Authors
Glenn Randall, Maryline Panis, Jacob D Cooper, Timothy L Tellinghuisen, Karen E Sukhodolets, Sebastien Pfeffer, Markus Landthaler, Pablo Landgraf, Sherry Kan, Brett D Lindenbach, Minchen Chien, David B Weir, James J Russo, Jingyue Ju, Michael J Brownstein, Robert Sheridan, Chris Sander, Mihaela Zavolan, Thomas Tuschl, Charles M Rice
Publication date
2007/7/31
Journal
Proceedings of the National Academy of Sciences
Volume
104
Issue
31
Pages
12884-12889
Publisher
National Academy of Sciences
Description
Recently identified hepatitis C virus (HCV) isolates that are infectious in cell culture provide a genetic system to evaluate the significance of virus–host interactions for HCV replication. We have completed a systematic RNAi screen wherein siRNAs were designed that target 62 host genes encoding proteins that physically interact with HCV RNA or proteins or belong to cellular pathways thought to modulate HCV infection. This includes 10 host proteins that we identify in this study to bind HCV NS5A. siRNAs that target 26 of these host genes alter infectious HCV production >3-fold. Included in this set of 26 were siRNAs that target Dicer, a principal component of the RNAi silencing pathway. Contrary to the hypothesis that RNAi is an antiviral pathway in mammals, as has been reported for subgenomic HCV replicons, siRNAs that target Dicer inhibited HCV replication. Furthermore, siRNAs that target several other …
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Scholar articles
G Randall, M Panis, JD Cooper, TL Tellinghuisen… - Proceedings of the National Academy of Sciences, 2007