| Literature DB >> 28854354 |
Meimei Zhao1, Rui Geng1, Xiang Guo1, Ruoshi Yuan1, Xiao Zhou1, Yanyan Zhong1, Yanfei Huo1, Mei Zhou1, Qinjian Shen1, Yinglu Li2, Weiguo Zhu2, Jiadong Wang3.
Abstract
The RPA complex can integrate multiple stress signals into diverse responses by activating distinct DNA repair pathways. However, it remains unclear how RPA1 elects to activate a specific repair pathway during different types of DNA damage. Here, we report that PCAF/GCN5-mediated K163 acetylation of RPA1 is crucial for nucleotide excision repair (NER) but is dispensable for other DNA repair pathways. Mechanistically, we demonstrate that the acetylation of RPA1 is critical for the steady accumulation of XPA at damaged DNA sites and preferentially activates the NER pathway. DNA-PK phosphorylates and activates PCAF upon UV damage and consequently promotes the acetylation of RPA1. Moreover, the acetylation of RPA1 is tightly regulated by HDAC6 and SIRT1. Together, our results demonstrate that the K163 acetylation of RPA1 plays a key role in the repair of UV-induced DNA damage and reveal how the specific RPA1 modification modulates the choice of distinct DNA repair pathways.Entities:
Keywords: PCAF; RPA1; UV damage; XPA; acetylation and deacetylation
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Year: 2017 PMID: 28854354 DOI: 10.1016/j.celrep.2017.08.015
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423