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Evidence against the Human Metapneumovirus G, SH, and M2-2 Proteins as Bona Fide Interferon Antagonists

Kevin Groen, Stefan van Nieuwkoop, Mart M. Lamers, Ron A. M. Fouchier, Bernadette van den Hoogen

2022Journal of Virology15 citationsDOIOpen Access PDF

Abstract

Understanding the interaction between viruses and the innate immune response is one of the barriers to the design of antiviral therapies. Here, we investigated the role of the G, SH, and M2-2 proteins of HMPV as type I IFN antagonists. In contrast to other studies, no IFN-antagonistic functions could be observed for the G and SH proteins. HMPV with a deletion of the M2-2 protein did induce type I IFN production upon infection of airway epithelial cells. However, during generation of virus stocks, these viruses rapidly accumulated DIs, which are strong activators of the type I IFN response. Additionally, the genomes of these viruses were hypermutated, which was prevented by generating stocks in ADAR knockdown cells, confirming a role for ADAR in hypermutation of HMPV genomes or DIs. These data indicate that a role of the HMPV M2-2 protein as a bona fide IFN antagonist remains elusive.

Topics & Concepts

BiologyInnate immune systemVirologyInterferonVirusViral replicationHuman metapneumovirusGeneticsImmune systemRespiratory tract infectionsAnatomyRespiratory systemViral Infections and Immunology ResearchRespiratory viral infections researchViral gastroenteritis research and epidemiology