Reversal of Terminal Differentiation Mediated by p107 in Rb <sup>-/-</sup> Muscle Cells
Jay W. Schneider(Boston Children's Hospital), Wei Gu(Boston Children's Hospital), Liang Zhu(Harvard University Press), Vijak Mahdavi(Boston Children's Hospital), Bernardo Nadal‐Ginard(Boston Children's Hospital)
Cited by 368
Abstract
The terminal differentiation of mammalian muscle cells requires the tumor suppressor retinoblastoma protein (Rb). Unlike their wild-type counterparts, multinucleated myotubes from mouse cells deficient in Rb (Rb-/-) were induced by serum to re-enter the cell cycle. Development of the myogenic phenotype in Rb-/- cells correlated with increased expression of p107, which interacted with myogenic transcription factors. Serum-induced cell cycle reentry, on the other hand, correlated with decreased p107 expression. Thus, although p107 could substitute for Rb as a cofactor for differentiation, it could not maintain the terminally differentiated state in Rb-/- myotubes.
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