VOICE-Early Response to Vedolizumab and IL-23 Antagonists in Participants With Crohn's Disease: A Prospective Observational Study

Last updated: January 31, 2025
Sponsor: Alimentiv Inc.
Overall Status: Active - Recruiting

Phase

N/A

Condition

Colic

Ulcerative Colitis

Crohn's Disease

Treatment

Vedolizumab (VDZ)

Ustekinumab (UST)

Risankizumab (RISA)

Clinical Study ID

NCT06249555
TAK01796
  • Ages > 18
  • All Genders

Study Summary

The primary aim of this study is to explore the time course of response to Vedolizumab in participants with CD as measured by the Patient-Reported Outcomes Measurement Information System (PROMIS) Pain Interference-short form (SF), as well as other PROMIS domain SFs (fatigue, anxiety, depression, sleep disturbance, physical function, and ability to participate in social roles and activities); other PRO measures will also be assessed.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  1. Participant is an adult 18 years of age or older with confirmed CD, as per standardclinical criteria which may include symptoms, endoscopy, histopathology, andimaging.

  2. Participant has active CD and has been prescribed as standard of care (SOC) and isplanned to start VDZ or IL-23 antagonist therapy (UST, RISA, or GUS or MIR [ifapproved for the treatment of CD during the recruitment period for this study]) forthe first time in accordance with the product label, as determined by the treatingphysician.

  3. Participant has a baseline PROMIS Pain Interference-SF score ≥ 15 (correspondingT-score ≥ 55) (PROMIS Pain Interference-SF 8a [V1.1]). a. Score is calculated by adding score (1 to 5) for each of the 8 subcomponents.

  4. Participant has completed all SOC biologic work-up assessments (this may includeassessment of tuberculosis, chronic infections, Clostridioides difficile infectionand vaccination status per local practice).

  5. Ability of participant to participate fully in all aspects of this observationalstudy. Full comprehension of consent language and informed consent must be obtainedfrom the participant and documented.

Exclusion

Exclusion Criteria:

  1. Participant has CD-related surgery planned or anticipated during the study.

  2. Participant has prior exposure to an advanced therapy for the treatment of CD (biologic or small molecule) other than an anti-TNF (i.e., anti-integrin, anti-IL,Janus kinase inhibitors, or sphingosine-1-phosphate receptor 1). Prior failure orintolerance to 2 or more anti-TNF (i.e., infliximab, adalimumab, or certolizumabpegol) therapies in the past 3 years is also cause for exclusion.

  3. Participant has an active infection at baseline requiring intravenous systemicantibiotics. Note: The treating physician must have completed all appropriate baseline screeningtests as per the product label.

  4. Participant has evidence of C. difficile toxin or is prescribed treatment for C.difficile infection, or other intestinal bacterial pathogen, ≤ 2 weeks prior toScreening.

  5. Participant has chronic non-inflammatory bowel disease pain.

Study Design

Total Participants: 300
Treatment Group(s): 3
Primary Treatment: Vedolizumab (VDZ)
Phase:
Study Start date:
March 20, 2024
Estimated Completion Date:
December 31, 2026

Study Description

Vedolizumab (VDZ), a monoclonal antibody that selectively targets intestinal T-cell trafficking, is an effective and safe treatment for moderately to severely active Crohn's disease (CD). Recent evidence from open-label, blinded endpoint studies such as VERSIFY and LOVE-CD provide further support for the efficacy of VDZ in achieving clinical, endoscopic, histologic and radiologic disease improvement in CD. Despite these data, VDZ is generally perceived to have a slower onset of action than other biologics, including tumor necrosis factor (TNF) antagonists and the interleukin (IL)-12/23 antagonist, ustekinumab (UST). The IL-23 antagonist risankizumab (RISA) has been more recently approved for treatment of CD and post-hoc analyses of SEQUENCE trial data showed RISA to be superior to UST for inducing clinical remission at Week 24, and thus, RISA may also be considered to have a quicker onset of action than VDZ. This perception largely emanates from the results of the VDZ pivotal for CD (GEMINI 2) where efficacy was assessed at Week 6 after only 2 doses in a largely refractory population. However, in clinical practice VDZ induction consists of 3 doses of VDZ 300 mg administered intravenously at weeks 0, 2 and 6 instead of the 2 doses used in the pivotal trials. In recent clinical trials, induction endpoints for therapeutics in CD are now typically measured at least after Week 12. Accordingly, it is uncertain whether the generally held perception of a relatively slow onset of action for VDZ is accurate. Moreover, it should also be noted that the perception of a slow onset of action has also been conflated to infer that VDZ is a relatively less effective induction therapy in CD than TNF antagonists or UST. Further data to evaluate these issues are needed.

Rapidity of symptom resolution, which is commonly used as a surrogate for speed of onset, is a priority for patients and clinicians. It is therefore important to better understand the kinetics of symptom improvement captured using patient-reported outcomes (PROs) in patients initiating VDZ for treatment of CD.

Connect with a study center

  • University of Alberta

    Edmonton, Alberta T6G2X8
    Canada

    Active - Recruiting

  • University of British Columbia

    Vancouver, British Columbia V6Z2K5
    Canada

    Active - Recruiting

  • GNRR Digestive Clinics and Research Center

    Brampton, Ontario L6S0E2
    Canada

    Active - Recruiting

  • Alimentiv

    London, Ontario N6Z5B6
    Canada

    Active - Recruiting

  • West GTA Research Inc.

    Mississauga, Ontario L5M7N4
    Canada

    Active - Recruiting

  • ABP Research Services Corp.

    Oakville, Ontario L6L5L7
    Canada

    Active - Recruiting

  • Rajbir Rai Medicine Professional Corporation

    Oakville, Ontario L6L4P7
    Canada

    Active - Recruiting

  • Scarborough Center for Inflammatory Bowel Disease

    Scarborough, Ontario M1B3V4
    Canada

    Active - Recruiting

  • Toronto Immune & Digestive Health Institute Inc.

    Toronto, Ontario M6A3B4
    Canada

    Active - Recruiting

  • McMaster University Medical Center

    Hamilton, Ontatrio L8N 3Z5
    Canada

    Active - Recruiting

  • GI Alliance - Sun City

    Sun City, Arizona 85351
    United States

    Site Not Available

  • Digestive and Liver Center of Florida

    Kissimmee, Florida 34741
    United States

    Active - Recruiting

  • Northwestern University

    Evanston, Illinois 60611
    United States

    Site Not Available

  • University of Iowa

    Iowa City, Iowa 52242
    United States

    Active - Recruiting

  • University Medical Center New Orleans

    New Orleans, Louisiana 70112
    United States

    Active - Recruiting

  • University of North Carolina

    Chapel Hill, North Carolina 27599
    United States

    Active - Recruiting

  • OR Clinic - East - GI

    Portland, Oregon 97220
    United States

    Active - Recruiting

  • GI Alliance Research Fort Worth

    Fort Worth, Texas 76104
    United States

    Site Not Available

  • GI Alliance Research Mansfield

    Mansfield, Texas 76063
    United States

    Site Not Available

  • GI Alliance - Bellevue - Washington Gastroenterology

    Bellevue, Washington 98004
    United States

    Site Not Available

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