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DEFINE

Determination of the Efficacy and Safety of Oral Fumarate in Relapsing–Remitting MS

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Year of Publication: 2012

Authors: Ralf Gold, Ludwig Kappos, Douglas L. Arnold, ..., for the DEFINE Study Investigators

Journal: New England Journal of Medicine

Citation: N Engl J Med 2012;367:1098-107

Link: https://clinicaltrials.gov/ct2/show/NCT00420212

PDF: https://www.nejm.org/doi/pdf/10.1056/NEJMoa1114287

Clinical Question

Does oral BG-12 (dimethyl fumarate) reduce relapse rates and disability progression compared to placebo in patients with relapsing-remitting multiple sclerosis?

Bottom Line

Both BG-12 regimens (240 mg twice daily and 240 mg three times daily) significantly reduced the proportion of patients with relapse, annualized relapse rate, disability progression, and MRI lesion burden compared to placebo in RRMS patients over 2 years.

Major Points

  • BG-12 reduced the proportion of patients with relapse at 2 years by approximately 50% compared to placebo (27% and 26% vs 46%)
  • Annualized relapse rate was reduced by 53% (twice-daily) and 48% (thrice-daily) compared to placebo
  • Risk of confirmed disability progression sustained for 12 weeks was reduced by 38% (twice-daily) and 34% (thrice-daily)
  • New or enlarging T2 lesions were reduced by 85% (twice-daily) and 74% (thrice-daily)
  • Gadolinium-enhancing lesions were reduced by 90% (twice-daily) and 73% (thrice-daily)
  • Main adverse events were flushing and gastrointestinal symptoms, highest in first month
  • Lymphocyte counts decreased by approximately 28% at 1 year but remained within normal limits
  • No opportunistic infections were observed

Design

Study Type: Randomized, double-blind, placebo-controlled phase 3 trial

Randomization: 1

Blinding: Double-blind; separate examining and treating neurologists at each site remained unaware of assignments; patients instructed to take study drug at least 4 hours before visits to avoid revealing flushing

Follow-up Duration: 2 years (96 weeks)

Centers: 198

Countries: 28 countries (not individually specified)

Sample Size: 1234

Analysis: Intention-to-treat; Cox proportional-hazards model for primary endpoint adjusted for baseline EDSS, age, region, and number of relapses in year before entry; negative binomial regression for ARR; sequential closed testing procedure to control type I error

Inclusion Criteria

  • Age 18 to 55 years
  • Diagnosis of relapsing-remitting multiple sclerosis per McDonald criteria
  • Baseline EDSS score of 0 to 5.0
  • At least one clinically documented relapse within 12 months before randomization OR
  • Brain MRI scan within 6 weeks before randomization showing at least one gadolinium-enhancing lesion

Exclusion Criteria

  • Progressive forms of multiple sclerosis
  • Another major disease that would preclude participation in a clinical trial
  • Abnormal results on prespecified laboratory tests
  • Recent exposure to contraindicated medications

Baseline Characteristics

Placebo:

  • N: 408
  • Age - years: 38.5 ± 9.1
  • Female sex: 306 (75%)
  • Weight - kg: 71.1 ± 17.0
  • Race - White: 318 (78%)
  • Race - Asian: 42 (10%)
  • Race - Black: 8 (2%)
  • Race - Other or unknown: 40 (10%)
  • Previous use of approved MS medication: 172 (42%)
  • Time since diagnosis - years: 5.8 ± 5.8
  • Relapses in previous 12 months: 1.3 ± 0.7
  • EDSS score 0: 21 (5%)
  • EDSS score 1.0 or 1.5: 105 (26%)
  • EDSS score 2.0 or 2.5: 112 (27%)
  • EDSS score 3.0 or 3.5: 97 (24%)
  • EDSS score 4.0 or 4.5: 56 (14%)
  • EDSS score 5.0: 16 (4%)
  • Mean EDSS score: 2.48 ± 1.24
  • Gadolinium-enhancing T1 lesions - no.: 1.6 ± 3.4
  • Hyperintense T2 lesions - mean no.: 49.2 ± 38.6

BG-12 Twice Daily:

  • N: 410
  • Age - years: 38.1 ± 9.1
  • Female sex: 296 (72%)
  • Weight - kg: 70.7 ± 18.5
  • Race - White: 321 (78%)
  • Race - Asian: 38 (9%)
  • Race - Black: 8 (2%)
  • Race - Other or unknown: 43 (10%)
  • Previous use of approved MS medication: 162 (40%)
  • Time since diagnosis - years: 5.6 ± 5.4
  • Relapses in previous 12 months: 1.3 ± 0.7
  • EDSS score 0: 29 (7%)
  • EDSS score 1.0 or 1.5: 109 (27%)
  • EDSS score 2.0 or 2.5: 116 (28%)
  • EDSS score 3.0 or 3.5: 82 (20%)
  • EDSS score 4.0 or 4.5: 56 (14%)
  • EDSS score 5.0: 16 (4%)
  • Mean EDSS score: 2.40 ± 1.29
  • Gadolinium-enhancing T1 lesions - no.: 1.2 ± 3.3
  • Hyperintense T2 lesions - mean no.: 47.6 ± 34.7

BG-12 Thrice Daily:

  • N: 416
  • Age - years: 38.8 ± 8.8
  • Female sex: 306 (74%)
  • Weight - kg: 71.3 ± 16.9
  • Race - White: 330 (79%)
  • Race - Asian: 36 (9%)
  • Race - Black: 10 (2%)
  • Race - Other or unknown: 40 (10%)
  • Previous use of approved MS medication: 168 (40%)
  • Time since diagnosis - years: 5.1 ± 5.3
  • Relapses in previous 12 months: 1.3 ± 0.6
  • EDSS score 0: 24 (6%)
  • EDSS score 1.0 or 1.5: 104 (25%)
  • EDSS score 2.0 or 2.5: 146 (35%)
  • EDSS score 3.0 or 3.5: 85 (20%)
  • EDSS score 4.0 or 4.5: 42 (10%)
  • EDSS score 5.0: 14 (3%)
  • Mean EDSS score: 2.36 ± 1.19
  • Gadolinium-enhancing T1 lesions - no.: 1.2 ± 4.1
  • Hyperintense T2 lesions - mean no.: 55.8 ± 44.3

Arms

FieldControlBG-12 Twice DailyBG-12 Thrice Daily
InterventionMatching placeboBG-12 (dimethyl fumarate) 240 mg orally twice dailyBG-12 (dimethyl fumarate) 240 mg orally three times daily
Duration96 weeks96 weeks96 weeks

Outcomes

OutcomeTypeControlInterventionHR / OR / RRP-value
Proportion of patients who had a relapse by 2 years (protocol-defined relapses confirmed by independent neurologic evaluation committee)Primary46%<0.001 for both comparisons
Annualized relapse rate at 2 yearsSecondary0.36 (95% CI 0.30–0.44)<0.001 for both
Confirmed disability progression sustained for 12 weeks at 2 yearsSecondary27%
New or newly enlarging T2-weighted hyperintense lesions at 2 yearsSecondary17.0 adjusted mean (95% CI 12.9–22.4)<0.001 for both
Gadolinium-enhancing T1-weighted lesions at 2 yearsSecondary1.8 ± 4.2<0.001 for both
Patients free from gadolinium-enhancing lesions at 2 yearsSecondary62%
Time to first relapse (25th percentile)Secondary38 weeks
Any adverse eventAdverse387 (95%)
FlushingAdverse20 (5%)
MS relapseAdverse189 (46%)
DiarrheaAdverse55 (13%)
NauseaAdverse38 (9%)
Upper abdominal painAdverse28 (7%)
ProteinuriaAdverse34 (8%)
Abdominal painAdverse22 (5%)
PruritusAdverse19 (5%)
VomitingAdverse24 (6%)
Adverse events leading to discontinuationAdverse55 (13%)
Any serious adverse eventAdverse86 (21%)
Serious infectionAdverse7 (2%)
Malignant neoplasmAdverse2 (<1%)
DeathAdverse0
White-cell count <3.0×10^9/L or lymphocyte count <0.5×10^9/LAdverse≤1%
ALT ≥3× ULNAdverse3%

Subgroup Analysis

Not detailed in main publication

Criticisms

  • No active comparator arm - comparison to approved MS therapies requires cross-trial comparisons
  • MRI cohort was a subgroup (540 patients) rather than the full study population
  • Approximately 23% of patients withdrew from the study, though balanced across groups
  • Unknown long-term safety profile beyond 2 years
  • Both BG-12 doses showed similar efficacy, leaving optimal dosing unclear
  • Cannot determine whether therapeutic effect stems predominantly from immunomodulatory or neuroprotective mechanisms
  • Short duration may not capture full disability progression effects

Funding

Biogen Idec

Based on: DEFINE (New England Journal of Medicine, 2012)

Authors: Ralf Gold, Ludwig Kappos, Douglas L. Arnold, ..., for the DEFINE Study Investigators

Citation: N Engl J Med 2012;367:1098-107

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