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Hzf Determines cell survival upon genotoxic stress by modulating p53 transactivation.


ABSTRACT: A critical unresolved issue about the genotoxic stress response is how the resulting activation of the p53 tumor suppressor can lead either to cell-cycle arrest and DNA repair or to apoptosis. We show here that hematopoietic zinc finger (Hzf), a zinc-finger-containing p53 target gene, modulates p53 transactivation functions in an autoregulatory feedback loop. Hzf is induced by p53 and binds to its DNA-binding domain, resulting in preferential transactivation of proarrest p53 target genes over its proapoptotic target genes. Thus, p53 activation results in cell-cycle arrest in Hzf wild-type MEFs, while in Hzf(-/-) MEFs, apoptosis is induced. Exposure of Hzf null mice to ionizing radiation resulted in enhanced apoptosis in several organs, as compared to in wild-type mice. These findings provide novel insights into the regulation of p53 transactivation function and suggest that Hzf functions as a key player in regulating cell fate decisions in response to genotoxic stress.

SUBMITTER: Das S 

PROVIDER: S-EPMC2779720 | biostudies-literature | 2007 Aug

REPOSITORIES: biostudies-literature

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Hzf Determines cell survival upon genotoxic stress by modulating p53 transactivation.

Das Sanjeev S   Raj Lakshmi L   Zhao Bo B   Kimura Yuki Y   Bernstein Alan A   Aaronson Stuart A SA   Lee Sam W SW  

Cell 20070801 4


A critical unresolved issue about the genotoxic stress response is how the resulting activation of the p53 tumor suppressor can lead either to cell-cycle arrest and DNA repair or to apoptosis. We show here that hematopoietic zinc finger (Hzf), a zinc-finger-containing p53 target gene, modulates p53 transactivation functions in an autoregulatory feedback loop. Hzf is induced by p53 and binds to its DNA-binding domain, resulting in preferential transactivation of proarrest p53 target genes over it  ...[more]

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