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Publication : Prepubertal skeletal muscle growth requires Pax7-expressing satellite cell-derived myonuclear contribution.

First Author  Bachman JF Year  2018
Journal  Development Volume  145
Issue  20 PubMed ID  30305290
Mgi Jnum  J:266540 Mgi Id  MGI:6220742
Doi  10.1242/dev.167197 Citation  Bachman JF, et al. (2018) Prepubertal skeletal muscle growth requires Pax7-expressing satellite cell-derived myonuclear contribution. Development 145(20):dev167197
abstractText  The functional role of Pax7-expressing satellite cells (SCs) in postnatal skeletal muscle development beyond weaning remains obscure. Therefore, the relevance of SCs during prepubertal growth, a period after weaning but prior to the onset of puberty, has not been examined. Here, we have characterized mouse skeletal muscle growth during prepuberty and found significant increases in myofiber cross-sectional area that correlated with SC-derived myonuclear number. Remarkably, genome-wide RNA-sequencing analysis established that post-weaning juvenile and early adolescent skeletal muscle have markedly different gene expression signatures. These distinctions are consistent with extensive skeletal muscle maturation during this essential, albeit brief, developmental phase. Indelible labeling of SCs with Pax7(CreERT2/+) ; Rosa26(nTnG/+) mice demonstrated SC-derived myonuclear contribution during prepuberty, with a substantial reduction at puberty onset. Prepubertal depletion of SCs in Pax7(CreERT2/+) ; Rosa26(DTA/+) mice reduced myofiber size and myonuclear number, and caused force generation deficits to a similar extent in both fast and slow-contracting muscles. Collectively, these data demonstrate SC-derived myonuclear accretion as a cellular mechanism that contributes to prepubertal hypertrophic skeletal muscle growth.
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