Poly(ADP-Ribose) Mediates the BRCA2-Dependent Early DNA Damage Response

Breast cancer susceptibility gene 2 (BRCA2) plays a key role in DNA damage repair for maintaining genomic stability. Previous studies have shown that BRCA2 contains three tandem oligonucleotide/oligosaccharide binding folds (OB-folds) that are involved in DNA binding during DNA double-strand break repair. However, the molecular mechanism of BRCA2 in DNA damage repair remains elusive. Unexpectedly, we found that the OB-folds of BRCA2 recognize poly(ADP-ribose) (PAR) and mediate the fast recruitment of BRCA2 to DNA lesions, which is suppressed by PARP inhibitor treatment. Cancer-associated mutations in the OB-folds of BRCA2 disrupt the interaction with PAR and abolish the fast relocation of BRCA2 to DNA lesions. The quickly recruited BRCA2 is important for the early recruitment of exonuclease 1(EXO1) and is involved in DNA end resection, the first step of homologous recombination (HR). Thus, these findings uncover a molecular mechanism by which BRCA2 participates in DNA damage repair. [Display omitted] •OB-folds of BRCA2 recognize DNA-damage-induced poly(ADP-ribosyl)ation•PARylation and OB-folds of BRCA2 mediate the fast recruitment of BRCA2 to DNA lesions•The early recruitment of BRCA2 is important for EXO1-dependent DNA end resection Zhang et al. show that BRCA2 OB-folds act as a poly(ADP-ribose)-binding module and mediate the fast recruitment of BRCA2 to DNA lesions. The early recruitment of BRCA2 is important for EXO1-dependent DNA end resection, the initial step of homologous recombination (HR) repair.