p53 regulation by post-translational modification and nuclear retention in response to diverse stresses

被引:0
|
作者
Gretchen S Jimenez
Shireen H Khan
Jayne M Stommel
Geoffrey M Wahl
机构
[1] Gene Expression Laboratory,Department of Biology
[2] The Salk Institute,undefined
[3] University of California at San Diego,undefined
来源
Oncogene | 1999年 / 18卷
关键词
p53; DNA damage; nuclear export signal; microtubule depolymerization; post translational modification;
D O I
暂无
中图分类号
学科分类号
摘要
p53 activation by diverse stresses involves post-translational modifications that alter its structure and result in its nuclear accumulation. We will discuss several unresolved topics regarding p53 regulation which are currently under investigation. DNA damage is perhaps the best-studied stress which activates p53, and recent data implicate phosphorylation at N-terminal serine residues as critical in this process. We discuss recent data regarding the potential kinases which modify p53 and the possible role of the resulting phosphorylation events. By contrast, much less is understood about agents which disrupt the mitotic spindle. The cell cycle phase, induction signal, and biochemical mechanism of the reversible arrest induced by microtubule disruption are currently under investigation. Finally, a key event in response to any genotoxic stress is the accumulation of p53 in the nucleus. The factors which determine the steady state level of p53 are starting to be elucidated, but the mechanisms responsible for nuclear accumulation and nuclear export remain controversial. We discuss new studies revealing a mechanism for nuclear retention of p53, and the potential contributions of MDM2 to this process.
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页码:7656 / 7665
页数:9
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