DNA double-strand breaks induce H2Ax phosphorylation domains in a contact-dependent manner.

Patrick L Collins, Caitlin Purman, Sofia I Porter, Vincent Nganga, Ankita Saini, Katharina E Hayer, Greer L Gurewitz, Barry P Sleckman, Jeffrey J Bednarski, Craig H Bassing, Eugene M Oltz

Nature communications 2020 Jun 22

filter terms:

Efficient repair of DNA double-strand breaks (DSBs) requires a coordinated DNA Damage Response (DDR), which includes phosphorylation of histone H2Ax, forming γH2Ax. This histone modification spreads beyond the DSB into neighboring chromatin, generating a DDR platform that protects against end disassociation and degradation, minimizing chromosomal rearrangements. However, mechanisms that determine the breadth and intensity of γH2Ax domains remain unclear. Here, we show that chromosomal contacts of a DSB site are the primary determinants for γH2Ax landscapes. DSBs that disrupt a topological border permit extension of γH2Ax domains into both adjacent compartments. In contrast, DSBs near a border produce highly asymmetric DDR platforms, with γH2Ax nearly absent from one broken end. Collectively, our findings lend insights into a basic DNA repair mechanism and how the precise location of a DSB may influence genome integrity.

Citation

Patrick L Collins, Caitlin Purman, Sofia I Porter, Vincent Nganga, Ankita Saini, Katharina E Hayer, Greer L Gurewitz, Barry P Sleckman, Jeffrey J Bednarski, Craig H Bassing, Eugene M Oltz. DNA double-strand breaks induce H2Ax phosphorylation domains in a contact-dependent manner. Nature communications. 2020 Jun 22;11(1):3158