| Literature DB >> 27342813 |
Hongren Qu1, Jing Li2, Limin Yang2, Lei Sun2, Wenjun Liu3, Hongxuan He4.
Abstract
Influenza A virus (IAV) is an important pathogen that has a wide range of hosts and represents a threat to the health of humans and several animal species. IAV infection can induce the transcription of many genes in the host. In the present study, we demonstrated for the first time that three different strains of H1N1 IAV induce the expression of an IFN-stimulated gene, ISG20. We determined the antiviral activity of ISG20 against IAV because ISG20 inhibited viral protein expression and reduced the progeny viral titer dependent upon its exonuclease activity. To elucidate the detailed mechanism of ISG20, we further demonstrated that ISG20 impairs the polymerase activity and inhibits both the replication and transcription levels of the M1 and NP genes. Notably, we identified that ISG20 colocalizes and interacts with NP during IAV infection, while exonuclease-inactive mutant ISG20 lacked association with NP, indicating that ISG20 inhibits IAV replication by interacting with NP. Together, these data provide a detailed explanation for the specific antiviral action of ISG20 and suggest that ISG20 may act as a promising antiviral drug candidate against IAV.Entities:
Keywords: Exonuclease; IFN-stimulated gene; Polymerase activity
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Year: 2016 PMID: 27342813 DOI: 10.1007/s11262-016-1366-2
Source DB: PubMed Journal: Virus Genes ISSN: 0920-8569 Impact factor: 2.332