InDuctIon TREatment with SubCuTaneous Infliximab for Crohn's Disease

Last updated: December 5, 2024
Sponsor: Academisch Medisch Centrum - Universiteit van Amsterdam (AMC-UvA)
Overall Status: Active - Recruiting

Phase

3

Condition

Inflammation

Ulcerative Colitis (Pediatric)

Inflammatory Bowel Disease

Treatment

Infliximab subcutaneous

Immunosuppressive Agents

Clinical Study ID

NCT06059989
NL76663.018.21
  • Ages 18-80
  • All Genders

Study Summary

Study Design:

A Prospective Multicenter Randomized Controlled, Open-label Non-inferiority Study to Investigate the Efficacy of Subcutaneous (SC) Infliximab (IFX) with and without Immunomodulators during Induction treatment in Moderate to Severe Crohn's Disease.

Primary endpoint:

The proportion of patients in corticosteroid-free clinical remission (as defined by a Crohn's disease activity index (CDAI)<150) and endoscopic response (as defined by a simple endoscopic score for Crohn's disease (SES-CD) drop of at least 50%) at week 26.

Accrual and feasibility:

This study will enroll 158 subjects at approximately 20 sites in the Netherlands (peripheral and academic hospitals). The estimated enrollment is 0.5 patient/centre/month leading to an inclusion duration of 16 months once all centres are open. The first enrolment is anticipated in Q1 2021.

Treatment, dosage and administration:

Eligible patients will be randomized to receive SC IFX monotherapy (240mg at week 0 and week 2 and then 120mg every other week (EOW) OR SC IFX (240mg at week 0 and week 2 and then 120mg EOW) in combination with immunosuppression.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  1. Patients 18 years or older diagnosed with Crohn's disease

  2. Patients with moderate to severely active Crohn's disease with a Crohn's DiseaseActivity Index (CDAI) of 250 to 450 and presence of endoscopic ulceration in theterminal ileum, colon or both. Minimal SES-CD is ≥ 6 or ≥ 4 for isolated ilealdisease.

  3. Patients who had no response or loss of response to or have had intolerable sideeffects to one or more to the following: glucocorticoids, thiopurines (azathioprine/6-mercaptopurine/6-thioguanin), methotrexate , adalimumab, vedolizumabor ustekinumab OR patients in need of immediate top-down treatment with IFX at thediscretion of the treating physician.

  4. In the opinion of the investigator, the subject is capable of understanding andcomplying with protocol requirements.

  5. The subject signs and dates a written, informed consent form and any requiredprivacy authorization prior to the initiation of any study procedure.

  6. Male or non-pregnant, non-lactating females. No wish to become pregnant in thecoming 26 weeks.

Exclusion

Exclusion Criteria:

  1. Patients at imminent need of surgery as judged by the treating clinician

  2. Patients with the short bowel syndrome, an ostomy or a symptomatic non-inflammatorystricture

  3. Patients previously exposed to IFX (intravenous or subcutaneous)

  4. Previously unacceptable side effects or intolerance to all immunosuppressants (boththiopurines and methotrexate)

  5. Treatment with adalimumab or vedolizumab or ustekinumab within 30 days

  6. Patients who have had a primary non-response to adalimumab or had intolerableclass-related side effects (as evaluated at the discretion of the treatingphysician)

  7. Enteric pathogens (such as Salmonella, Shigella, Yersinia, Campylobacter and C.difficile) detected by stool analysis within 2 weeks prior to enrollment or atscreening

  8. Ongoing participation in another interventional trial

  9. Patients with Ulcerative Colitis or Inflammatory bowel disease unclassified (IBD-U)

  10. Patients with ongoing abdominal or undrained perianal abscess

  11. Patients with a history of colon cancer or colonic dysplasia, unless sporadicadenoma, which has been removed

  12. Active or latent tuberculosis (screening according to national guidelines). Exceptwhen the latter has been treated appropriately according to national guidelines.

  13. Cardiac failure in the New York heart Association (NYHA) stage III-IV

  14. History of demyelinating disease

  15. Recent live vaccination (≤ 4 weeks)

  16. Patients with ongoing acute/chronic infection (including but not limited to HIV,hepatitis B and C) with the exception of chronic herpes labialis or cervical humanpapillomavirus (HPV)

  17. History of cancer in the last 5 years with the exception of non-melanoma skin cancer

  18. Male patients with Epstein-Barr virus (EBV) negative serology

  19. A history of alcohol or illicit drug use that in the opinion of the principalinvestigator (PI) would interfere with study procedures

  20. Patients with psychiatric problems that in the opinion of the PI would interferewith study procedures

  21. Patients unable to attend all study visits

  22. Patients with a history of non-compliance with clinical study protocols

  23. Contraindication for endoscopy

  24. Patients who received any investigational drug in the past 30 days or 5 half-lives,whichever is longer

  25. Pregnancy or lactation or wish to become pregnant in the coming 26 weeks

Study Design

Total Participants: 158
Treatment Group(s): 2
Primary Treatment: Infliximab subcutaneous
Phase: 3
Study Start date:
November 25, 2021
Estimated Completion Date:
December 31, 2025

Study Description

Permitted concomitant medications:

Oral prednisone (≤40 mg per day) or budesonide (≤9 mg per day) are permitted if on stable dose 2 weeks prior to screening. After 2 weeks into treatment, systemic corticosteroids will be tapered at a rate of at least 5 mg per week and budesonide will be tapered at a rate of 3 mg every 2 weeks. If tapering fails, re-introduction of lowest effective dose of corticosteroid is allowed a single time at the discretion of the treating physician, after which tapering is required beginning 2 weeks later.

