logo logo
Impeding DNA Break Repair Enables Oocyte Quality Control. Qiao Huanyu,Rao H B D Prasada,Yun Yan,Sandhu Sumit,Fong Jared H,Sapre Manali,Nguyen Michael,Tham Addy,Van Benjamin W,Chng Tiffany Y H,Lee Amy,Hunter Neil Molecular cell Oocyte quality control culls eggs with defects in meiosis. In mouse, oocyte death can be triggered by defects in chromosome synapsis and recombination, which involve repair of DNA double-strand breaks (DSBs) between homologous chromosomes. We show that RNF212, a SUMO ligase required for crossing over, also mediates oocyte quality control. Both physiological apoptosis and wholesale oocyte elimination in meiotic mutants require RNF212. RNF212 sensitizes oocytes to DSB-induced apoptosis within a narrow window as chromosomes desynapse and cells transition into quiescence. Analysis of DNA damage during this transition implies that RNF212 impedes DSB repair. Consistently, RNF212 is required for HORMAD1, a negative regulator of inter-sister recombination, to associate with desynapsing chromosomes. We infer that oocytes impede repair of residual DSBs to retain a "memory" of meiotic defects that enables quality-control processes. These results define the logic of oocyte quality control and suggest RNF212 variants may influence transmission of defective genomes. 10.1016/j.molcel.2018.08.031