A randomized, double-blind, placebo-controlled, multicenter phase III study to evaluate the efficacy and safety of ABX464 once daily for induction treatment in subjects with moderately to severely active ulcerative colitis
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A constituent unit of Datta Meghe Institute of Medical Sciences (Deemed University), Sawangi (Meghe) - 442004 Wardha MAHARASHTRA
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Dr Vineet Ahuja
All India Institute of Medical Sciences
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Dr Pankaj Puri
Fortis Escorts Heart Institute
Escorts Heart Institute and Research Centre Ltd, Okhla Road, New Delhi - 110025 New Delhi DELHI
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Dr Shravan Kumar Porika
Gandhi Hospital
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Dr Chandan Kumar Kedarisetty
Gleneagles Global Hospital
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Dr Saumin Prakashbhai Shah
Gujarat Hospital-Gastro and Vascular Centre
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International Gastro Institute- Isha Hospital
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Dr Abraham Koshy
Lakeshore Hospital &. Research Centre Ltd
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Dr Meghraj Ananda Ingle
Lokmanya Tilak Muncipal Medical College and Lokmanya Tilak Municipal General Hospital
Department of Gestroentrology, Sion -400022, , India Mumbai (Suburban) MAHARASHTRA
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Dr Vivek Bhatia
Maharaja Agrasen Hospital
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Dr Mohammed Aejaz Habeeb
Origin Hospital Centre
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Dr Usha Dutta
Postgraduate Institute of Medical Education and Research
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Dr Rajiv Manhar Mehta
SIDS Hospital and Research Centre
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Dr Balakrishnan Siddhartha Ramakrishna
SRM Institutes for Medical Science
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Dr Hamsraj Alva
Vinaya Hospital and Research Centre
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Dr Praveen Mathew
Vydehi Institution of Sciences and Research Centre
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DrKiran Kumar Peddi
Yashoda Hospitals
Raj Bhavan Road, Somajiguda, -500082, , India Hyderabad TELANGANA
A subject will be eligible to participate in this study if ALL the following criteria are met:
1. Men or women at least 16 years old; Adolescent subjects will only be enrolled if approved by the country regulatory/health authority. If these approvals have not been granted, only subjects ≥ 18 years old will be enrolled. To be eligible, adolescent subjects must weight ≥ 40 kg and meet the definition of Tanner Stage 5 at the screening visit.
2. Subjects must understand, sign and date the written voluntary informed consent form at the visit prior to any protocol-specific procedures. For under-aged subjects, national requirements regarding consent should also be met.
3. Documented diagnosis of UC confirmed by endoscopy and histology. Should histology results not be available at screening, results from biopsies taken at screening may be used.
4. Active disease defined by modified Mayo score (MMS) ≥ 5 with rectal bleeding subscore (RBS) ≥ 1 and endoscopy subscore (MES) of 2 or 3 (confirmed by central reader).
5. Subjects with documented inadequate response (defined as lack of response or loss of response or intolerance) to at least one of the following treatments: corticosteroids, immunosuppressant, biologic therapies, S1P receptor modulators and/or JAK inhibitors and/or new drugs approved during the study (note: failure to only 5-ASA is not accepted).
a. Inadequate response to corticosteroids (CS) is defined as either a CS resistance (i.e., signs and symptoms of persistently active disease despite current or prior course of oral prednisone/prednisolone ≥ 40 mg/d for at least 2 weeks, or to budesonide ≥ 9 mg/d for at least 2 weeks, or to beclomethasone ≥ 5 mg/d for at least 2 weeks) or a CS dependence (i.e., failure to taper to ≤10 mg of prednisone/prednisolone, < 9 mg/d of budesonide or < 5 mg of beclomethasone or relapse occurring within 3 months after stopping CS).
