NUDT2 initiates viral RNA degradation by removal of 5′-phosphates

While viral replication processes are largely understood, comparably little is known on cellular mechanisms degrading viral RNA. Some viral RNAs bear a 5′-triphosphate (PPP-) group that impairs degradation by the canonical 5′-3′ degradation pathway. Here we show that the Nudix hydrolase 2 (NUDT2) tr...

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Veröffentlicht in:Nature communications 2021-11, Vol.12 (1), p.6918-13, Article 6918
Hauptverfasser: Laudenbach, Beatrice T., Krey, Karsten, Emslander, Quirin, Andersen, Line Lykke, Reim, Alexander, Scaturro, Pietro, Mundigl, Sarah, Dächert, Christopher, Manske, Katrin, Moser, Markus, Ludwig, Janos, Wohlleber, Dirk, Kröger, Andrea, Binder, Marco, Pichlmair, Andreas
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Sprache:eng
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Zusammenfassung:While viral replication processes are largely understood, comparably little is known on cellular mechanisms degrading viral RNA. Some viral RNAs bear a 5′-triphosphate (PPP-) group that impairs degradation by the canonical 5′-3′ degradation pathway. Here we show that the Nudix hydrolase 2 (NUDT2) trims viral PPP-RNA into monophosphorylated (P)-RNA, which serves as a substrate for the 5′-3′ exonuclease XRN1. NUDT2 removes 5′-phosphates from PPP-RNA in an RNA sequence- and overhang-independent manner and its ablation in cells increases growth of PPP-RNA viruses, suggesting an involvement in antiviral immunity. NUDT2 is highly homologous to bacterial RNA pyrophosphatase H (RppH), a protein involved in the metabolism of bacterial mRNA, which is 5′-tri- or diphosphorylated. Our results show a conserved function between bacterial RppH and mammalian NUDT2, indicating that the function may have adapted from a protein responsible for RNA turnover in bacteria into a protein involved in the immune defense in mammals. RNA of some viruses is protected from degradation by a 5′ triphosphate group. Here the authors identify nudix hydrolase 2 (NUDT2) as novel antiviral defense protein that dephosphorylates viral RNA and thereby enables its degradation.
ISSN:2041-1723
2041-1723
DOI:10.1038/s41467-021-27239-y