作者
Fei Zhao,Wootae Kim,Huanyao Gao,Chao Liu,Yong Zhang,Yuping Chen,Min Deng,Qin Zhou,Jinzhou Huang,Qi Hu,Shih-Hsun Chen,Somaira Nowsheen,Jake A. Kloeber,Bo Qin,Ping Yin,Xinyi Tu,Guijie Guo,Sisi Qin,Chao Zhang,Ming Gao,Kuntian Luo,Yilun Liu,Zhenkun Lou,Jian Yuan
摘要
The shieldin complex functions as the downstream effector of 53BP1-RIF1 to promote DNA double-strand break end-joining by restricting end resection. The SHLD2 subunit binds to single-stranded DNA ends and blocks end resection through OB-fold domains. Besides blocking end resection, it is unclear how the shieldin complex processes SHLD2-bound single-stranded DNA and promotes non-homologous end-joining. Here, we identify a downstream effector of the shieldin complex, ASTE1, as a structure-specific DNA endonuclease that specifically cleaves single-stranded DNA and 3' overhang DNA. ASTE1 localizes to DNA damage sites in a shieldin-dependent manner. Loss of ASTE1 impairs non-homologous end-joining, leads to hyper-resection and causes defective immunoglobulin class switch recombination. ASTE1 deficiency also causes resistance to poly(ADP-ribose) polymerase inhibitors in BRCA1-deficient cells owing to restoration of homologous recombination. These findings suggest that ASTE1-mediated 3' single-stranded DNA end cleavage contributes to the control of DSB repair choice by 53BP1, RIF1 and shieldin.