Guévin, Carl; Manna, David; Bélanger, Claudia; Konan, Kouacou V.; Mak, Paul et Labonté, Patrick ORCID: https://orcid.org/0000-0001-7262-3125 (2010). Autophagy protein ATG5 interacts transiently with the hepatitis C virus RNA polymerase (NS5B) early during infection Virology , vol. 405 , nº 1. pp. 1-7. DOI: 10.1016/j.virol.2010.05.032.
Ce document n'est pas hébergé sur EspaceINRS.Résumé
Autophagy is an important cellular process by which ATG5 initiates the formation of double membrane vesicles (DMVs). Upon infection, DMVs have been shown to harbor the replicase complex of positive-strand RNA viruses such as MHV, poliovirus, and equine arteritis virus. Recently, it has been shown that autophagy proteins are proviral factors that favor initiation of hepatitis C virus (HCV) infection. Here, we identified ATG5 as an interacting protein for the HCV NS5B. ATG5/NS5B interaction was confirmed by co-IP and metabolic labeling studies. Furthermore, ATG5 protein colocalizes with NS4B, a constituent of the membranous web. Importantly, immunofluorescence staining demonstrated a strong colocalization of ATG5 and NS5B within perinuclear regions of infected cells at 2 days postinfection. However, colocalization was completely lacking at 5DPI, suggesting that HCV utilizes ATG5 as a proviral factor during the onset of viral infection. Finally, inhibition of autophagy through ATG5 silencing blocks HCV replication.
Type de document: | Article |
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Mots-clés libres: | HCV; Autophagy; ATG5; RdRp; NS5B; siRNA |
Centre: | Centre INRS-Institut Armand Frappier |
Date de dépôt: | 30 juin 2024 21:06 |
Dernière modification: | 30 juin 2024 21:06 |
URI: | https://espace.inrs.ca/id/eprint/14733 |
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