ECM is required for skeletal muscle differentiation independently of muscle regulatory factor expression

Osses N.; Brandan, E.

Abstract

Transcription of specific skeletal muscle genes requires the expression of the muscle regulatory factor myogenin. To assess the role of the extracellular matrix (ECM) in skeletal muscle differentiation, the specific inhibitors of proteoglycan synthesis, sodium chlorate and ?-D-xyloside, were used. Treatment of cultured skeletal muscle cells with each inhibitor substantially abolished the expression of creatine kinase and ?-dystroglycan. This inhibition was totally reversed by the addition of exogenous ECM. Myoblast treatment with each inhibitor affected the deposition and assembly of the ECM constituents glypican, fibronectin, and laminin. These treatments did not affect MyoD, MEF2A, and myogenin expression and nuclear localization. Differentiated myoblast treatment with RGDS peptides completely inhibited myogenesis without affecting the expression or nuclear localization of myogenin. Integrin-mediated signaling of focal adhesion kinase was partially inhibited by chlorate and ?-D-xyloside, an effect reversed by the addition of exogenous ECM gel. These results suggested that the expression of myogenin is not sufficient to successfully drive skeletal muscle formation and that ECM is required to complete the skeletal muscle differentiation process.

Más información

Título según WOS: ECM is required for skeletal muscle differentiation independently of muscle regulatory factor expression
Título según SCOPUS: ECM is required for skeletal muscle differentiation independently of muscle regulatory factor expression
Título de la Revista: AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY
Volumen: 282
Número: 2
Editorial: AMER PHYSIOLOGICAL SOC
Fecha de publicación: 2002
Página de inicio: C383
Página final: C394
Idioma: English
Notas: ISI, SCOPUS