Crohn's Disease Clinical Trial
Official title:
A Multi-Center, Double-Blind Study to Evaluate the Safety, Efficacy and Pharmacokinetics of the Human Anti-TNF Monoclonal Antibody Adalimumab in Pediatric Subjects With Moderate to Severe Crohn's Disease
The purpose of this study is to determine Efficacy, Pharmacokinetics, and Safety of Adalimumab in Pediatric Subjects With Moderate to Severe Crohn's Disease
M06-806 (NCT # NCT00409682) was a Phase 3, multi-center, randomized, double-blind (DB),
efficacy, safety, and pharmacokinetic (PK) study designed to evaluate the efficacy of 2 dose
regimens for the induction and maintenance of clinical remission in pediatric subjects
between the ages of 6 and 17 (inclusive) with moderate to severe Crohn's disease (CD)
(defined by Pediatric Crohn's Disease Activity Index [PCDAI > 30]). Subjects must have
either failed conventional therapy for CD or have previously received infliximab and lost
response/had intolerance to infliximab.
Approximately 186 pediatric subjects between the ages of 6 and 17 were planned to be entered
into the study at approximately 55 sites in the US, Canada, and Europe. At least 80 subjects
were to be ≥ 13 years old at Baseline and one-third to one-half of the study population were
to be subjects who had previously lost response or were intolerant to infliximab.
The duration of the study was to be up to 65 weeks, which included a 1- to 3-week Screening
period, an Induction period, a Maintenance period, and a 70-day follow-up phone call for all
subjects that either terminated early from the study or did not rollover into the extension
study ([NCT # 00686374], to evaluate the long-term maintenance of clinical response, safety,
and tolerability of repeated administration of adalimumab).
All subjects received an induction regimen administered at Baseline (Week 0) and Week 2. The
open-label (OL) induction dose was based on the subject's Baseline body weight. Subjects
weighing ≥ 40 kg were to receive 160 mg at Week 0 and 80 mg adalimumab at Week 2. Subjects
weighing < 40 kg were to receive 80 mg at Week 0 and 40 mg adalimumab at Week 2.
At Week 4, subjects were to be randomized 1:1 to 1 of 2 DB maintenance treatment groups
(Low-Dose or High-Dose), stratified by Week 4 clinical responder status (clinical response
was defined as decrease in PCDAI of ≥ 15 points from the Baseline score), body weight at
Week 4 and prior exposure to infliximab. Subjects randomized to the High-Dose treatment
group were to receive either 40 mg adalimumab subcutaneous (SC) every other week (eow) (if
Week 4 body weight ≥ 40 kg) or 20 mg adalimumab SC eow (if Week 4 body weight < 40 kg).
Subjects randomized to the Low-Dose treatment group were to receive either 20 mg adalimumab
SC eow (if Week 4 body weight ≥ 40 kg) or 10 mg adalimumab SC eow (if Week 4 body weight <
40 kg).
Subject's body weight taken at Week 26 was to be used to readjust the maintenance dosing
regimen for a subject whose body weight had increased from < 40 kg to ≥ 40 kg during the
study.
Subjects were expected to remain on blinded eow therapy throughout the 48-week study DB
Maintenance period. However, starting at the Week 12 study visit, subjects who experienced a
disease flare (increase in the PCDAI ≥ 15 points when compared to Week 4 and an absolute
PCDAI above 30) or were non-responders (not achieving a decrease in the PCDAI score of at
least 15 points when compared to the Baseline score for 2 consecutive visits at least 2
weeks apart) could be switched from blinded eow dosing to blinded every week (ew) dosing,
continuing with the same blinded dose. During blinded ew treatment, if a subject continued
to experience a flare or met the definition of non-response following an 8 week course of DB
ew therapy, they were to be switched to OL ew therapy. The dosage of the OL ew therapy was
20 mg for subjects < 40 kg and 40 mg for subjects ≥ 40 kg.
This study used the PCDAI to determine efficacy of the study drug. The primary efficacy
endpoint is the proportion of subjects who are in clinical remission at Week 26, as measured
by the PCDAI in the intent-to-treat population. Clinical remission is defined as a PCDAI
score of ≤ 10.
The clinical response indicators include clinical remission as defined by PCDAI score at
Week 52 and clinical response as defined by PCDAI score at Week 26 and at Week 52.
The patient reported outcome is the change from Baseline in total IMPACT III scores at Week
26 and Week 52.
The safety parameters (adverse events, laboratory data, and vital signs) were assessed at
all visits throughout the study.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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