MRNA 3'UTR Lengthening by Alternative Polyadenylation Attenuates Inflammatory Responses and Correlates with Virulence of Influenza A Virus

Overview

Journal Nat Commun

Specialty Biology

Date 2023 Aug 15

PMID 37582777

Authors

Valter Bergant

Daniel Schnepf

Niklas de Andrade Kratzig

Philipp Hubel

Christian Urban

Thomas Engleitner

Ronald Dijkman

Bernhard Ryffel

Katja Steiger

Percy A Knolle

Georg Kochs

Roland Rad

Peter Staeheli

Andreas Pichlmair

Affiliations

Soon will be listed here.

Abstract

Changes of mRNA 3'UTRs by alternative polyadenylation (APA) have been associated to numerous pathologies, but the mechanisms and consequences often remain enigmatic. By combining transcriptomics, proteomics and recombinant viruses we show that all tested strains of IAV, including A/PR/8/34(H1N1) (PR8) and A/Cal/07/2009 (H1N1) (Cal09), cause APA. We mapped the effect to the highly conserved glycine residue at position 184 (G184) of the viral non-structural protein 1 (NS1). Unbiased mass spectrometry-based analyses indicate that NS1 causes APA by perturbing the function of CPSF4 and that this function is unrelated to virus-induced transcriptional shutoff. Accordingly, IAV strain PR8, expressing an NS1 variant with weak CPSF binding, does not induce host shutoff but only APA. However, recombinant IAV (PR8) expressing NS1(G184R) lacks binding to CPSF4 and thereby also the ability to cause APA. Functionally, the impaired ability to induce APA leads to an increased inflammatory cytokine production and an attenuated phenotype in a mouse infection model. Investigating diverse viral infection models showed that APA induction is a frequent ability of many pathogens. Collectively, we propose that targeting of the CPSF complex, leading to widespread alternative polyadenylation of host transcripts, constitutes a general immunevasion mechanism employed by a variety of pathogenic viruses.

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