- Nowak, Richard J;
- Coffey, Christopher S;
- Goldstein, Jonathan M;
- Dimachkie, Mazen M;
- Benatar, Michael;
- Kissel, John T;
- Wolfe, Gil I;
- Burns, Ted M;
- Freimer, Miriam L;
- Nations, Sharon;
- Granit, Volkan;
- Smith, A Gordon;
- Richman, David P;
- Ciafaloni, Emma;
- Al-Lozi, Muhammad T;
- Sams, Laura Ann;
- Quan, Dianna;
- Ubogu, Eroboghene;
- Pearson, Brenda;
- Sharma, Aditi;
- Yankey, Jon W;
- Uribe, Liz;
- Shy, Michael;
- Amato, Anthony A;
- Conwit, Robin;
- O'Connor, Kevin C;
- Hafler, David A;
- Cudkowicz, Merit E;
- Barohn, Richard J;
- Team, on behalf of the NeuroNEXT NN103 BeatMG Study
Objective
To determine whether rituximab is safe and potentially beneficial, warranting further investigation in an efficacy trial for acetylcholine receptor antibody-positive generalized MG (AChR-Ab+ gMG).Methods
The B-Cell Targeted Treatment in MG (BeatMG) study was a randomized, double-blind, placebo-controlled, multicenter phase-2 trial that utilized a futility design. Individuals 21-90 years of age, with AChR-Ab+ gMG (MG Foundation of America Class II-IV) and receiving prednisone ≥15 mg/day were eligible. The primary outcome was a measure of steroid-sparing effect, defined as the proportion achieving ≥75% reduction in mean daily prednisone dose in the 4-weeks prior to week 52 and with clinical improvement or no significant worsening as compared to the 4-week period prior to randomization. The co-primary outcome was safety. Secondary outcomes included MG-specific clinical assessments. Fifty-two individuals were randomized (1:1) to either a two-cycle rituximab/placebo regimen, with follow-up through 52-weeks.Results
Of the 52 participants included, mean (±SD) age at enrollment was 55.1 (±17.1) years; 23 (44.2%) were female, and 31 (59.6%) were MGFA Class II. The mean (±SD) baseline prednisone dose was 22.1 (±9.7) mg/day. The primary steroid-sparing outcome was achieved in 60% of those on rituximab vs. 56% on placebo. The study reached its futility endpoint (p=0.03) suggesting that the pre-defined clinically meaningful improvement of 30% due to rituximab over placebo was unlikely to be achieved in a subsequent, larger trial. No safety issues identified.Conclusions
While rituximab was safe and well-tolerated, these results suggest that there is a low probability of observing the defined clinically meaningful steroid-sparing effect over a 12-month period in a phase-3 trial of mild-moderately symptomatic AChR-Ab+ gMG.Classification of evidence
This study provides Class I evidence that for mild-to-moderate AChR-Ab+ gMG, compared with placebo, rituximab is safe but unlikely to reduce steroid use by an absolute difference of at least 30% at 1 year.Trial registration
ClinicalTrials.gov Identifier: NCT02110706.