Intolerance to CS includes (but not limited to) Cushing’s syndrome, osteopenia/osteoporosis, hyperglycemia, insomnia, infection.
b. Inadequate response to immunosuppressants is defined as signs and symptoms of persistently active disease despite azathioprine treatment at 1.5 to 2.5 mg/kg/day for at least 8 weeks, or mercaptopurine 0.5 to 1.5 mg/kg/day for at least 8 weeks, or methotrexate 12.5 mg to 15 mg/week for at least 8 weeks
Intolerance to immunosuppressant includes (but not limited to) nausea/vomiting, abdominal pain, pancreatitis, liver enzyme abnormalities, lymphopenia, infection.
c. Inadequate response to biologics is defined as:
• Primary non responders to full induction course as in the USPI/SmPC of the following:
- infliximab or biosimilars (≥ 5 mg/kg intravenously at 0, 2, and 6 weeks),
- adalimumab or biosimilars (160 mg subcutaneous dose followed by 80 mg SC [or 80 mg SC dose in countries where this dosing regimen is allowed] followed by 40 mg SC dose at least 2 weeks apart),
- golimumab (200 mg SC dose followed by 100 mg SC dose at least 2 weeks apart),
- vedolizumab (300 mg IV at 0, 2, and 6 weeks),
- ustekinumab (one single IV using weight-based dosing - 260 mg for subjects with body ≤ 55 kg; 390 mg for subjects with body weight > 55 kg and ≤ 85 kg; 520 mg for subjects with body weight > 85 kg),
• Loss of response is defined as recurrence of symptoms during maintenance course following primary response after full induction course (discontinuation despite clinical benefit does not qualify)
Intolerance includes (but not limited to) infusion-related reaction, serious opportunistic infection, malignancies.
d. Inadequate response to JAK inhibitors is defined as signs and symptoms of persistently active disease despite at least one full induction course according to USPI/SmPC of tofacitinib (i.e., at least 8 weeks), or to at least one full induction course according to SmPC of filgotinib (i.e., at least 10 weeks), or to at least one full induction course according to USPI of upadacitinib (i.e., 8 weeks), or recurrence of symptoms during maintenance course.
Intolerance to JAK inhibitor treatment that includes (but not limited to) increase of serious infection, malignancies, deep venous thrombosis (DVT), or major adverse cardiac event (MACE).
e. Inadequate response to S1P receptor modulators is defined as signs and symptoms of persistently active disease despite at least one full induction course according to USPI/SmPC of ozanimod (i.e., at least 12 weeks) or recurrence of symptoms during maintenance course.
Intolerance to ozanimod that includes (but not limited to) serious infections, liver enzyme, cardiac abnormalities, lymphopenia.
f. Inadequate response or intolerance to any new drug approved for moderate to severe active UC during the course of the study defined according to USPI/SmPC.
6. Women of childbearing potential (WOCBP) subjects and male subjects with WOCBP partner must agree to use highly effective contraception methods as stated in Section 4.4. (Contraception) of this protocol.
7. Subjects able and willing to comply with study visits and procedures as per protocol.
8. Subjects should be affiliated to a health insurance policy whenever required by a participating country or state.
ExclusionCriteria
Details
Subjects who meet ANY of the following exclusion criteria will be excluded from the study:
1. Subjects with ulcerative colitis limited to an isolated proctitis (≤ 15cm from anal verge).
2. Subjects with primary sclerosing cholangitis or autoimmune hepatitis.
3. Subjects who have failed on 5-ASA therapy only.
4. Subjects with CD or presence or history of fistula, indeterminate colitis, infectious/ischemic colitis or microscopic colitis (lymphocytic and collagenous colitis).
5. History or current evidence of toxic megacolon, fulminant colitis, bowel perforation.
6. History of colon cancer, past or current evidence of low grade or high-grade colonic dysplasia and/or adenomatous polyps that have not been completely removed.
