Fibrosis and adipogenesis originate from a common mesenchymal progenitor in skeletal muscle

Akiyoshi Uezumi(Fujita Health University), Takahito Ito(The University of Osaka), Daisuke Morikawa(The University of Osaka), Natsuko Shimizu(The University of Osaka), Tomohiro Yoneda(The University of Osaka), Masashi Segawa(The University of Osaka), Masahiko Yamaguchi(The University of Osaka), Ryo Ogawa(The University of Osaka), Miroslav M. Matev(The University of Osaka), Yuko Miyagoe‐Suzuki(National Center of Neurology and Psychiatry), Shin’ichi Takeda(National Center of Neurology and Psychiatry), Kazutake Tsujikawa(The University of Osaka), Kunihiro Tsuchida(Fujita Health University), Hiroshi Yamamoto(The University of Osaka), So‐ichiro Fukada(The University of Osaka)
Journal of Cell Science
November 1, 2011
Cited by 663

Abstract

Accumulation of adipocytes and collagen type-I-producing cells (fibrosis) is observed in muscular dystrophies. The origin of these cells had been largely unknown, but recently we identified mesenchymal progenitors positive for platelet-derived growth factor receptor alpha (PDGFRα) as the origin of adipocytes in skeletal muscle. However, the origin of muscle fibrosis remains largely unknown. In this study, clonal analyses show that PDGFRα(+) cells also differentiate into collagen type-I-producing cells. In fact, PDGFRα(+) cells accumulated in fibrotic areas of the diaphragm in the mdx mouse, a model of Duchenne muscular dystrophy. Furthermore, mRNA of fibrosis markers was expressed exclusively in the PDGFRα(+) cell fraction in the mdx diaphragm. Importantly, TGF-β isoforms, known as potent profibrotic cytokines, induced expression of markers of fibrosis in PDGFRα(+) cells but not in myogenic cells. Transplantation studies revealed that fibrogenic PDGFRα(+) cells mainly derived from pre-existing PDGFRα(+) cells and that the contribution of PDGFRα(-) cells and circulating cells was limited. These results indicate that mesenchymal progenitors are the main origin of not only fat accumulation but also fibrosis in skeletal muscle.


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