Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
2177222 | Developmental Cell | 2010 | 12 Pages |
SummaryMuscle progenitors, labeled by the transcription factor Pax7, are responsible for muscle growth during development. The signals that regulate the muscle progenitor number during myogenesis are unknown. We show, through in vivo analysis, that Bmp signaling is involved in regulating fetal skeletal muscle growth. Ectopic activation of Bmp signaling in chick limbs increases the number of fetal muscle progenitors and fibers, while blocking Bmp signaling reduces their numbers, ultimately leading to small muscles. The Bmp effect that we observed during fetal myogenesis is diametrically opposed to that previously observed during embryonic myogenesis and that deduced from in vitro work. We also show that Bmp signaling regulates the number of satellite cells during development. Finally, we demonstrate that Bmp signaling is active in a subpopulation of fetal progenitors and satellite cells at the extremities of muscles. Overall, our results show that Bmp signaling plays differential roles in embryonic and fetal myogenesis.
► In fetal development, Bmp signaling is active in progenitors at muscle tips ► Bmp signaling regulates the number of fetal muscle progenitors and fibers ► Developmental satellite cell numbers are also regulated by Bmp signals ► Bmp signaling is detected in activated satellite cells during regeneration