7. Recent or planned bowel surgery or history of proctocolectomy or partial colectomy or current stoma.
8. Subjects on antidiarrheals including those working on motility (e.g., loperamide, diphenoxylate with atropine, etc.).
9. Subjects on probiotics (e.g., Culturelle® [Lactobacillus GG, i-Health, Inc.], Saccharomyces boulardii).
10. Subjects who do not meet the washout period requirements prior to the screening endoscopy as described in the prohibited medication section (section 4.3.2) of the study protocol.
11. Subjects with the following hematological and biochemical laboratory parameters obtained during the screening period:
• Hemoglobin ≤ 8.0 g dL-1
• Absolute neutrophil count < 750 mm-3
• Platelets < 100,000 mm-3
• Creatinine clearance < 60 mL.min-1 (Cockroft-Gault formula)
• Total serum bilirubin > 1.5 x ULN
• Alkaline phosphatase, aspartate aminotransferase (AST) and alanine aminotransferase (ALT) > 2 x ULN
12. Subjects with the following conditions (infection):
• Subjects with chronic or recurrent grade 3 or grade 4 infection within the last 2 months prior to screening or a history of opportunistic infection while not on immunosuppressive therapy.
• Herpes zoster reactivation within the last 2 months prior to screening.
• Subjects with active infection at screening or any major episode of infection that required hospitalization or treatment with intravenous antibiotics within 1 month of screening or during screening. Fungal infection of nail beds is allowed.
• Positive assay or stool culture for pathogens (ova and parasite examination, bacteria) or positive test for Clostridium difficile toxin at screening. If C. difficile is positive, subject may be treated and retested ≥ 2 weeks after completing treatment.
• Subjects with HIV infection.
• Subjects having acute or chronic hepatitis B infection at screening (positive for hepatitis B surface antigen [HbsAg], or negative for HbsAg and positive for anti-hepatitis B core antibody in conjunction with detectable HBV DNA, or detectable HBV DNA).
• Subjects having acute or chronic hepatitis C infection at screening as defined by positive for hepatitis C antibody (subjects successfully treated and without recurrence ≥ 1 year with no detectable HCV RNA [assessed centrally] are eligible).
• Active tuberculosis (TB) or untreated latent TB are ruled out. For subjects with positive or intermediate QuantiFERON test see section 5.3.8.1 of the current study protocol
13. Subjects with an uncontrolled ischemic heart disease and/or a history of congestive heart failure with New York Heart Association (NYHA) class 3 or 4 symptoms.
14. Subjects with a family or personal history of congenital or acquired long QT syndrome, or subjects with a marked baseline prolongation of QT/QTc interval (e.g., repeated demonstration of a QTc interval [Fridericia or Bazett correction] >450 milliseconds for male and > 460 milliseconds for female).
15. Subjects with a history of torsade de pointe (TdP).
16. Acute or chronic of clinically relevant pulmonary, hepatic, pancreatic or renal functional abnormality, encephalopathy, neuropathy or unstable central nervous system pathology such as seizure disorder, or any other clinically significant medical problems as determined by physical examination and/or laboratory screening tests and/or medical history (note: treated autoimmune hypothyroidy and autoimmune diabetes are allowed).
17. History or active malignancy (subjects with a 5-year disease free survival are eligible).
18. Serious illness requiring hospitalization within 4 weeks prior to screening (except UC flare).
19. Subjects previously treated with ABX464.
20. WOCBP subject and WOCBP partner of male subject who are pregnant at screening, intend or are planning to become pregnant during the study duration, and breast-feeding women.
21. Illicit drug or alcohol abuse or dependence.
22. Subjects who received live vaccine within 3 months prior to screening and/or who’s planning to receive such a vaccine during the study duration.
23. Use of any investigational or non-registered product within 3 months or within 5 half-lives preceding baseline, whichever is longer, and during the study.
24. Any condition, which in the opinion of the investigator, could compromise the subject’s safety or adherence to the study protocol
Method of Generating Random Sequence
Other
Method of Concealment
Other
Blinding/Masking
Participant and Investigator Blinded
Primary Outcome
Outcome
TimePoints
The primary objective is to compare the efficacy of ABX464 versus placebo on clinical remission
• To compare the efficacy of obefazimod versus placebo on endoscopic improvement.
