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Differential roles of ATM- and Chk2-mediated phosphorylations of Hdmx in response to DNA damage. | LitMetric

AI Article Synopsis

  • The p53 tumor suppressor is essential for maintaining genomic stability, with its activation primarily regulated by the ATM protein kinase in response to DNA double strand breaks (DSBs).
  • ATM modifies p53 and its inhibitors, Hdm2 and Hdmx, through phosphorylation and ubiquitination, promoting Hdmx degradation after DSBs.
  • Specific phosphorylation sites on Hdmx (S403, S367, and S342) are crucial for its interaction with 14-3-3 proteins, affecting Hdmx's nuclear accumulation and subsequent degradation, illustrating ATM's complex regulation of the DNA damage response.

Article Abstract

The p53 tumor suppressor plays a major role in maintaining genomic stability. Its activation and stabilization in response to double strand breaks (DSBs) in DNA are regulated primarily by the ATM protein kinase. ATM mediates several posttranslational modifications on p53 itself, as well as phosphorylation of p53's essential inhibitors, Hdm2 and Hdmx. Recently we showed that ATM- and Hdm2-dependent ubiquitination and subsequent degradation of Hdmx following DSB induction are mediated by phosphorylation of Hdmx on S403, S367, and S342, with S403 being targeted directly by ATM. Here we show that S367 phosphorylation is mediated by the Chk2 protein kinase, a downstream kinase of ATM. This phosphorylation, which is important for subsequent Hdmx ubiquitination and degradation, creates a binding site for 14-3-3 proteins which controls nuclear accumulation of Hdmx following DSBs. Phosphorylation of S342 also contributed to optimal 14-3-3 interaction and nuclear accumulation of Hdmx, but phosphorylation of S403 did not. Our data indicate that binding of a 14-3-3 dimer and subsequent nuclear accumulation are essential steps toward degradation of p53's inhibitor, Hdmx, in response to DNA damage. These results demonstrate a sophisticated control by ATM of a target protein, Hdmx, which itself is one of several ATM targets in the ATM-p53 axis of the DNA damage response.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1592859PMC
http://dx.doi.org/10.1128/MCB.00562-06DOI Listing

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