AMARETTO: Subcutaneous Infliximab After A Previous Intravenous Dose Optimization

Sponsor
Belgian Inflammatory Bowel Disease Research and Development (BIRD) VZW (Other)
Overall Status
Not yet recruiting
CT.gov ID
NCT06113913
Collaborator
Celltrion (Industry)
310
3
32

Study Details

Study Description

Brief Summary

The goal of this clinical trial is to learn about the treatment with subcutaneous infliximab in patients with inflammatory bowel disease (IBD) that were previously treated with an optimized dose of intravenous infliximab.

The main question it aims to answer is:
  • Is switching to a weekly dose of subcutaneous infliximab (120 mg) associated with a better outcome compared to the standard fortnightly administration of 120 mg subcutaneous infliximab in patients who received an optimized intravenous dosing schedule?

Participants will switch from intravenous infliximab to subcutaneous infliximab and will be randomized to the intervention arm (Subcutaneous infliximab weekly) or the interventional comparison arm (subcutaneous infliximab bi-weekly). Participants will follow daily clinical practice in the monitoring for clinical and biological remission.

The participants that are willing to switch to subcutaneous infliximab will be compared to a group of participants not willing to switch. These participants will continue to be treated with their optimized intravenous dose of infliximab.

Detailed Description

Inflammatory bowel diseases (IBD) are a group of immune mediated disorders primarily targeting the gastro-intestinal tract and consist of two distinct phenotypes: Crohn's disease (CD) and ulcerative colitis (UC) that share similarities in both clinical presentation, pathophysiology and treatment. A small proportion of IBD patients cannot be correctly characterized in one of those categories and is referred to as IBD type unclassified (IBDU), which is often classified under UC for clinical research purposes. TNF inhibitors are one of the most frequently prescribed biological therapies and remain an important part of the therapeutic arsenal with international guidelines recommending their use in moderate-to-severe CD and UC when conventional treatments have failed.

Infliximab, a chimer monoclonal antibody against tumor necrosis factor (TNF), was the first anti-TNF agent to be approved for treating IBD as early as 1999. After losing its product patent in 2013, several biosimilars of infliximab have been commercialized including CT-P13. Originally only available in an intravenous (IV) formulation, a subcutaneous (SC) formulation of CT-P13 has been registered for treating moderate-to-severe CD and UC as well. However, many questions on the use of these subcutaneous formulations of infliximab in daily clinical practice remain unanswered, especially in patients who previously required IV dose optimization of infliximab.

The primary objective of the AMARETTO trial is to compare clinical and biological outcome between a regimen with SC infliximab every week and SC infliximab every other week among patients who were in clinical and biological remission with an optimized IV schedule when they switched to SC infliximab.

The secondary objectives of this study are:
  • To compare treatment optimization and discontinuation between a regimen with SC inflixmab every week and SC infliximab every other week among patients who were in clinical and biological remission with an optimized IV schedule when they switched to infliximab SC.

  • To evaluate the willingness and the experience of patients switching to SC infliximab.

  • To compare clinical and biological outcome, as well as treatment optimization and discontinuation between a regimen with SC infliximab (every week or every other week) and IV infliximab among patients who were in clinical and biological remission with an optimized IV schedule.

This study is a national, multicenter, randomized, open-label, prospective, pragmatic trial in Belgium. The trial design is as follows:

  • All subjects will undergo screening procedures. The screening visit of eligible patients will include the review of inclusion and exclusion criteria, and the informed consent form procedure. After screening, if the patient fulfils all inclusion and none of the exclusion criteria, and is willing to participate, the gastroenterologist will record the characteristics of patients and of the disease, medical and surgical history, current and past IBD treatments physical examination, the PRO-2 score about the last 3 days before the visit, blood analysis, stool analysis and patients will be asked to fill in a questionnaire about healt-related quality of life.

  • Afterwards the patients will visit the gastroenterologist 4 times in one year (week 0, week 6 or 8, week 24 or 26 and week 52 or 54). During these visits a physical examination will be done, the PRO-2 score based on the 3 previous days before the visit will be calculated, a blood analysis and stool analysis will be done, the concomittant medication will be collected and patients will be asked to answer the questionnaire about the health related quality of life.

