ADAR-mediated RNA editing of DNA:RNA hybrids is required for DNA double strand break repair

Author:

Jimeno Sonia,Prados-Carvajal Rosario,Fernández-Ávila María JesúsORCID,Silva SoniaORCID,Silvestris Domenico Alessandro,Endara-Coll Martín,Rodríguez-Real Guillermo,Domingo-Prim JuditORCID,Mejías-Navarro FernandoORCID,Romero-Franco Amador,Jimeno-González SilviaORCID,Barroso SoniaORCID,Cesarini Valeriana,Aguilera AndrésORCID,Gallo Angela,Visa NeusORCID,Huertas PabloORCID

Abstract

AbstractThe maintenance of genomic stability requires the coordination of multiple cellular tasks upon the appearance of DNA lesions. RNA editing, the post-transcriptional sequence alteration of RNA, has a profound effect on cell homeostasis, but its implication in the response to DNA damage was not previously explored. Here we show that, in response to DNA breaks, an overall change of the Adenosine-to-Inosine RNA editing is observed, a phenomenon we call the RNA Editing DAmage Response (REDAR). REDAR relies on the checkpoint kinase ATR and the recombination factor CtIP. Moreover, depletion of the RNA editing enzyme ADAR2 renders cells hypersensitive to genotoxic agents, increases genomic instability and hampers homologous recombination by impairing DNA resection. Such a role of ADAR2 in DNA repair goes beyond the recoding of specific transcripts, but depends on ADAR2 editing DNA:RNA hybrids to ease their dissolution.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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