Processing of matched and mismatched rNMPs in DNA by archaeal ribonucleotide excision repair

Maurane Reveil; Lucie Chapel; Blandine Vourc'h; Audrey Bossé; Léa Vialle; Raphaël Brizard; Yann Moalic; Mohamed Jebbar; Ghislaine Henneke

doi:10.1016/j.isci.2023.108479

Processing of matched and mismatched rNMPs in DNA by archaeal ribonucleotide excision repair

iScience. 2023 Nov 17;26(12):108479. doi: 10.1016/j.isci.2023.108479. eCollection 2023 Dec 15.

Authors

Maurane Reveil¹, Lucie Chapel¹, Blandine Vourc'h¹, Audrey Bossé¹, Léa Vialle¹, Raphaël Brizard¹, Yann Moalic¹, Mohamed Jebbar¹, Ghislaine Henneke¹

Affiliation

¹ University Brest, CNRS, Ifremer, UMR6197 Biologie et Ecologie des Ecosystèmes marins Profonds, 1625 Rte de Sainte-Anne, 29280 Plouzané, France.

Abstract

Ribonucleoside monophosphates (rNMPs) are the main non-canonical nucleotides in genomic DNA, and their incorporation can occur as mismatches or matches in vivo. To counteract the mutagenic potential of rNMPs in DNA, all organisms evolved ribonucleotide excision repair (RER), a mechanism initiated by type 2 RNase H. Here, we describe the in vitro reconstitution of matched and mismatched rNMP repair using archaeal RER enzymes. Our data suggest two types of RER pathways, including the classical flap RER and a backup RER with the order of reactions changed for Fen1 and Pols. The genomic rNMP level in RER-deficient or PolB-deficient archaeal cells along with in vitro reconstitution of RER suggests an in vivo role of PolD in RER. Our results provide insights into how matched and mismatched rNMPs may be processed by RER.

Keywords: Bacteriology; Biochemistry; Molecular biology.