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ssDNA accessibility of Rad51 is regulated by orchestrating multiple RPA dynamics

Jiawei Ding, Xiangting Li, Jiangchuan Shen, Yiling Zhao, Shuchen Zhong, Luhua Lai, Hengyao Niu () and Zhi Qi ()
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Jiawei Ding: Peking University
Xiangting Li: University of California
Jiangchuan Shen: Indiana University
Yiling Zhao: Peking University
Shuchen Zhong: Peking University
Luhua Lai: Peking University
Hengyao Niu: Indiana University
Zhi Qi: Peking University

Nature Communications, 2023, vol. 14, issue 1, 1-17

Abstract: Abstract The eukaryotic single-stranded DNA (ssDNA)-binding protein Replication Protein A (RPA) plays a crucial role in various DNA metabolic pathways, including DNA replication and repair, by dynamically associating with ssDNA. While the binding of a single RPA molecule to ssDNA has been thoroughly studied, the accessibility of ssDNA is largely governed by the bimolecular behavior of RPA, the biophysical nature of which remains unclear. In this study, we develop a three-step low-complexity ssDNA Curtains method, which, when combined with biochemical assays and a Markov chain model in non-equilibrium physics, allow us to decipher the dynamics of multiple RPA binding to long ssDNA. Interestingly, our results suggest that Rad52, the mediator protein, can modulate the ssDNA accessibility of Rad51, which is nucleated on RPA coated ssDNA through dynamic ssDNA exposure between neighboring RPA molecules. We find that this process is controlled by the shifting between the protection mode and action mode of RPA ssDNA binding, where tighter RPA spacing and lower ssDNA accessibility are favored under RPA protection mode, which can be facilitated by the Rfa2 WH domain and inhibited by Rad52 RPA interaction.

Date: 2023
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DOI: 10.1038/s41467-023-39579-y

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