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Publication : Puma is required for p53-induced depletion of adult stem cells.

First Author  Liu D Year  2010
Journal  Nat Cell Biol Volume  12
Issue  10 Pages  993-8
PubMed ID  20818388 Mgi Jnum  J:170216
Mgi Id  MGI:4944151 Doi  10.1038/ncb2100
Citation  Liu D, et al. (2010) Puma is required for p53-induced depletion of adult stem cells. Nat Cell Biol 12(10):993-8
abstractText  Mammalian ageing is accompanied by accumulation of genomic DNA damage and progressive decline in the ability of tissues to regenerate. DNA damage activates the tumour suppressor p53, which leads to cell-cycle arrest, senescence or apoptosis. The stability and activity of p53 are induced by DNA damage through posttranslational modifications such as phosphorylation of Thr 21 and Ser 23 (refs 2, 3, 4, 5). To investigate the roles of DNA damage and p53 in tissue-regenerative capability, two phosphorylation-site mutations (T21D and S23D) were introduced into the endogenous p53 gene in mice, so that the synthesized protein mimics phosphorylated p53. The knock-in mice exhibit constitutive p53 activation and segmental progeria that is correlated with the depletion of adult stem cells in multiple tissues, including bone marrow, brain and testes. Furthermore, a deficiency of Puma, which is required for p53-dependent apoptosis after DNA damage, rescues segmental progeria and prevents the depletion of adult stem cells. These findings suggest a key role of p53-dependent apoptosis in depleting adult stem cells after the accumulation of DNA damage, which leads to a decrease in tissue regeneration.
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