Reduce Risk for Crohn's Disease Patients

Phase 4

Completed

• Conditions: Crohn's Disease
• Interventions: Drug: Methotrexate; Drug: Azathioprine / 6 Mercaptopurine; Drug: Adalimumab

• Registration Number: NCT02852694
• Lead Sponsor: PIBD-Net

Brief Summary

The purpose of this study is to compare the effectiveness of weekly subcutaneously administered Methotrexate for maintaining relapse-free sustained steroid/Enteral Nutrition -free 1-year remission compared with:

* daily oral Azathioprine / 6 mercaptopurine in low risk paediatric Crohn's disease

* subcutaneously administered adalimumab in high risk paediatric Crohn's disease

Detailed Description

In this randomized controlled trial PIBDNet (pediatric inflammatory bowel diseases network) aims to compare the following treatment strategy by dividing patients into two risk groups for aggressive disease evolution: the effectiveness of Methotrexate versus Azathioprine / 6 mercaptopurine for the maintenance of remission in Crohn's disease in children who are at low risk for aggressive disease and the effectiveness of Methotrexate versus adalimumab in the high risk group. PIBDNet hypothesizes that Methotrexate is superior to Azathioprine / 6 mercaptopurine for maintaining remission in Crohn's disease in the low risk strata and adalimumab is superior to Methotrexate in the high risk strata. In addition, the ancillary study is planned to analyse of Adalimumab treated patients from inclusion (TOP-Down) versus patients switched to Adalimumab due to failure of immunomodulator therapy (STEP-Up).

Study Timeline

• Study First Submitted: 2016-06-09
• Study First Submitted QC: 2016-07-28
• Study First Posted: 2016-08-02
• Study Start: 2017-02-28
• Primary Completion: 2021-06-14
• Study Completion: 2021-06-14
• Status Verified: 2025-01
• Last Update Submitted: 2025-01-29
• Last Update Posted: 2025-01-31

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 192

Inclusion Criteria

1. Children 6-17, with a new-onset Crohn Disease diagnosed using established criteria (37, 38), requiring a steroid-based or Enteral nutrition based induction therapy

2. At initial diagnosis, wPCDAI >40 or CRP>2 times upper limit at diagnosis

3. all wPCDAI scores (0-120) are possible at inclusion (patients in remission and patients with active disease)

4. Luminal active Crohn Disease (B1) with or without B2 and/or B3 disease behavior

5. Initial exposure to 5-ASA and derivate is tolerated

6. Exposure to antibiotics is tolerated

7. If one of the following criteria is present, patients are allocated to the high risk group prior randomization:

   • Complex fistulizing perianal disease
   • Panenteric disease phenotype (defined as L3 with L4b per Paris classification or L3 with deep ulcers in duodenum, stomach or oesophagus (not HP (helicobacter pylori)- or NSAID-related))
   • Severe growth impairment (height z-score <-2 or crossing 2 percentiles or more) likely related to CD
   • Significant hypoalbuminemia (<30g/l), elevated C reactive protein (CRP) (at least 2 times above normal range), or wPCDAI >12.5 despite 3 weeks of optimized induction therapy with steroids or Exclusive enteral nutrition
   • B2, B3 or B2B3 disease behavior
   • Overall cumulative disease extend of ≥60 cm

8. Informed and signed consent

Exclusion Criteria

1. Patients with wPCDAI<42,5 at initial diagnosis, except if CRP>2 times upper limit
2. No induction therapy with steroids or enteral nutrition
3. Previous therapy with any IBD (inflammatory bowel desease) -related medications other than induction therapy as detailed in this protocol (except 5-ASA).
4. Pregnancy or refusal to use contraceptives during the study period in pubertal patients (both boys and girls) unless absolute abstinence (no sexual activity) is confirmed at each study visit. Positive pregnancy testing throughout the study will trigger prompt withdrawal of the patient from the study.
5. Lactating mothers
6. Children with perianal fistulising disease who require surgical therapy (drainage, seton placement)
7. Patients homozygous for Thiopurine methyl transferase or those with Thiopurine methyl transferase activity <6 nmol/h/ml erythrocytes or <9nmol 6MTG (6 methylthioguanine/g Hb/h), unless they qualify as high risk patients
8. Evidence of un-drained and un-controlled abscess/phlegmon
9. Contraindication to any drugs used in the trial (including intolerance/hypersensitivity or allergy to either study drug (thiopurines, methotrexate or adalimumab))
10. Current or previous malignancy
11. Serious comorbidities (such as renal insufficiency, hepatitis, respiratory insufficiency) interfering with drug therapy or interpretation of outcome parameters or will make it unlikely that the patients will finish the trial.
12. Infection with mycobacterium tuberculosis
13. Moderate to severe heart failure (NYHA classe III/IV)
14. Oral anticoagulant therapy, anti-malaria therapy
15. Live vaccines exposure (including yellow fever) less than 3 weeks prior inclusion

