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Sca-1-expressing nonmyogenic cells contribute to fibrosis in aged skeletal muscle.


ABSTRACT: We report an age-dependent increase in nonimmunohematopoietic cells (CD45neg) in regenerating muscle characterized by high stem-cell antigen (Sca-1) expression. In aged regenerating muscle, only 14% of these CD45negSca-1pos cells express MyoD, whereas 82% of CD45negSca-1(pos) cells are MyoDpos in young adult muscle. In vitro, CD45negMyoDnegSca-1pos cells overexpress fibrosis-promoting genes, potentially controlled by Wnt2. The cells are proliferative, nonmyogenic, and nonadipogenic, and arise in clonally derived myoblast cultures from aged mice. MyoDneg Sca-1pos nonmyogenic cells also emerge in C2C12 myoblast cultures at late passage. Both in vitro and in vivo studies suggest that MyoDnegSca-1pos cells from aged muscle are more susceptible to apoptosis than myoblasts, which may contribute to depletion of the satellite cell pool. Thus, with age, a subset of myoblasts takes on an altered phenotype, which is marked by high Sca-1 expression. These cells do not participate in muscle regeneration, and instead may contribute to muscle fibrosis in aged muscle.

SUBMITTER: Hidestrand M 

PROVIDER: S-EPMC2755567 | biostudies-literature | 2008 Jun

REPOSITORIES: biostudies-literature

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Sca-1-expressing nonmyogenic cells contribute to fibrosis in aged skeletal muscle.

Hidestrand Mats M   Richards-Malcolm Sonia S   Gurley Catherine M CM   Nolen Greg G   Grimes Barry B   Waterstrat Amanda A   Zant Gary Van GV   Peterson Charlotte A CA  

The journals of gerontology. Series A, Biological sciences and medical sciences 20080601 6


We report an age-dependent increase in nonimmunohematopoietic cells (CD45neg) in regenerating muscle characterized by high stem-cell antigen (Sca-1) expression. In aged regenerating muscle, only 14% of these CD45negSca-1pos cells express MyoD, whereas 82% of CD45negSca-1(pos) cells are MyoDpos in young adult muscle. In vitro, CD45negMyoDnegSca-1pos cells overexpress fibrosis-promoting genes, potentially controlled by Wnt2. The cells are proliferative, nonmyogenic, and nonadipogenic, and arise in  ...[more]

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