TY - JOUR
T1 - Modulating fast skeletal muscle contraction protects skeletal muscle in animal models of Duchenne muscular dystrophy
AU - Russell, Alan J.
AU - DuVall, Mike
AU - Barthel, Ben
AU - Qian, Ying
AU - Peter, Angela K.
AU - Newell-Stamper, Breanne L.
AU - Hunt, Kevin
AU - Lehman, Sarah
AU - Madden, Molly
AU - Schlachter, Stephen
AU - Robertson, Ben
AU - Van Deusen, Ashleigh
AU - Rodriguez, Hector M.
AU - Vera, Carlos
AU - Su, Yu
AU - Claflin, Dennis R.
AU - Brooks, Susan V.
AU - Nghiem, Peter
AU - Rutledge, Alexis
AU - Juehne, Twlya I.
AU - Yu, Jinsheng
AU - Barton, Elisabeth R.
AU - Luo, Yangyi E.
AU - Patsalos, Andreas
AU - Nagy, Laszlo
AU - Sweeney, H. Lee
AU - Leinwand, Leslie A.
AU - Koch, Kevin
N1 - Publisher Copyright:
© 2023, Russell et al.
PY - 2023/5/15
Y1 - 2023/5/15
N2 - Duchenne muscular dystrophy (DMD) is a lethal muscle disease caused by absence of the protein dystrophin, which acts as a structural link between the basal lamina and contractile machinery to stabilize muscle membranes in response to mechanical stress. In DMD, mechanical stress leads to exaggerated membrane injury and fiber breakdown, with fast fibers being the most susceptible to damage. A major contributor to this injury is muscle contraction, controlled by the motor protein myosin. However, how muscle contraction and fast muscle fiber damage contribute to the pathophysiology of DMD has not been well characterized. We explored the role of fast skeletal muscle contraction in DMD with a potentially novel, selective, orally active inhibitor of fast skeletal muscle myosin, EDG-5506. Surprisingly, even modest decreases of contraction (<15%) were sufficient to protect skeletal muscles in dystrophic mdx mice from stress injury. Longer-term treatment also decreased muscle fibrosis in key disease-implicated tissues. Importantly, therapeutic levels of myosin inhibition with EDG-5506 did not detrimentally affect strength or coordination. Finally, in dystrophic dogs, EDG-5506 reversibly reduced circulating muscle injury biomarkers and increased habitual activity. This unexpected biology may represent an important alternative treatment strategy for Duchenne and related myopathies.
AB - Duchenne muscular dystrophy (DMD) is a lethal muscle disease caused by absence of the protein dystrophin, which acts as a structural link between the basal lamina and contractile machinery to stabilize muscle membranes in response to mechanical stress. In DMD, mechanical stress leads to exaggerated membrane injury and fiber breakdown, with fast fibers being the most susceptible to damage. A major contributor to this injury is muscle contraction, controlled by the motor protein myosin. However, how muscle contraction and fast muscle fiber damage contribute to the pathophysiology of DMD has not been well characterized. We explored the role of fast skeletal muscle contraction in DMD with a potentially novel, selective, orally active inhibitor of fast skeletal muscle myosin, EDG-5506. Surprisingly, even modest decreases of contraction (<15%) were sufficient to protect skeletal muscles in dystrophic mdx mice from stress injury. Longer-term treatment also decreased muscle fibrosis in key disease-implicated tissues. Importantly, therapeutic levels of myosin inhibition with EDG-5506 did not detrimentally affect strength or coordination. Finally, in dystrophic dogs, EDG-5506 reversibly reduced circulating muscle injury biomarkers and increased habitual activity. This unexpected biology may represent an important alternative treatment strategy for Duchenne and related myopathies.
UR - http://www.scopus.com/inward/record.url?scp=85159732735&partnerID=8YFLogxK
U2 - 10.1172/JCI153837
DO - 10.1172/JCI153837
M3 - Article
C2 - 36995778
AN - SCOPUS:85159732735
SN - 0021-9738
VL - 133
JO - Journal of Clinical Investigation
JF - Journal of Clinical Investigation
IS - 10
M1 - e153837
ER -