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Human RAD52 double-ring remodels replication forks restricting fork reversal.

Masayoshi HondaMortezaali RazzaghiParas GaurEva MalacariaLudovica Di BiagiFrancesca Antonella AielloEmeleeta A PaintsilAndrew StanfieldBailey J DeppeLokesh GakharNicholas J SchnickerM Ashley SpiesPietro PichierriMaria Spies
Published in: bioRxiv : the preprint server for biology (2023)
Human RAD52 1,2 is a multifunctional DNA repair protein involved in several cellular events that support genome stability including protection of stalled DNA replication forks from excessive degradation 3-7 . In its gatekeeper role, RAD52 binds to and stabilizes stalled replication forks during replication stress protecting them from reversal by SMARCAL1 5 . The structural and molecular mechanism of the RAD52-mediated fork protection remains elusive. Here, using P1 nuclease sensitivity, biochemical and single-molecule analyses we show that RAD52 dynamically remodels replication forks through its strand exchange activity. The presence of the ssDNA binding protein RPA at the fork modulates the kinetics of the strand exchange without impeding the reaction outcome. Mass photometry and single-particle cryo-electron microscopy show that the replication fork promotes a unique nucleoprotein structure containing head-to-head arrangement of two undecameric RAD52 rings with an extended positively charged surface that accommodates all three arms of the replication fork. We propose that the formation and continuity of this surface is important for the strand exchange reaction and for competition with SMARCAL1.
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