p53-Independent Expression of p21 <sup>Cip1</sup> in Muscle and Other Terminally Differentiating Cells

Susan B. Parker; Gregor Eichele; Pumin Zhang; Alan Rawls; Arthur Sands; Allan Bradley; Eric N. Olson; J. Wade Harper; Stephen J. Elledge

doi:10.1126/science.7863329

p53-Independent Expression of p21 <sup>Cip1</sup> in Muscle and Other Terminally Differentiating Cells

Susan B. Parker(Howard Hughes Medical Institute), Gregor Eichele(Baylor College of Medicine), Pumin Zhang(Baylor College of Medicine), Alan Rawls(The University of Texas MD Anderson Cancer Center), Arthur Sands(Howard Hughes Medical Institute), Allan Bradley(Howard Hughes Medical Institute), Eric N. Olson(The University of Texas MD Anderson Cancer Center), J. Wade Harper(Baylor College of Medicine), Stephen J. Elledge(Howard Hughes Medical Institute)

Science

February 17, 1995

10.1126/science.7863329

Cited by 1,035

Abstract

Terminal differentiation is coupled to withdrawal from the cell cycle. The cyclin-dependent kinase inhibitor (CKI) p21Cip1 is transcriptionally regulated by p53 and can induce growth arrest. CKIs are therefore potential mediators of developmental control of cell proliferation. The expression pattern of mouse p21 correlated with terminal differentiation of multiple cell lineages including skeletal muscle, cartilage, skin, and nasal epithelium in a p53-independent manner. Although the muscle-specific transcription factor MyoD is sufficient to activate p21 expression in 10T1/2 cells, p21 was expressed in myogenic cells of mice lacking the genes encoding MyoD and myogenin, demonstrating that p21 expression does not require these transcription factors. The p21 protein may function during development as an inducible growth inhibitor that contributes to cell cycle exit and differentiation.

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