Regulation of DNA Repair through DeSUMOylation and SUMOylation of Replication Protein A Complex

SummaryThe replication protein A complex (RPA) plays a crucial role in DNA replication and damage response. However, it is not known whether this complex is regulated by the SUMOylation pathway. Here, we show that the 70 kDa subunit of RPA (RPA70) associates with a Sentrin/SUMO-specific protease, SENP6, in the nucleus to maintain RPA70 in a hypoSUMOylated state during S phase. Campothecin (CPT), an inducer of replication stress, dissociates SENP6 from RPA70, allowing RPA70 to be modified by a small ubiquitin-like modifier 2/3 (SUMO-2/3). RPA70 SUMOylation facilitates recruitment of Rad51 to the DNA damage foci to initiate DNA repair through homologous recombination (HR). Cell lines that expressed a RPA70 mutant that cannot be SUMOylated are defective in HR and have a marked increase in sensitivity to CPT. These results demonstrate that SUMOylation status of RPA70 plays a critical role in the regulation of DNA repair through homologous recombination.

Graphical AbstractFigure optionsDownload high-quality image (120 K)Download as PowerPoint slideHighlights
► SENP6 associates with RPA70 in S phase, keeping RPA70 in a hypoSUMOylated state
► DSB dissociates SENP6 from RPA70, allowing RPA70 to be modified by SUMO2/3
► RPA70 SUMOylation facilitates the recruitment of Rad51 to initiate HR
► SUMOylation of RPA70 is important DNA repair by HR