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Low risk group	Azathioprine / 6 Mercaptopurine	subcutaneous methotrexate versus oral dose of azathioprine / 6 mercaptopurine
High Risk Group	Methotrexate	subcutaneous methotrexate versus subcutaneous adalimumab
Low risk group	Methotrexate	subcutaneous methotrexate versus oral dose of azathioprine / 6 mercaptopurine
High Risk Group	Adalimumab	subcutaneous methotrexate versus subcutaneous adalimumab
Ancillary	Adalimumab	the ancillary study is planned to analyse of Adalimumab treated patients from inclusion (TOP-Down) versus patients switched to Adalimumab due to failure of immunomodulator therapy (STEP-Up).

Primary Outcome Measures

Name	Time	Method
Rate of sustained steroid/EEN-free remission at Month 12	Month 12	Rate of sustained steroid/EEN-free remission at Month 12, where sustained remission is defined as wPCDAI (weighted pediatric crohn disease activity index) ≤12.5 and CRP ≤1,5 fold the normal upper limit without a relapse since week 12.

Secondary Outcome Measures

Name	Time	Method
Linear height velocity	12 months	the goal is to compare linear height velocity
Steroid sparing effect of the regimens	12 months	the goal is to compare steroid sparing effect of the regimen
Clinical predictors for response, including genomic and serological markers	12 months	Clinical predictors for response to Study treatment will be determined, using genomic and serological markers, such as ASCA.
Questionnaire : School Attendance (patient reported outcome) at month 12	12 months	the goal is to evauate School Attendance questionnaire (patient reported outcome) for all patients at month 12
Time to first relapse	Month 12	the goal is to compare the time of the first relapse
Predictive value of fecal calprotectin levels, CRP and other serum tests	12 months	the goal is to evaluate predictive value of fecal calprotectin levels, CRP and other serum tests
DNA pharmacogenetics (multiplex genotyping of polymorphism in drug metabolism) in relation to toxicity and response to therapy	12 months	the goal is to evaluate DNA pharmacogenetics (multiplex genotyping of polymorphism in drug metabolism) in relation to toxicity and response to therapy
Anti-adalimumab antibodies monitoring : concentration of anti-adalimumab antibodies in relation to adherence, toxicity and response	12 months	the goal is to evaluate anti-adalimumab antibodies monitoring : concentration of anti-adalimumab antibodies in relation to adherence, toxicity and response
Questionnaire : TUMMY-CD (patient reported outcome) at month 12	12 months	the goal is to evaluate questionnaire : TUMMY-CD (patient reported outcome) for all patients patients at month 12
Concentration of protocol drug (ADA or MTX) monitoring in relation to adherence, toxicity and response	12 months	the goal is to evaluate concentration of protocol drug (ADA or MTX) monitoring in relation to adherence, toxicity and response
Questionnaire : health-related life of quality (IMPACT 3) between the different treatment arms	12 months	Health-related life of quality willl be compared between the different treatment arms, based on the IMPACT-III questionnaire, a questionnaire developed for use in pediatric inflammatory bowel disease
Questionnaire : WPAI:CD Caregiver (patient reported outcome) at month 12	12 months	the goal is to evauate WPAI:CD Caregiver (patient reported outcome) for all patients at month 12
Remission at 12 weeks (measured by wPCDAI</=12.5 and normal CRP and being off steroids/exclusive enteral nutrition)	12 weeks	the goal is to compare the remission at 12 weeks
Comparison of toxicity of the different protocol drugs	12 months	Toxicity of the different protocol drugs will be compared using incidence of Adverse Events (AE) and Serious Adverse Events (SAE).
6 Mercaptopurine and azathioprine metabolites monitoring : concentration of metabolites in relation to adherence, toxicity and response	12 months	the goal is to evaluate 6 Mercaptopurine and azathioprine metabolites monitoring : concentration of metabolites in relation to adherence, toxicity and response

Trial Locations

Locations (1)

Hôpital Necker -Enfants Malades (Service de gastro-enterologie); 🇫🇷 Paris, France