NOTE: patients that switch to subcutaneous infliximab will be asked to collect all at home administrations in a diary and to additionnaly answer a questionnaire about the satisfaction of switching to subcutaneous infliximab.

Study Design

Study Type:
Interventional
Anticipated Enrollment :
310 participants
Allocation:
Randomized
Intervention Model:
Parallel Assignment
Masking:
None (Open Label)
Primary Purpose:
Treatment
Official Title:
Subcutaneous Infliximab After A Previous Intravenous Dose Optimization
Anticipated Study Start Date :
Jan 1, 2024
Anticipated Primary Completion Date :
Jan 1, 2026
Anticipated Study Completion Date :
Sep 1, 2026

Arms and Interventions

Arm Intervention/Treatment
Experimental: Interventional (SC infliximab, weekly)

Participants will switch from an optimized dose of intravenous infliximab to an optimized dose of subcutaneous infliximab. This means the participants will inject 120 mg subcutaneous infliximab every week.

Drug: Infliximab
Weekly administration of subcutaneous infliximab.

Experimental: Interventional comparator (SC infliximab, bi-weekly)

Participants will switch from an optimized dose of intravenous infliximab to subcutaneous infliximab. This means the participants will inject 120 mg subcutaneous infliximab every other week.

Drug: Infliximab
Bi-weekly administration of subcutaneous infliximab.

Active Comparator: Intravenous comparator (IV infliximab, optimized dosing schedule)

Participants not willing to switch will continue treatment with intravenous infliximab at the same dosing schedule as before.

Drug: Infliximab
Optimized dosing schedule of intravenous infliximab.

Outcome Measures

Primary Outcome Measures

  1. • The number of patients that maintain steroid-free clinical and biological remission by week 52 without treatment optimization after switch to SC infliximab (composite endpoint) [week 52]

Secondary Outcome Measures

  1. • The number of patients that maintain steroid-free clinical and biological remission by week 52 or 54 with treatment optimization [week 52 or 54]

  2. • The number of patients that maintain steroid-free clinical and biological remission by week 52 or 54 (with or without treatment optimization) [week 52 or 54]

  3. • The number of patients that maintain steroid-free clinical and biological remission by week 6 or 8, by week 24 or 26 (without treatment optimization) [week 6 or 8 and week 24 or 26]

  4. • The number of patients that maintain steroid-free clinical remission by week 6 or 8, by week 24 or 26, by week 52 or 54 (without treatment optimization) [week 6 or 8, week 24 or 26 and week 52 or 54]

  5. • The number of patients that maintain steroid-free biological remission by week 6 or 8, by week 24 or 26, by week 52 or 54 (without treatment optimization) [week 6 or 8, week 24 or 26 and week 52 or 54]

  6. • The number of patients switching back to IV infliximab by week 8, by week 26, by week 52 [week 6, week 26 and week 52]

  7. • Time to an objectified clinical relapse [over 52 weeks]

  8. • Time to treatment optimization [over 52 weeks]

  9. • Time to treatment discontinuation [over 52 weeks]

  10. • Patients experience and satisfaction score with switching to SC therapy by week 6 or 8, week 24 or 26 and by week 52 or 54. [week 6 or 8, week 24 or 26 and week 52 or 54]

    Patients who switched to subcutaneous infliximab will be asked to answer a satisfaction questionnaire about the subcutaneous administration at each on site visit. This questionnaire involves questions whit answers on a scale from 1 to 10.

  11. • The number of eligible patients willing to switch and effectively switching to SC therapy [week 0]

  12. • Identification of reasons for willing or not willing to switch to SC therapy [week 0]

    During the inclusion visit, patients will be asked why they are willing or not willing to switch to SC infliximab. This is a descriptive outcome.