• To compare the efficacy of obefazimod versus placebo on clinical response.
• To compare the efficacy of obefazimod versus placebo on HEMI.
•To compare the efficacy of ABX464 versus placebo on clinical response as per MMS
•To compare the efficacy of ABX464 versus placebo on symptomatic remission.
•To compare the efficacy of ABX464 versus placebo on histologic-endoscopic mucosal improvement (HEMI).
•Proportion of subjects who achieve endoscopic improvement at week 8.
•Proportion of subjects who achieve clinical response per MMS at week 8.
•Proportion of subjects with symptomatic remission at week 8.
•Proportion of subjects with HEMI per Geboes scoring at week 8.
Target Sample Size
Total Sample Size="612" Sample Size from India="40" Final Enrollment numbers achieved (Total)= "Applicable only for Completed/Terminated trials" Final Enrollment numbers achieved (India)="Applicable only for Completed/Terminated trials"
Individual Participant Data (IPD) Sharing Statement
Will individual participant data (IPD) be shared publicly (including data dictionaries)?
Response - NO
Brief Summary
This is a multicenter, randomized,
placebo controlled study to evaluate the efficacy and safety of ABX464 given at
25 or 50 mg QD in inducing clinical remission in subjects with moderately to
severely active ulcerative colitis who have inadequate response, no response, a
loss of response, or an intolerance to either conventional therapies
[corticosteroids, immunosuppressant (i.e. azathioprine, 6-mercaptopurine,
methotrexate)] and/or advanced therapies [biologics (TNF inhibitors,
anti-integrins, anti-IL-23), and/or S1P receptor modulators, and/or JAK
inhibitors].
As shown below, this study consists
of a screening period of up to 28 days, an 8-week induction period followed by
28-day follow up period. Subjects who complete the 8-week induction will be
given the opportunity to take part in the maintenance study (i.e. ABX464-107)
either:
·In the randomized double-blind placebo-controlled
study part [part 1; placebo, 25 mg, 50 mg] for clinical responders at week 8.
·In the randomized open label arms study part
[part 2; 25 mg or 50 mg] for non-clinical responders at week 8.
Approximately 612 subjects, aged at
least 16 years, will be randomized in this study.
On Day 1, eligible subjects will be
randomized and allocated into three treatment arms according to ratio 1:1:2 as
follows:
·Placebo: 153 subjects
·ABX464 –
Daily dose 25 mg QD: 153 subjects
·ABX464 –
Daily dose 50 mg QD: 306 subjects
Randomization will be stratified
according to the following factors:
·Subjects with inadequate response to advanced
therapies [AT-IR subjects] (no response, loss of response or intolerance to
biologics, S1P receptor modulators, JAK inhibitors) (Yes/No)
·Subjects with concomitant corticosteroids at
baseline (Yes/No)
·Japanese subjects or non- Japanese subjects
Approximately 60% of the enrolled
population should be subjects with inadequate response to Advanced Therapies
(biologics, S1P receptor modulators, JAK inhibitors). In addition, percentage
of subjects who have failed to JAK inhibitors should be limited to 15% of
subjects with inadequate response to Advanced Therapies.
Subjects with previous exposure to
Advanced Therapies without a documented inadequate response will be considered
as non-AT-IR subjects.
Following Day 1 (randomization
day), subjects will come at the investigational site at Day 28 (Week 4) and Day
56 (Week 8) according to the study schedule of assessments.
At Day 56, subjects will be given the choice to
either take part in the maintenance study (ABX464 107) or to end their
participation in the present induction study by completing the study. For the
latter option, subjects will return for an end of study visit 28 days after the
last study drug intake. However, subjects who are eligible for the maintenance
study should be encouraged to enter the maintenance study