Muscle repair after physiological damage relies on nuclear migration for cellular reconstruction
Roman, William; Pinheiro, Helena; Pimentel, Mafalda R.; Segales, Jessica; Oliveira, Luis M.; Garcia-Dominguez, Esther; Gomez-Cabrera, Mari Carmen; Serrano, Antonio L.; Gomes, Edgar R.; Munoz-Canoves, Pura
SCIENCE
2021
VL / 374 - BP / 355 - EP / +
abstract
Regeneration of skeletal muscle is a highly synchronized process that requires muscle stem cells (satellite cells). We found that localized injuries, as experienced through exercise, activate a myofiber self-repair mechanism that is independent of satellite cells in mice and humans. Mouse muscle injury triggers a signaling cascade involving calcium, Cdc42, and phosphokinase C that attracts myonuclei to the damaged site via microtubules and dynein. These nuclear movements accelerate sarcomere repair and locally deliver messenger RNA (mRNA) for cellular reconstruction. Myofiber self-repair is a cell-autonomous protective mechanism and represents an alternative model for understanding the restoration of muscle architecture in health and disease.
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