AAV gene therapy for Duchenne muscular dystrophy: the EMBARK phase 3 randomized trial

Jerry R Mendell; Francesco Muntoni; Craig M McDonald; Eugenio M Mercuri; Emma Ciafaloni; Hirofumi Komaki; Carmen Leon-Astudillo; Andrés Nascimento; Crystal Proud; Ulrike Schara-Schmidt; Aravindhan Veerapandiyan; Craig M Zaidman; Maitea Guridi; Alexander P Murphy; Carol Reid; Christoph Wandel; Damon R Asher; Eddie Darton; Stefanie Mason; Rachael A Potter; Teji Singh; Wenfei Zhang; Paulo Fontoura; Jacob S Elkins; Louise R Rodino-Klapac

doi:10.1038/s41591-024-03304-z

AAV gene therapy for Duchenne muscular dystrophy: the EMBARK phase 3 randomized trial

Nat Med. 2024 Oct 9. doi: 10.1038/s41591-024-03304-z. Online ahead of print.

Authors

Jerry R Mendell^#^{1

2

3}, Francesco Muntoni^#⁴, Craig M McDonald⁵, Eugenio M Mercuri⁶, Emma Ciafaloni⁷, Hirofumi Komaki⁸, Carmen Leon-Astudillo⁹, Andrés Nascimento¹⁰, Crystal Proud¹¹, Ulrike Schara-Schmidt¹², Aravindhan Veerapandiyan¹³, Craig M Zaidman¹⁴, Maitea Guridi¹⁵, Alexander P Murphy¹⁶, Carol Reid¹⁶, Christoph Wandel¹⁵, Damon R Asher¹⁷, Eddie Darton¹⁷, Stefanie Mason¹⁷, Rachael A Potter¹⁷, Teji Singh¹⁷, Wenfei Zhang¹⁷, Paulo Fontoura¹⁵, Jacob S Elkins¹⁷, Louise R Rodino-Klapac¹⁷

Affiliations

¹ Center for Gene Therapy, Nationwide Children's Hospital, Columbus, OH, USA. JMendell@Sarepta.com.
² The Ohio State University, Columbus, OH, USA. JMendell@Sarepta.com.
³ Sarepta Therapeutics, Inc., Cambridge, MA, USA. JMendell@Sarepta.com.
⁴ Dubowitz Neuromuscular Centre, NIHR Great Ormond Street Hospital Biomedical Research Centre, Great Ormond Street Institute of Child Health and Institute of Neurology, University College London and Great Ormond Street Hospital Trust, London, UK.
⁵ UC Davis Health, Sacramento, CA, USA.
⁶ Pediatric Neurology Institute, Catholic University and Nemo Pediatrico, Fondazione Policlinico Gemelli IRCCS, Rome, Italy.
⁷ University of Rochester Medical Center, Rochester, NY, USA.
⁸ Translational Medical Center, National Center of Neurology and Psychiatry, Tokyo, Japan.
⁹ Department of Pediatrics, University of Florida, Gainesville, FL, USA.
¹⁰ Neuromuscular Unit, Neuropaediatrics Department, Hospital Sant Joan de Déu, Fundacion Sant Joan de Déu, CIBERER - ISC III, Barcelona, Spain.
¹¹ Children's Hospital of the King's Daughters, Norfolk, VA, USA.
¹² Department of Pediatric Neurology, Center for Neuromuscular Disorders in Children and Adolescents, University Clinic Essen, University of Duisburg-Essen, Essen, Germany.
¹³ Department of Pediatrics, Division of Neurology, University of Arkansas for Medical Sciences, Arkansas Children's Hospital, Little Rock, AR, USA.
¹⁴ Department of Neurology, Washington University in St. Louis, St. Louis, MO, USA.
¹⁵ F. Hoffmann-La Roche, Ltd., Basel, Switzerland.
¹⁶ Roche Products, Ltd., Welwyn Garden City, UK.
¹⁷ Sarepta Therapeutics, Inc., Cambridge, MA, USA.

^# Contributed equally.

PMID: 39385046
DOI: 10.1038/s41591-024-03304-z

Abstract

Duchenne muscular dystrophy (DMD) is a rare, X-linked neuromuscular disease caused by pathogenic variants in the DMD gene that result in the absence of functional dystrophin, beginning at birth and leading to progressive impaired motor function, loss of ambulation and life-threatening cardiorespiratory complications. Delandistrogene moxeparvovec, an adeno-associated rh74-viral vector-based gene therapy, addresses absent functional dystrophin in DMD. Here the phase 3 EMBARK study aimed to assess the efficacy and safety of delandistrogene moxeparvovec in patients with DMD. Ambulatory males with DMD, ≥4 years to <8 years of age, were randomized and stratified by age group and North Star Ambulatory Assessment (NSAA) score to single-administration intravenous delandistrogene moxeparvovec (1.33 × 10¹⁴ vector genomes per kilogram; n = 63) or placebo (n = 62). At week 52, the primary endpoint, change from baseline in NSAA score, was not met (least squares mean 2.57 (delandistrogene moxeparvovec) versus 1.92 (placebo) points; between-group difference, 0.65; 95% confidence interval (CI), -0.45, 1.74; P = 0.2441). Secondary efficacy endpoints included mean micro-dystrophin expression at week 12: 34.29% (treated) versus 0.00% (placebo). Other secondary efficacy endpoints at week 52 (between-group differences (95% CI)) included: Time to Rise (-0.64 (-1.06, -0.23)), 10-meter Walk/Run (-0.42 (-0.71, -0.13)), stride velocity 95th centile (0.10 (0.00, 0.19)), 100-meter Walk/Run (-3.29 (-8.28, 1.70)), time to ascend 4 steps (-0.36 (-0.71, -0.01)), PROMIS Mobility and Upper Extremity (0.05 (-0.08, 0.19); -0.04 (-0.24, 0.17)) and number of NSAA skills gained/improved (0.19 (-0.67, 1.06)). In total, 674 adverse events were recorded with delandistrogene moxeparvovec and 514 with placebo. There were no deaths, discontinuations or clinically significant complement-mediated adverse events; 7 patients (11.1%) experienced 10 treatment-related serious adverse events. Delandistrogene moxeparvovec did not lead to a significant improvement in NSAA score at week 52. Some of the secondary endpoints numerically favored treatment, although no statistical significance can be claimed. Safety was manageable and consistent with previous delandistrogene moxeparvovec trials. ClinicalTrials.gov: NCT05096221.

Associated data

ClinicalTrials.gov/NCT05096221