BCMA-directed mRNA CAR T cell therapy for myasthenia gravis: a randomized, double-blind, placebo-controlled phase 2b trial

Tuan Vu(University of South Florida), Hacer Durmus(Istanbul University), Michael H. Rivner(Augusta University), Sheetal Shroff(Methodist Hospital), Thomas Ragole(University of Colorado Anschutz Medical Campus), Bennett H. Myers(Dent Neurologic Institute), Mamatha Pasnoor(University of Kansas Medical Center), George Small(Allegheny General Hospital), Chafic Karam(University of Pennsylvania), Mithila Vullaganti(Tufts University), Amanda Peltier(Vanderbilt University), Gregory Sahagian(GlobalFoundries (United States)), Marc H. Feinberg(Boca Raton Regional Hospital), Adam Slanksy(Neurology Associates), Carolina Barnett-Tapia(Toronto General Hospital), Zaeem Siddiqi(University of Alberta), Kelly Gwathmey(Virginia Commonwealth University), Michael Badruddoja(Center for Neurosciences), Hafsa Kamboh(Cara Therapeutics (United States)), Rachel N. Ruggerie(Cara Therapeutics (United States)), Renee Fedak(Cara Therapeutics (United States)), C. Andrew Stewart(Cara Therapeutics (United States)), Metin Kurtoğlu(Cara Therapeutics (United States)), Murat V. Kalayoglu(Cara Therapeutics (United States)), Michael Singer(Cara Therapeutics (United States)), Christopher M. Jewell(Cara Therapeutics (United States)), Miloš D. Miljković(Cara Therapeutics (United States)), Mazen Dimachkie(University of Kansas Medical Center), Tahseen Mozaffar(University of California, Irvine), James F. Howard(University of North Carolina at Chapel Hill), on behalf the SPPiRE Study Research Team
Nature Medicine
January 9, 2026
10.1038/s41591-025-04171-y
Cited by 9Open Access
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Abstract

Myasthenia gravis (MG) is driven by the secretion of autoantibodies from pathogenic B cell maturation antigen (BCMA)-expressing plasma cells. In this phase 2b randomized, controlled, double-blind trial, we evaluated Descartes-08, an autologous BCMA-directed mRNA chimeric antigen receptor T cell therapy, in patients with generalized MG (gMG). Patients (n = 26) were randomly allocated to receive once-weekly intravenous infusions of Descartes-08 (n = 15) or placebo (n = 11) over 6 weeks. The primary endpoint was a ≥5-point improvement in the MG Composite (MGC) score at month 3. Secondary endpoints included the mean change from baseline in MGC, MG Activities of Daily Living (MG-ADL) and Quantitative MG (QMG) scores by month 12. At month 3, the proportion of patients achieving a ≥5-point improvement in the MGC score was significantly higher for those treated with Descartes-08 compared to placebo in the overall population (66.7% (n = 10/15) versus 27.3% (n = 3/11), P = 0.0472) and in a subpopulation of those positive for autoantibodies to the acetylcholine receptor (63.6% (n = 7/11) versus 12.5% (n = 1/8), P = 0.0258). For patients treated with Descartes-08, the changes from baseline in mean MGC, MG-ADL and QMG scores at month 4 were -7.1, -5.5 and -4.8, respectively, with 83.0% of patients achieving a sustained and clinically meaningful response at month 12. Notably, 33.0% of patients achieved minimum symptom expression (MSE) (MG-ADL score ≤1) by month 6, which was sustained through month 12. Among biologic-naive patients, 55.60% achieved MSE by month 6, which was maintained through month 12 without additional treatment. Descartes-08 was generally safe and well tolerated. Infusion-related reactions were the most common adverse events reported (Descartes-08, 80.0% (n = 16/20); placebo, 56.3% (n = 9/16)). In summary, a single course of six once-weekly infusions of Descartes-08 was well tolerated and resulted in sustained clinically meaningful responses among patients with gMG. ClinicalTrials.gov identifier: NCT04146051 .

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