| Literature DB >> 33879772 |
Yang Wang1,2,3, Jing Tian1,2,3, Chao Huang4, Jiao Ma1,2,3, Gaolei Hu1,2,3, Yalan Chen1,2,3, Tianshi Wang1,2,3, Rong Cai1,2,3, Yong Zuo1,2,3, Hongsheng Tan5, Qiuju Fan1,2,3, Baijun Dong1,3, Wei Xue1,3, Jing Yi1,2,3, Guoqiang Chen2, Jun Tu6,7,8, Jinke Cheng9,10,11.
Abstract
In response to DNA damage, p53-mediated signaling is regulated by protein phosphorylation and ubiquitination to precisely control G2 checkpoint. Here we demonstrated that protein SUMOylation also engaged in regulation of p53-mediated G2 checkpoint. We found that G2 DNA damage suppressed SENP3 phosphorylation at G2/M phases in p53-dependent manner. We further found that the suppression of SENP3 phosphorylation was crucial for efficient DNA damage/p53-induced G2 checkpoint and G2 arrest. Mechanistically, we identified Cdh1, a subunit of APC/C complex, was a SUMOylated protein at G2/M phase. SENP3 could de-SUMOylate Cdh1. DNA damage/p53-induced suppression of SENP3 phosphorylation activated SENP3 de-SUMOylation of Cdh. De-SUMOylation promoted Cdh1 de-phosphorylation by phosphatase Cdc14B, and then activated APC/CCdh1 E3 ligase activity to ubiquitate and degrade Polo-like kinase 1 (Plk1) in process of G2 checkpoint. These data reveal that p53-mediated inhibition of SENP3 phosphorylation regulates the activation of Cdc14b-APC/CCdh1-Plk1 axis to control DNA damage-induced G2 checkpoint.Entities:
Year: 2020 PMID: 33879772 DOI: 10.1038/s41421-020-0154-2
Source DB: PubMed Journal: Cell Discov ISSN: 2056-5968 Impact factor: 10.849