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JCS ePress online publication date 8 Apr 2008
doi: 10.1242/jcs.024885


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Research Article

{beta}-catenin promotes self-renewal of skeletal-muscle satellite cells


Ana Perez-Ruiz, Yusuke Ono, Viola F. Gnocchi, and Peter S. Zammit*
* Author for correspondence (e-mail: peter.zammit{at}kcl.ac.uk)

Satellite cells are the resident stem cells of adult skeletal muscle. As with all stem cells, how the choice between self-renewal or differentiation is controlled is central to understanding their function. Here, we have explored the role of {beta}-catenin in determining the fate of myogenic satellite cells. Satellite cells express {beta}-catenin, and expression is maintained as they activate and undergo proliferation. Constitutive retroviral-driven expression of wild-type or stabilised {beta}-catenin results in more satellite cells expressing Pax7 without any MyoD - therefore, adopting the self-renewal pathway, with fewer cells undergoing myogenic differentiation. Similarly, preventing the degradation of endogenous {beta}-catenin by inhibiting GSK3{beta} activity also results in more Pax7-positive-MyoD-negative (Pax7+MyoD-) satellite-cell progeny. Consistent with these observations, downregulation of {beta}-catenin using small interfering RNA (siRNA) reduced the proportion of satellite cells that express Pax7 and augmented myogenic differentiation after mitogen withdrawal. Since a dominant-negative version of {beta}-catenin had the same effect as silencing {beta}-catenin using specific siRNA, {beta}-catenin promotes self-renewal via transcriptional control of target genes. Thus, {beta}-catenin signalling in proliferating satellite cells directs these cells towards the self-renewal pathway and, so, contributes to the maintenance of this stem-cell pool in adult skeletal muscle.


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