Background & aims: Current treatment strategies for hepatitis C virus (HCV) infection include pegylated interferon (IFN)-alfa and ribavirin. Approximately 50% of patients control HCV infection after treatment, but the broad range of patients' outcomes and responses to treatment, among all genotypes, indicates a role for host factors. Although the IFN system is important in limiting HCV replication, the virus has evolved mechanisms to circumvent the IFN response. However, direct, IFN-independent antiviral processes also might help control HCV replication. We examined the role of IFN-independent responses against HCV replication.
Methods: We analyzed replication of the subgenomic JFH1 replicon in embryonic fibroblasts and primary hepatocytes from mice with disruptions in genes encoding factors in the IFN-dependent and alternative antiviral pathways (signal transducers and activators of transcription 1 [STAT1], protein kinase R, interferon regulatory factors (IRF) IRF-1, IRF-3, IRF-5, IRF-7, mitochondrial antiviral signaling molecule [MAVS], and IFN receptor [IFNAR]). We also assessed the effects of expression of these factors by mouse primary hepatocytes on HCV replication.
Results: In addition to IRF-3- and IFN-mediated antiviral responses, IFN-independent, but IRF-1- and IRF-5-dependent mechanisms, restrict HCV replication in mouse embryonic fibroblasts. In primary hepatocytes these IFN-independent require MAVS and IRF-1.
Conclusions: HCV replication is limited by interferon-mediated pathways as well pathways that are independent of type I IFNs. IRF1 and IRF5 control IFN-independent signaling events that lead to antiviral responses. We observed antiviral roles of IRF1 and IRF5 that were IFN-independent and cell-type specific. These mechanisms are important in controlling viruses that interfere with the IFN signaling because cells retain the ability to induce functional but local antiviral states through expression of interferon-stimulated genes.
Keywords: HCV; IFN; IFN-Independent; IFNAR; IRES; IRF; ISG; Interferon Regulatory Factor; JFH; JFH1 replicon with deletion of the GDD motif of NS5B; JFH1ΔGDD; Japanese fulminant hepatitis; MAVS; MEF; Mouse Embryonic Fibroblasts; PBS; PKR; Primary Mouse Hepatocytes; STAT; WT; hepatitis C virus; interferon; interferon regulatory factors; interferon-stimulated genes; internal ribosomal entry site; miR; microRNA; mitochondrial antiviral signaling molecule; mouse embryonic fibroblast; phosphate-buffered saline; protein kinase R; signal transducers and activators of transcription; type I interferon receptor; wild type.
Copyright © 2013 AGA Institute. Published by Elsevier Inc. All rights reserved.