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AIMP2/p38是多tRNA合成酶复合体的支架蛋白,它通过p53对基因毒性应激作出反应。

AIMP2/p38, the scaffold for the multi-tRNA synthetase complex, responds to genotoxic stresses via p53.

作者信息

Han Jung Min, Park Bum-Joon, Park Sang Gyu, Oh Young Sun, Choi So Jung, Lee Sang Won, Hwang Soon-Kyung, Chang Seung-Hee, Cho Myung-Haing, Kim Sunghoon

机构信息

Center for Medicinal Protein Network and Systems Biology, College of Pharmacy, and College of Veterinary Medicine, Seoul National University, Seoul 151-742, Korea.

出版信息

Proc Natl Acad Sci U S A. 2008 Aug 12;105(32):11206-11. doi: 10.1073/pnas.0800297105. Epub 2008 Aug 11.

DOI:10.1073/pnas.0800297105
PMID:18695251
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2516205/
Abstract

AIMP2/p38 is a scaffolding protein required for the assembly of the macromolecular tRNA synthetase complex. Here, we describe a previously unknown function for AIMP2 as a positive regulator of p53 in response to genotoxic stresses. Depletion of AIMP2 increased resistance to DNA damage-induced apoptosis, and introduction of AIMP2 into AIMP2-deficient cells restored the susceptibility to apoptosis. Upon DNA damage, AIMP2 was phosphorylated, dissociated from the multi-tRNA synthetase complex, and translocated into the nuclei of cells. AIMP2 directly interacts with p53, thereby preventing MDM2-mediated ubiquitination and degradation of p53. Mutations in AIMP2, affecting its interaction with p53, hampered its ability to activate p53. Nutlin-3 recovered the level of p53 and the susceptibility to UV-induced cell death in AIMP2-deficient cells. This work demonstrates that AIMP2, a component of the translational machinery, functions as proapoptotic factor via p53 in response to DNA damage.

摘要

AIMP2/p38是组装大分子tRNA合成酶复合体所需的一种支架蛋白。在此,我们描述了AIMP2作为p53在应对基因毒性应激时的正向调节因子这一此前未知的功能。AIMP2的缺失增加了对DNA损伤诱导的细胞凋亡的抗性,而将AIMP2导入AIMP2缺陷细胞可恢复其对细胞凋亡的易感性。在DNA损伤时,AIMP2被磷酸化,从多tRNA合成酶复合体解离,并转位进入细胞核。AIMP2直接与p53相互作用,从而防止MDM2介导的p53泛素化和降解。AIMP2中影响其与p53相互作用的突变阻碍了其激活p53的能力。Nutlin-3恢复了AIMP2缺陷细胞中p53的水平以及对紫外线诱导的细胞死亡的易感性。这项工作表明,作为翻译机制组成部分的AIMP2,在应对DNA损伤时通过p53发挥促凋亡因子的作用。

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