作者
Na Wei, Yi Shi, Lan N Truong, Kathleen M Fisch, Tao Xu, Elisabeth Gardiner, Guangsen Fu, Yun-Shiuan Olivia Hsu, Shuji Kishi, Andrew I Su, Xiaohua Wu, Xiang-Lei Yang
发表日期
2014/10/23
期刊
Molecular cell
卷号
56
期号
2
页码范围
323-332
出版商
Elsevier
简介
Tyrosyl-tRNA synthetase (TyrRS) is known for its essential aminoacylation function in protein synthesis. Here we report a function for TyrRS in DNA damage protection. We found that oxidative stress, which often downregulates protein synthesis, induces TyrRS to rapidly translocate from the cytosol to the nucleus. We also found that angiogenin mediates or potentiates this stress-induced translocalization. The nuclear-localized TyrRS activates transcription factor E2F1 to upregulate the expression of DNA damage repair genes such as BRCA1 and RAD51. The activation is achieved through direct interaction of TyrRS with TRIM28 to sequester this vertebrate-specific epigenetic repressor and its associated HDAC1 from deacetylating and suppressing E2F1. Remarkably, overexpression of TyrRS strongly protects against UV-induced DNA double-strand breaks in zebrafish, whereas restricting TyrRS nuclear entry …
引用总数
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