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The DEAD box RNA helicase DDX42 is an intrinsic inhibitor of positive‐strand RNA viruses

Boris Bonaventure, Antoine Rebendenne, Ana Luiza Chaves Valadão, Mary Arnaud‐Arnould, Ségolène Gracias, Francisco García-de-Gracia, Joe McKellar, Emmanuel Labaronne, Marine Tauziet, Valérie Vivet‐Boudou, Éric Bernard, Laurence Briant, Nathalie Gros, Wassila Djilli, Valérie Courgnaud, Hugues Parrinello, Stéphanie Rialle, Mickaël Blaise, Laurent Lacroix, Marc Lavigne, Jean‐Christophe Paillart, Emiliano P. Ricci, Reiner Schulz, Nolwenn Jouvenet, Olivier Moncorgé, Caroline Goujon

2022EMBO Reports17 citationsDOIOpen Access PDF

Abstract

Genome‐wide screens are powerful approaches to unravel regulators of viral infections. Here, a CRISPR screen identifies the RNA helicase DDX42 as an intrinsic antiviral inhibitor of HIV‐1. Depletion of endogenous DDX42 increases HIV‐1 DNA accumulation and infection in cell lines and primary cells. DDX42 overexpression inhibits HIV‐1 infection, whereas expression of a dominant‐negative mutant increases infection. Importantly, DDX42 also restricts LINE‐1 retrotransposition and infection with other retroviruses and positive‐strand RNA viruses, including CHIKV and SARS‐CoV‐2. However, DDX42 does not impact the replication of several negative‐strand RNA viruses, arguing against an unspecific effect on target cells, which is confirmed by RNA‐seq analysis. Proximity ligation assays show DDX42 in the vicinity of viral elements, and cross‐linking RNA immunoprecipitation confirms a specific interaction of DDX42 with RNAs from sensitive viruses. Moreover, recombinant DDX42 inhibits HIV‐1 reverse transcription in vitro. Together, our data strongly suggest a direct mode of action of DDX42 on viral ribonucleoprotein complexes. Our results identify DDX42 as an intrinsic viral inhibitor, opening new perspectives to target the life cycle of numerous RNA viruses. A CRISPR screen identifies the helicase DDX42 as an intrinsic inhibitor of HIV‐1. DDX42 also inhibits replication of various positive‐strand viruses, with a strong impact on coronaviruses, possibly through binding viral RNAs. A CRISPR screen identifies the helicase DDX42 as an intrinsic inhibitor of HIV‐1. DDX42 also inhibits replication of various positive‐strand viruses, with a strong impact on coronaviruses, possibly through binding viral RNAs.

Topics & Concepts

RNABiologyRNA Helicase ARibonucleoproteinRNA silencingViral replicationTranscription (linguistics)RNA-dependent RNA polymeraseVirologyHelicaseMolecular biologyCell biologyVirusRNA interferenceGeneticsGeneLinguisticsPhilosophyHIV Research and TreatmentRNA Research and SplicingViral Infections and Immunology Research