Different SWI/SNF complexes coordinately promote R-loop- and RAD52-dependent transcription-coupled homologous recombination

Author:

Davó-Martínez Carlota1ORCID,Helfricht Angela1,Ribeiro-Silva Cristina1,Raams Anja1,Tresini Maria1,Uruci Sidrit1,van Cappellen Wiggert A2,Taneja Nitika1,Demmers Jeroen A A3,Pines Alex1,Theil Arjan F1ORCID,Vermeulen Wim1ORCID,Lans Hannes1ORCID

Affiliation:

1. Department of Molecular Genetics, Erasmus MC Cancer Institute, Erasmus University Medical Center , Rotterdam  3015 GD , The Netherlands

2. Erasmus Optical Imaging Center, Erasmus University Medical Center , Rotterdam  3015 GD , The Netherlands

3. Proteomics Center, Erasmus University Medical Center , Rotterdam  3015 GD , The Netherlands

Abstract

Abstract The SWI/SNF family of ATP-dependent chromatin remodeling complexes is implicated in multiple DNA damage response mechanisms and frequently mutated in cancer. The BAF, PBAF and ncBAF complexes are three major types of SWI/SNF complexes that are functionally distinguished by their exclusive subunits. Accumulating evidence suggests that double-strand breaks (DSBs) in transcriptionally active DNA are preferentially repaired by a dedicated homologous recombination pathway. We show that different BAF, PBAF and ncBAF subunits promote homologous recombination and are rapidly recruited to DSBs in a transcription-dependent manner. The PBAF and ncBAF complexes promote RNA polymerase II eviction near DNA damage to rapidly initiate transcriptional silencing, while the BAF complex helps to maintain this transcriptional silencing. Furthermore, ARID1A-containing BAF complexes promote RNaseH1 and RAD52 recruitment to facilitate R-loop resolution and DNA repair. Our results highlight how multiple SWI/SNF complexes perform different functions to enable DNA repair in the context of actively transcribed genes.

Funder

Netherlands Organization for Scientific Research

Worldwide Cancer Research

Dutch Cancer Society KWF

European Research Council

CancerGenomiCs.nl from Netherlands Organization for Scientific Research

Oncode Institute

Dutch Cancer Society

Publisher

Oxford University Press (OUP)

Subject

Genetics

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