Myf6/MRF4 is a myogenic niche regulator required for the maintenance of the muscle stem cell pool

Myf6/MRF4 是维持肌肉干细胞库所需的成肌生态位调节剂

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作者:Felicia Lazure #, Darren M Blackburn #, Aldo H Corchado, Korin Sahinyan, Nabila Karam, Ahmad Sharanek, Duy Nguyen, Christoph Lepper, Hamed S Najafabadi, Theodore J Perkins, Arezu Jahani-Asl, Vahab D Soleimani

Abstract

The function and maintenance of muscle stem cells (MuSCs) are tightly regulated by signals originating from their niche environment. Skeletal myofibers are a principle component of the MuSC niche and are in direct contact with the muscle stem cells. Here, we show that Myf6 establishes a ligand/receptor interaction between muscle stem cells and their associated muscle fibers. Our data show that Myf6 transcriptionally regulates a broad spectrum of myokines and muscle-secreted proteins in skeletal myofibers, including EGF. EGFR signaling blocks p38 MAP kinase-induced differentiation of muscle stem cells. Homozygous deletion of Myf6 causes a significant reduction in the ability of muscle to produce EGF, leading to a deregulation in EGFR signaling. Consequently, although Myf6-knockout mice are born with a normal muscle stem cell compartment, they undergo a progressive reduction in their stem cell pool during postnatal life due to spontaneous exit from quiescence. Taken together, our data uncover a novel role for Myf6 in promoting the expression of key myokines, such as EGF, in the muscle fiber which prevents muscle stem cell exhaustion by blocking their premature differentiation.

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