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Genetic interrogation of replicative senescence uncovers a dual role for USP28 in coordinating the p53 and GATA4 branches of the senescence program
Cited 25 time in
Web of Science
Cited 24 time in Scopus
- Authors
- Issue Date
- 2017-10
- Publisher
- Cold Spring Harbor Laboratory Press
- Citation
- Genes and Development, Vol.31 No.19, pp.1933-1938
- Abstract
- Senescence is a terminal differentiation program that halts the growth of damaged cells and must be circumvented for cancer to arise. Here we describe a panel of genetic screens to identify genes required for replicative senescence. We uncover a role in senescence for the potent tumor suppressor and ATM substrate USP28. USP28 controls activation of both the TP53 branch and the GATA4/NFkB branch that controls the senescence-associated secretory phenotype (SASP). These results suggest a role for ubiquitination in senescence and imply a common node downstream from ATM that links the TP53 and GATA4 branches of the senescence response.
- ISSN
- 0890-9369
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