Stable doses of mesalazine (at a maximum dose of 4g/day) are permitted throughout the study.

Stable doses of antibiotics are permitted until week 12. Adverse events to antibiotics can prompt treatment discontinuation, in that case a switch is allowed during week 12.

Patients randomized to IFX combination therapy will also receive 6-mercaptopurine 1-1.5 mg/kg. If participants are already using azathioprine or thioguanine, they will receive continued dosing 2-2.5mg/kg or 20mg once daily, respectively (unless shunter status or previous adverse events suggest differently). In case of previous adverse event leading to thiopurine discontinuation methotrexate 15 mg/week sc. in combination with oral folic acid 5mg/week will be prescribed.

Immunosuppressive treatment will be stopped at screening (approximately 2 weeks before randomization) for all patients and will be restarted for patients in the combination treatment group. Patients randomized to IFX monotherapy will not receive concomitant immunosuppression.

Primary Objectives:

The aim of this study is to investigate the efficacy of subcutaneous IFX in the treatment of moderate to severe Crohn's disease with and without concomitant immunosuppression, as measured by the proportion of patients in corticosteroid-free clinical remission (as defined by a CDAI<150) and endoscopic response (as defined by a SES-CD drop of at least 50%) at week 26. The Investigator hypothesizes that subcutaneous IFX monotherapy is non-inferior to subcutaneous IFX with concomitant immunosuppression in inducing this combined primary endpoint of corticosteroid free remission (CSF), clinical remission and endoscopic response by week 26.

Secondary Objectives: (not hierarchical)

  • The proportion of patients in endoscopic remission at week 26 (defined as the absence of ulcerations larger then 5mm)

  • Proportion of patients with endoscopic remission at week 26 (as measured by SES-CD≤2)

  • Proportion of patients with endoscopic response at week 26 (as measured by at least 50% reduction in the SES-CD as compared to baseline)

  • Proportion of patients in corticosteroid-free clinical remission at week 26 (defined as a CDAI<150)

  • The proportion of patients in corticosteroid-free remission (CSF) deep remission at week 26, as defined by corticosteroid-free clinical (CDAI<150) AND endoscopic remission (defined as the absence of ulcerations larger then 5mm)

  • Proportion of patients in clinical remission at week 2, 4, 8, 14 and 26 (defined as a CDAI<150)

  • Proportion of patients achieving clinical response at week 2, 4, 8, 14 and 26 (defined as a CDAI-70)

  • Proportion of patients achieving clinical response at week 26 (defined as a CDAI-100)

  • Proportion of patients in symptomatic remission at week 2, 4, 8, 14 and 26 (defined as a patient reported outcome (PRO-2) (stool frequency and abdominal pain) <8)

  • Proportion of patients achieving symptomatic response at week 2, 4, 8, 14 and 26 (defined as a PRO-2 -8)

  • Time to symptomatic remission (defined as a PRO-2 (stool frequency and abdominal pain) <8)

  • Proportion of patients in biochemical remission at week 8, 14 and 26 : C-reactive protein (CRP ≤ 5.0 mg/L and fecal calprotectin < 250 mg/g)

  • Time to biochemical remission (CRP ≤ 5.0 mg/L and fecal calprotectin < 250 mg/g)

  • Proportion of patients achieving minimally clinically important difference in quality of life at week 2, 4, 8, 14 and week 26 compared to baseline as assessed by the inflammatory bowel disease questionnaire (IBDQ) and EuroQol - 5 dimension - 5 level (EQ-5D-5L) questionnaire

  • Proportion of patients developing anti-drug antibodies (ADA) against IFX at week 2, 4, 8, 14 and 26 as measured by a drug-tolerant assay

  • IFX trough levels at week 2, 4, 8, 14 and 26

  • Human Leukocyte antigen (HLA) haplotyping and correlation with anti-drug antibodies (ADA) development

  • Thiopurine metabolites at baseline, week 14 and week 26 (for patients randomized for the combination therapy group, only at baseline for those in the monotherapy group and with previous IS use)

  • Proportion of patients having IFX trough levels of >5ug/ml at week 26

  • Proportion of patients achieving histological healing at week 26

  • Proportion of patients (of those with active perianal disease at baseline) in clinical remission and response of their perianal disease, as defined by the fistula drainage assessment at week 26

  • Proportion of patients with extraintestinal manifestations at week 26 as compared to baseline

  • Adverse events.

Subject Population:

158 patients with moderate to severe Crohn's disease between the age of 18-80 years who are starting with IFX treatment.

Treatment Arms:

Group 1: Subcutaneous IFX monotherapy 240mg at week 0 and week 2 and then 120mg EOW.

Group 2: Subcutaneous IFX 240mg at week 0 and week 2 and then 120mg EOW in combination with immunosuppressive.

Randomly assigned to either of these groups in a 1:1 ratio. Randomization will be stratified according to immunosuppressive use at screening.

Duration of Treatment: 26 weeks. Period of evaluation: 26 weeks.

Connect with a study center

  • Amsterdam UMC AMC

    Amsterdam, North Holland 1105AZ
    Netherlands

    Active - Recruiting

Not the study for you?

Let us help you find the best match. Sign up as a volunteer and receive email notifications when clinical trials are posted in the medical category of interest to you.