Replication of Hepatitis C Virus (HCV) RNA in Mouse Embryonic Fibroblasts: Protein Kinase R (PKR)-Dependent and PKR-Independent Mechanisms for Controlling HCV RNA Replication and Mediating Interferon Activities

doi:10.1128/JVI.00586-06

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Journal of Virology, August 2006, p. 7364-7374, Vol. 80, No. 15
0022-538X/06/$08.00+0 doi:10.1128/JVI.00586-06
Copyright © 2006, American Society for Microbiology. All Rights Reserved.

Replication of Hepatitis C Virus (HCV) RNA in Mouse Embryonic Fibroblasts: Protein Kinase R (PKR)-Dependent and PKR-Independent Mechanisms for Controlling HCV RNA Replication and Mediating Interferon Activities

Kyung-Soo Chang,¹ Zhaohui Cai,¹ Chen Zhang,¹ Ganes C. Sen,² Bryan R. G. Williams,²^,3 and Guangxiang Luo¹^*

Department of Microbiology, Immunology, and Molecular Genetics, University of Kentucky College of Medicine, 800 Rose Street, Lexington, Kentucky 40536-0298,¹ Lerner Research Institute, Cleveland Clinic Foundation, Cleveland, Ohio 44195,² Monash Institute of Medical Research, Monash University, Melbourne, Australia³

Received 23 March 2006/ Accepted 9 May 2006

Hepatitis C virus (HCV) infection causes chronic hepatitis andis currently treated with alpha interferon (IFN- ${alpha}$ )-based therapies.The underlying mechanisms of chronic HCV infection and IFN-basedtherapies, however, have not been defined. Protein kinase R(PKR) was implicated in the control of HCV replication and mediationof IFN-induced antiviral response. In this report, we demonstratethat a subgenomic RNA replicon of genotype 2a HCV replicatedefficiently in mouse embryonic fibroblasts (MEFs), as determinedby cell colony formation efficiency and the detection of HCVproteins and both positive- and negative-strand RNAs. Additionally,the subgenomic HCV RNA was found to replicate more efficientlyin the PKR knockout (PKR^–/–) MEF than in the wild-type(PKR^+/+) MEF. The knockdown expression of PKR by specific smallinterfering RNAs significantly enhanced the level of HCV RNAreplication, suggesting that PKR is involved in the controlof HCV RNA replication. The level of ISG56 (p56) was inducedby HCV RNA replication, indicating the activation of PKR-independentantiviral pathways. Furthermore, IFN- ${alpha}$ /ß inhibitedHCV RNA replication in PKR^–/– MEFs as efficientlyas in PKR^+/+ MEFs. These findings demonstrate that PKR-independentantiviral pathways play important roles in controlling HCV replicationand mediating IFN-induced antiviral effect. Our findings alsoprovide a foundation for the development of transgenic mousemodels of HCV replication and set a stage to further definethe roles of cellular genes in the establishment of chronicHCV infection and the mediation of intracellular innate antiviralresponse by using MEFs derived from diverse gene knockout animals.

* Corresponding author. Mailing address: Department of Microbiology, Immunology, and Molecular Genetics, University of Kentucky College of Medicine, 800 Rose St., Lexington, KY 40536-0298. Phone: (859) 257-5577. Fax: (859) 257-8994. E-mail: gluo0{at}uky.edu.

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