  13. • Identification of reasons for treatment optimization (clinical disease activity, biological disease activity, endoscopic disease activity, radiological disease activity, and/or other) [over 52 weeks]

    During the study, it is possible that the patient will need a treatment optimization as sometimes needed in standard of care. The number of patients needing a treatment optimization will be checked as well as the reason for this treatment optimization (descriptive)

  14. • Identification of reasons for treatment discontinuation (clinical disease activity, biological disease activity, endoscopic disease activity, radiological disease activity, adverse events, pregnancy, patient's request, and/or other) [over 52 weeks]

    During the study, it is possible that the patient will need to discontinue the infliximab treatment as sometimes needed in standard of care. The number of patients undergoing a treatment discontinuation will be checked as well as the reason for this treatment discontinuation (descriptive)

  15. • The number and type of (serious) adverse events by week 52 or 54 [week 52 or 54]

Other Outcome Measures

  1. The association of infliximab trough level and antibody level (if available) at screening to the maintenance of clinical and biological remission after switch to SC infliximab. [Between week 0 and week 52]

  2. The association of the IV dosing schedule to the maintenance of clinical and biological remission after switch to SC infliximab. [Between week 0 and week 52]

  3. The total cost of infliximab therapy [Between week 0 and week 52]

  4. The quality-adjusted life years [Between week 0 and week 52]

  5. The total cost to quality-adjusted life year ratio [Between week 0 and week 52]

Eligibility Criteria

Criteria

Ages Eligible for Study:
18 Years and Older
Sexes Eligible for Study:
All
Accepts Healthy Volunteers:
No
Inclusion Criteria:
  • Voluntary written informed consent of the participant or their legally authorized representative has been obtained prior to any Screening procedures.

  • Patients with a previously documented CD, UC, IBDU diagnosis confirmed by clinical, endoscopic, histological, and/or radiological criteria

  • Males and females ≥18 years old.

  • Patients must be in steroid-free clinical remission at Screening defined as a rectal bleeding score of 0 and a stool frequency score of ≤1 for patients with UC / IBDU, or an average daily abdominal pain score ≤1 and a liquid stool frequency score ≤2.8 for patients with CD (based on the 3 days before the screening visit, excluding the day of or the day before an eventual endoscopy with bowel preparation) and this without the need for any type of steroids in the previous eight weeks.

  • Patients must be in biological remission at screening defined as a CRP <10 mg/L and a fecal calprotectin <250 µg/g.

  • Patients receiving IV infliximab for at least 26 consecutive weeks.

  • Patients receiving IV infliximab at a dose of ~5 mg/kg every 6 weeks or every 4 weeks, ~7.5 mg/kg every 6 weeks or every 4 weeks, or ~10 mg/kg every 8 weeks, every 6 weeks or every 4 weeks where the IV dosing schedule has remained stable for at least twenty weeks;

  • Patients who speak and read fluently Dutch, French or English.

Exclusion Criteria:
  • Male or female ≤ 18 years

  • Patients with an ileorectal anastomosis, an ileal pouch-anal anastomosis or an ostomy

  • Patients participating in an interventional clinical trial with an Investigational Medicinal Product (IMP) or device

  • Patients previously treated with SC infliximab

  • Patients with active perianal fistulizing disease

  • Patients with microscopic colitis

Contacts and Locations

Locations

No locations specified.

Sponsors and Collaborators

  • Belgian Inflammatory Bowel Disease Research and Development (BIRD) VZW
  • Celltrion

Investigators

  • Principal Investigator: Tom Holvoet, MD, PhD, Department of Gastroenterology, VITAZ Sint-Niklaas
  • Principal Investigator: Annick Moens, MD, PhD, Department of Gastroenterology Heilig Hartziekenhuis Lier

Study Documents (Full-Text)

None provided.

More Information

Additional Information:

Publications

None provided.
Responsible Party:
Belgian Inflammatory Bowel Disease Research and Development (BIRD) VZW
ClinicalTrials.gov Identifier:
NCT06113913
Other Study ID Numbers:
  • BIRD2023001
First Posted:
Nov 2, 2023
Last Update Posted:
Nov 2, 2023
Last Verified:
Oct 1, 2023
Individual Participant Data (IPD) Sharing Statement:
No
Plan to Share IPD:
No
Studies a U.S. FDA-regulated Drug Product:
No
Studies a U.S. FDA-regulated Device Product:
No
Keywords provided by Belgian Inflammatory Bowel Disease Research and Development (BIRD) VZW
Additional relevant MeSH terms:

Study Results

No Results Posted as of Nov 2, 2023