4.6 Article

Nogo-A regulates myogenesis via interacting with Filamin-C

Journal

CELL DEATH DISCOVERY
Volume 7, Issue 1, Pages -

Publisher

SPRINGERNATURE
DOI: 10.1038/s41420-020-00384-x

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Funding

  1. National Research Foundation of Korea [NRF-2017R1E1A1A01072781]
  2. Korea Institute of Planning and Evaluation for Technology in Food, Agriculture, Forestry and Fisheries (IPET) through the Agri-Bioindustry Technology Development Program - Ministry of Agriculture, Food and Rural Affairs (MAFRA), Republic of Korea [312062-5]

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Among the three isoforms encoded by Rtn4, Nogo-A has been extensively studied as a CNS inhibitor. Increased Nogo-A expression in various muscle-related pathological conditions suggests a role in muscle regeneration. Nogo(-/-) mice exhibit dystrophic muscle structure, impaired regeneration, and altered gene expression, indicating the importance of Nogo-A in muscle homeostasis and regeneration.
Among the three isoforms encoded by Rtn4, Nogo-A has been intensely investigated as a central nervous system inhibitor. Although Nogo-A expression is increased in muscles of patients with amyotrophic lateral sclerosis, its role in muscle homeostasis and regeneration is not well elucidated. In this study, we discovered a significant increase in Nogo-A expression in various muscle-related pathological conditions. Nogo(-/-) mice displayed dystrophic muscle structure, dysregulated muscle regeneration following injury, and altered gene expression involving lipid storage and muscle cell differentiation. We hypothesized that increased Nogo-A levels might regulate muscle regeneration. Differentiating myoblasts exhibited Nogo-A upregulation and silencing Nogo-A abrogated myoblast differentiation. Nogo-A interacted with filamin-C, suggesting a role for Nogo-A in cytoskeletal arrangement during myogenesis. In conclusion, Nogo-A maintains muscle homeostasis and integrity, and pathologically altered Nogo-A expression mediates muscle regeneration, suggesting Nogo-A as a novel target for the treatment of myopathies in clinical settings.

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