Berger Michael, Stahl Nathalie, Del Sal Giannino, Haupt Ygal
Lautenberg Center for General and Tumor Immunology, The Hebrew University Hadassah Medical School, P.O. Box 12272, Jerusalem 91120, Israel.
Mol Cell Biol. 2005 Jul;25(13):5380-8. doi: 10.1128/MCB.25.13.5380-5388.2005.
Tumor suppression by the p53 protein largely depends on the elimination of damaged cells by apoptosis. Mutations in the polyproline region (PPR) of p53 impair its apoptotic function. Deletion of the PPR renders p53 more sensitive to inhibition by Mdm2 via an unknown mechanism. We have explored the mechanism by which the PPR modulates the p53/Mdm2 loop. Proline 82 of p53 was identified to be essential for its interaction with the checkpoint kinase 2 (Chk2) and consequent phosphorylation of p53 on serine 20, following DNA damage. These physical and functional interactions are regulated by Pin1 through cis-trans isomerization of proline 82. Our study unravels the pathway by which Pin1 activates p53 in response to DNA damage and explains how Pin1 protects p53 from Mdm2. Further, we propose a role for Pin1-dependent induction of p53 conformational change as a mechanism responsible for the enhanced interaction between p53 and Chk2 following DNA damage. Importantly, our findings elucidate the selection for mutations in the Pin1 target Thr81/Pro82 motif within the PPR of p53 in human cancer.
p53蛋白的肿瘤抑制作用很大程度上取决于通过凋亡消除受损细胞。p53多聚脯氨酸区域(PPR)的突变会损害其凋亡功能。PPR的缺失使p53通过未知机制对Mdm2的抑制作用更敏感。我们探究了PPR调节p53/Mdm2环路的机制。p53的脯氨酸82被确定对于其与检查点激酶2(Chk2)的相互作用以及DNA损伤后p53丝氨酸20位点的磷酸化至关重要。这些物理和功能相互作用由Pin1通过脯氨酸82的顺反异构化进行调节。我们的研究揭示了Pin1响应DNA损伤激活p53的途径,并解释了Pin1如何保护p53免受Mdm2的影响。此外,我们提出Pin1依赖的p53构象变化诱导作用,作为DNA损伤后p53与Chk2之间增强相互作用的一种机制。重要的是,我们的发现阐明了人类癌症中p53的PPR内Pin1靶标苏氨酸81/脯氨酸82基序突变的选择。
