JCI Insight (Nov 2023)

Dimethyl fumarate modulates the dystrophic disease program following short-term treatment

  • Cara A. Timpani,
  • Stephanie Kourakis,
  • Danielle A. Debruin,
  • Dean G. Campelj,
  • Nancy Pompeani,
  • Narges Dargahi,
  • Angelo P. Bautista,
  • Ryan M. Bagaric,
  • Elya J. Ritenis,
  • Lauren Sahakian,
  • Didier Debrincat,
  • Nicole Stupka,
  • Patricia Hafner,
  • Peter G. Arthur,
  • Jessica R. Terrill,
  • Vasso Apostolopoulos,
  • Judy B. de Haan,
  • Nuri Guven,
  • Dirk Fischer,
  • Emma Rybalka

Journal volume & issue
Vol. 8, no. 21

Abstract

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New medicines are urgently required to treat the fatal neuromuscular disease Duchenne muscular dystrophy (DMD). Dimethyl fumarate (DMF) is a potent immunomodulatory small molecule nuclear erythroid 2-related factor 2 activator with current clinical utility in the treatment of multiple sclerosis and psoriasis that could be effective for DMD and rapidly translatable. Here, we tested 2 weeks of daily 100 mg/kg DMF versus 5 mg/kg standard-care prednisone (PRED) treatment in juvenile mdx mice with early symptomatic DMD. Both drugs modulated seed genes driving the DMD disease program and improved force production in fast-twitch muscle. However, only DMF showed pro-mitochondrial effects, protected contracting muscles from fatigue, improved histopathology, and augmented clinically compatible muscle function tests. DMF may be a more selective modulator of the DMD disease program than PRED, warranting follow-up longitudinal studies to evaluate disease-modifying impact.

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