of >=3 points from baseline, or if unknown, Modified HBI score decrease of >=3 points from baseline, or if unknown, changes in biomarker assessments (CRP, FCP, and albumin) or treatment response recorded in the medical chart as 'complete response' or 'partial response'. CDAI score <150 indicates quiescent disease and >450 indicates extremely severe disease. HBI consisted of 5 clinical parameters: general well-being, abdominal pain, number of liquid stools per day, abdominal mass, and complications. mHBI consisted of 4 clinical parameters- general well-being, abdominal pain, number of liquid stools per day and additional manifestation. HBI and mHBI total score will be sum of individual parameters, score ranges 0 to no pre-specified maximum score as it depends on number of liquid stools, where higher scores is more severe disease. Baseline up to 36 months post-index date
Secondary Cumulative Rates of Clinical Remission Over 30 Months Compared Between VDZ and UST Cohorts Clinical remission will be defined as CDAI score <150 points, or if unknown, HBI Overall score of <=4 points, or if unknown, mHBI score of <=4 points, or if unknown, changes in biomarker assessments (CRP, FCP, and albumin) or remission status recorded in the medical chart as 'in remission'. CDAI score <150 indicates quiescent disease and >450 indicates extremely severe disease. HBI consisted of 5 clinical parameters: general well-being, abdominal pain, number of liquid stools per day, abdominal mass, and complications. mHBI consisted of 4 clinical parameters- general well-being, abdominal pain, number of liquid stools per day and additional manifestation. HBI and mHBI total score will be sum of individual parameters, score ranges 0 to no pre-specified maximum score as it depends on number of liquid stools, where higher scores is more severe disease. Baseline up to 30 months post-index date
Secondary Cumulative Rates of Mucosal Healing Over 36 Months Compared Between VDZ and UST Cohorts Mucosal healing will be defined as endoscopic assessment score = 0 or 1 (that is, normal or inactive disease or mild disease), or if unknown, Simple Endoscopic Score for Crohn's Disease [SES-CD] score of <3, 'lack of ulceration' defined by one or more of the following endoscopic procedure findings either selection of 'no ulcers' or free-text indication of 'lack of ulceration', or if unknown, one or more endoscopic procedure findings indicating inactive disease (no findings/no active disease, no erosion, no ulcers, no inflammation or inflammatory activity, or no pathological findings), with higher scores indicating more severe disease. The score for each endoscopic variable is sum of values obtained for each segment. The SES-CD total is sum of the 4 endoscopic variable scores from 0 to 56, where higher scores indicate more severe disease. Baseline up to 36 months post-index date
Secondary Cumulative Rates of Deep Remission Over 36 Months Compared Between VDZ and UST Cohorts Deep remission (clinical remission and mucosal healing) is defined as CDAI score <150 and SES-CD score <3. CDAI is scoring system for the assessment of CD activity, index values of 150 and below are associated with quiescent disease; values above that indicate active disease and values above 450 are seen with extremely severe disease. The SES-CD evaluates 4 endoscopic variables (ulcer size, percentage of the surface area affected, and stenosis in 5 colonic segments evaluated during ileocolonoscopy (ileum, right colon, transverse colon, left colon, and rectum). The SES-CD total is the sum of the 4 endoscopic variable scores from 0 to 56, where higher scores indicate more severe disease. Baseline up to 36 months post-index date
Secondary Cumulative Rates of Corticosteroid (CS)-free Remission Over 36 Months Compared Between VDZ and UST Cohorts CS-free remission is defined as participants using oral corticosteroids at baseline who have discontinued corticosteroids and have clinical remission up to 36-months. Baseline up to 36 months post-index date
Secondary Cumulative Rates of CS-free Response Over 36 Months Compared Between VDZ and UST Cohorts Corticosteroid-free response is defined as participants using oral corticosteroids at baseline who have discontinued oral corticosteroids and have clinical response up to 36-months. Baseline up to 36 months post-index date
Secondary Time to Treatment Switching Compared Between VDZ and UST Cohorts Time to Treatment Switching is defined as time from index treatment initiation until a participant initiates subsequent treatments. From index event up to a maximum of 36 months post-index date
Secondary Time to Treatment Discontinuation Compared Between VDZ and UST Cohorts Time to Treatment Discontinuation is defined as time from index treatment initiation until participant discontinues index treatment without switching to subsequent treatments. From index event up to a maximum of 36 months post-index date
Secondary Time to Dose Escalation Compared Between VDZ and UST Cohorts Time to Dose Escalation is defined as time from index treatment initiation until increase in index treatment frequency or dose and/or treatment frequency for >=2 consecutive drug administrations. From index event up to a maximum of 36 months post-index date
Secondary Incidence Rate of Adverse Events (AEs) Compared Between VDZ and UST Cohorts Incidence rate of AE will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. From the index event (Baseline) to the earliest date of chart abstraction initiation, death or last contact with the site (up to approximately Month 6 post-index date)
Secondary Incidence Rate of Serious Adverse Events (SAEs) Compared Between VDZ and UST Cohorts Incidence rate of SAEs will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. SAE is defined as an AE that either results in death, was a life threatening event), requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, results in a congenital anomaly/birth defect, or is a medically important event in the opinion of the physician. From the index event (Baseline) to the earliest date of chart abstraction initiation, death or last contact with the site (up to approximately Month 6 post-index date)
Secondary Incidence Rate of Serious Infections (SIs) Compared Between VDZ and UST Cohorts Incidence rate of SIs will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. SI is defined as an SAE that is an infection. From the index event (Baseline) to the earliest date of chart abstraction initiation, death or last contact with the site (up to approximately Month 6 post-index date)
Secondary Incidence Rate of Emergency Department (ED) Visits Compared Between VDZ and UST Cohorts Incidence rate of ED will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. From the index event (Baseline) to the earliest date of chart abstraction initiation, death or last contact with the site (up to approximately Month 12 post-index date)
