New research into HepC with wide implications

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Recent functional genomics studies including genome-wide small 
interfering RNA (siRNA) screens demonstrated that hepatitis C virus 
(HCV) exploits an extensive network of host factors for productive 
infection and propagation. How these co-opted host functions interact 
with various steps of HCV replication cycle and exert pro- or antiviral 
effects on HCV infection remains largely undefined. Here we present an 
unbiased and systematic strategy to functionally interrogate HCV host 
dependencies uncovered from our previous infectious HCV (HCVcc) siRNA 
screen. Applying functional genomics approaches and various in vitro
 HCV model systems, including HCV pseudoparticles (HCVpp), single-cycle 
infectious particles (HCVsc), subgenomic replicons, and HCV cell culture
 systems (HCVcc), we identified and characterized novel host factors or 
pathways required for each individual step of the HCV replication cycle.
 Particularly, we uncovered multiple HCV entry factors, including 
E-cadherin, choline kinase α, NADPH oxidase CYBA, Rho GTPase RAC1 and 
SMAD family member 6. We also demonstrated that guanine nucleotide 
binding protein GNB2L1, E2 ubiquitin-conjugating enzyme UBE2J1, and 39 
other host factors are required for HCV RNA replication, while the 
deubiquitinating enzyme USP11 and multiple other cellular genes are 
specifically involved in HCV IRES-mediated translation. Families of 
antiviral factors that target HCV replication or translation were also 
identified. In addition, various virologic assays validated that 66 host
 factors are involved in HCV assembly or secretion. These genes included
 insulin-degrading enzyme (IDE), a proviral factor, and N-Myc down 
regulated Gene 1 (NDRG1), an antiviral factor. Bioinformatics 
meta-analyses of our results integrated with literature mining of 
previously published HCV host factors allows the construction of an 
extensive roadmap of cellular networks and pathways involved in the 
complete HCV replication cycle. This comprehensive study of HCV host 
dependencies yields novel insights into viral infection, pathogenesis 
and potential therapeutic targets.

Source and full article:   http://www.plospathogens.org/article/info:doi/10.1371/journal.ppat.1004163

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Technophobe Members Profile Send Private Message Find Members Posts Add to Buddy List Assistant Admin Joined: January 16 2014 Location: Scotland Status: Offline Points: 88450	Post Options Post Reply Quote Technophobe Report Post Thanks(0) Quote Reply Topic: New research into HepC with wide implications Posted: May 23 2014 at 3:25am
	Recent functional genomics studies including genome-wide small interfering RNA (siRNA) screens demonstrated that hepatitis C virus (HCV) exploits an extensive network of host factors for productive infection and propagation. How these co-opted host functions interact with various steps of HCV replication cycle and exert pro- or antiviral effects on HCV infection remains largely undefined. Here we present an unbiased and systematic strategy to functionally interrogate HCV host dependencies uncovered from our previous infectious HCV (HCVcc) siRNA screen. Applying functional genomics approaches and various in vitro HCV model systems, including HCV pseudoparticles (HCVpp), single-cycle infectious particles (HCVsc), subgenomic replicons, and HCV cell culture systems (HCVcc), we identified and characterized novel host factors or pathways required for each individual step of the HCV replication cycle. Particularly, we uncovered multiple HCV entry factors, including E-cadherin, choline kinase α, NADPH oxidase CYBA, Rho GTPase RAC1 and SMAD family member 6. We also demonstrated that guanine nucleotide binding protein GNB2L1, E2 ubiquitin-conjugating enzyme UBE2J1, and 39 other host factors are required for HCV RNA replication, while the deubiquitinating enzyme USP11 and multiple other cellular genes are specifically involved in HCV IRES-mediated translation. Families of antiviral factors that target HCV replication or translation were also identified. In addition, various virologic assays validated that 66 host factors are involved in HCV assembly or secretion. These genes included insulin-degrading enzyme (IDE), a proviral factor, and N-Myc down regulated Gene 1 (NDRG1), an antiviral factor. Bioinformatics meta-analyses of our results integrated with literature mining of previously published HCV host factors allows the construction of an extensive roadmap of cellular networks and pathways involved in the complete HCV replication cycle. This comprehensive study of HCV host dependencies yields novel insights into viral infection, pathogenesis and potential therapeutic targets. Source and full article: http://www.plospathogens.org/article/info:doi/10.1371/journal.ppat.1004163
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