| Literature DB >> 33536619 |
Liana Goehring1,2,3, Serena Landini1,2,3, Konstantina Skourti-Stathaki4, Elodie Hatchi5,6,7, Derrick K DeConti8, Fieda O Abderazzaq1,2,3, Priyankana Banerjee1,2,3, Timothy M Demers1,2,3, Yaoyu E Wang8, John Quackenbush8, David M Livingston9,10,11.
Abstract
Strong connections exist between R-loops (three-stranded structures harbouring an RNA:DNA hybrid and a displaced single-strand DNA), genome instability and human disease1-5. Indeed, R-loops are favoured in relevant genomic regions as regulators of certain physiological processes through which homeostasis is typically maintained. For example, transcription termination pause sites regulated by R-loops can induce the synthesis of antisense transcripts that enable the formation of local, RNA interference (RNAi)-driven heterochromation6. Pause sites are also protected against endogenous single-stranded DNA breaks by BRCA17. Hypotheses about how DNA repair is enacted at pause sites include a role for RNA, which is emerging as a normal, albeit unexplained, regulator of genome integrity8. Here we report that a species of single-stranded, DNA-damage-associated small RNA (sdRNA) is generated by a BRCA1-RNAi protein complex. sdRNAs promote DNA repair driven by the PALB2-RAD52 complex at transcriptional termination pause sites that form R-loops and are rich in single-stranded DNA breaks. sdRNA repair operates in both quiescent (G0) and proliferating cells. Thus, sdRNA repair can occur in intact tissue and/or stem cells, and may contribute to tumour suppression mediated by BRCA1.Entities:
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Year: 2021 PMID: 33536619 PMCID: PMC8245199 DOI: 10.1038/s41586-020-03150-2
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 69.504