Secondary Incidence Rate of CD-related Hospitalizations Compared Between VDZ and UST Cohorts Incidence rate of CD-related hospitalizations will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. and CD-related Hospitalizations is defined as hospitalization with reason for hospitalization related to CD. From the index event (Baseline) to the earliest date of chart abstraction initiation, death or last contact with the site (up to approximately Month 12 post-index date)
Secondary Incidence Rate of CD-related Surgical Procedures compared between VDZ and UST cohorts Incidence rate of CD-related surgical procedures will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. CD-related surgical procedures are defined as types of surgeries that are related to CD. From the index event (Baseline) to the earliest date of chart abstraction initiation, death or last contact with the site (up to approximately Month 12 post-index date)
Secondary Incidence Rate of Disease Exacerbations Compared Between VDZ and UST Cohorts Incidence rate of disease exacerbations will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. Exacerbations are defined as disease flares documented in the participant's medical chart. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Time to Treatment Switching of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Time to Treatment Discontinuation of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Time to Dose Escalation of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Cumulative Rates of Clinical Response of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Clinical response defined as CDAI positive change in score from baseline, if unknown, HBI overall score decrease >=3 points from baseline, if unknown, mHBI score decrease >=3 points from baseline, if unknown, changes in CRP, FCP, albumin or treatment response as complete response/partial response. CDAI score <150 indicates quiescent disease, >450 indicates extremely severe disease. HBI includes general well-being, abdominal pain, number of liquid stools per day, abdominal mass, complications. mHBI includes general well-being, abdominal pain, number of liquid stools/day, additional manifestation. HBI and mHBI total score is sum of individual parameters, score ranges 0 to no pre-specified maximum score, as it depends on number of liquid stools, higher scores means severe disease. Subsequent line treatment: biologic and advanced therapy regimen for participants who discontinued biologic VDZ and UST, initiated 1 or more biologic, advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Cumulative Rates of Clinical Remission of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Clinical remission defined as CDAI score <150 points, or if unknown, HBI Overall score of <=4 points, or if unknown, mHBI score of <=4 points, or if unknown, changes in CRP, FCP, and albumin or remission status recorded in the medical chart as 'in remission'. CDAI score <150 indicates quiescent disease and >450 indicates extremely severe disease. HBI includes: general well-being, abdominal pain, number of liquid stools/day, abdominal mass, complications. mHBI includes- general well-being, abdominal pain, number of liquid stools/day and additional manifestation. HBI and mHBI total score will be sum of individual parameters, score ranges 0 to no pre-specified maximum score as it depends on number of liquid stools, where higher scores is more severe disease. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic VDZ or UST and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Cumulative Rates of Mucosal Healing of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Mucosal healing defined as endoscopic score = 0 or 1 (normal or inactive disease or mild disease), or if unknown, Simple Endoscopic Score for Crohn's Disease [SES-CD] score of <3, 'lack of ulceration' defined by one or more of following endoscopic procedure findings either selection of 'no ulcers' or free-text indication of 'lack of ulceration', or if unknown, one or more endoscopic procedure findings: inactive disease (no findings/no active disease, no erosion, no ulcers, no inflammation or inflammatory activity, or no pathological findings), higher scores more severe disease. Score for each endoscopic variable is sum of values obtained for each segment. SES-CD total is sum endoscopic variable scores: 0 to 56, higher scores indicate more severe disease. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic VDZ or UST and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Cumulative Rates of Deep Remission of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Deep remission (clinical remission and mucosal healing) is defined as CDAI score <150 and SES-CD score <3. CDAI is scoring system for the assessment of CD activity, index values of 150 and below are associated with quiescent disease; values above that indicate active disease and values above 450 are seen with extremely severe disease. The SES-CD evaluates 4 endoscopic variables (ulcer size, percentage of the surface area affected, and stenosis in 5 colonic segments evaluated during ileocolonoscopy (ileum, right colon, transverse colon, left colon, and rectum). The SES-CD total is the sum of the 4 endoscopic variable scores from 0 to 56, where higher scores indicate more severe disease. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Cumulative Rates of Corticosteroid (CS)-free Remission of Subsequent Line Treatments Compared Between VDZ and UST Cohorts CS-free remission is defined as participants using oral corticosteroids at baseline. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Cumulative Rates of CS-free Response of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Corticosteroid-free response is defined as participants using oral corticosteroids at baseline. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Incidence Rate of AEs of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Incidence rate of AE will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Incidence Rate of SAEs of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Incidence rate of SAEs will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. SAE is defined as an AE that either results in death, was a life threatening event), requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, results in a congenital anomaly/birth defect, or is a medically important event in the opinion of the physician. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
Secondary Incidence Rate of SIs of Subsequent Line Treatments Compared Between VDZ and UST Cohorts Incidence rate of SIs will be measured in per 100 person-years. 100 person-years will be used as it is a method that can account for large among-participant variations in follow-up time. SI is defined as an SAE that is an infection. Subsequent line treatment is defined as biologic and advanced therapy regimen(s) for participants who discontinued biologic vedolizumab or ustekinumab and initiated one or more biologic and advanced therapies, post-index treatment discontinuation. From the date of initiation of subsequent line treatment up to the earliest date of chart abstraction initiation, death or last contact with the site (up to a maximum of 36 months post-index date)
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