Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells

Here we demonstrate that primary cultures of human fetal liver cells (HFLC) reliably support infection with laboratory strains of hepatitis C virus (HCV), although levels of virus replication vary significantly between different donor cell preparations and frequently decline in a manner suggestive o...

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Autores principales: Andrus, Linda, Marukian, Svetlana, Jones, Christopher T, Catanese, Maria Teresa, Sheahan, Timothy P, Schoggins, John W, Barry, Walter T, Dustin, Lynn B, Trehan, Kartik, Ploss, Alexander, Bhatia, Sangeeta N, Rice, Charles M
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Wiley Subscription Services, Inc., A Wiley Company 2011
Materias:
Viral Hepatitis
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3233237/
https://www.ncbi.nlm.nih.gov/pubmed/22144107
http://dx.doi.org/10.1002/hep.24557
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author Andrus, Linda
Marukian, Svetlana
Jones, Christopher T
Catanese, Maria Teresa
Sheahan, Timothy P
Schoggins, John W
Barry, Walter T
Dustin, Lynn B
Trehan, Kartik
Ploss, Alexander
Bhatia, Sangeeta N
Rice, Charles M
author_facet Andrus, Linda
Marukian, Svetlana
Jones, Christopher T
Catanese, Maria Teresa
Sheahan, Timothy P
Schoggins, John W
Barry, Walter T
Dustin, Lynn B
Trehan, Kartik
Ploss, Alexander
Bhatia, Sangeeta N
Rice, Charles M
author_sort Andrus, Linda
collection PubMed
description Here we demonstrate that primary cultures of human fetal liver cells (HFLC) reliably support infection with laboratory strains of hepatitis C virus (HCV), although levels of virus replication vary significantly between different donor cell preparations and frequently decline in a manner suggestive of active viral clearance. To investigate possible contributions of the interferon (IFN) system to control HCV infection in HFLC, we exploited the well-characterized ability of paramyxovirus (PMV) V proteins to counteract both IFN induction and antiviral signaling. The V proteins of measles virus (MV) and parainfluenza virus 5 (PIV5) were introduced into HFLC using lentiviral vectors encoding a fluorescent reporter for visualization of HCV-infected cells. V protein-transduced HFLC supported enhanced (10 to 100-fold) levels of HCV infection relative to untransduced or control vector-transduced HFLC. Infection was assessed by measurement of virus-driven luciferase, by assays for infectious HCV and viral RNA, and by direct visualization of HCV-infected hepatocytes. Live cell imaging between 48 and 119 hours postinfection demonstrated little or no spread of infection in the absence of PMV V protein expression. In contrast, V protein-transduced HFLC showed numerous HCV infection events. V protein expression efficiently antagonized the HCV-inhibitory effects of added IFNs in HFLC. In addition, induction of the type III IFN, IL29, following acute HCV infection was inhibited in V protein-transduced cultures. Conclusion: These studies suggest that the cellular IFN response plays a significant role in limiting the spread of HCV infection in primary hepatocyte cultures. Strategies aimed at dampening this response may be key to further development of robust HCV culture systems, enabling studies of virus pathogenicity and the mechanisms by which HCV spreads in its natural host cell population. (Hepatology 2011;54:1901-1912)
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spelling pubmed-32332372012-11-26 Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells Andrus, Linda Marukian, Svetlana Jones, Christopher T Catanese, Maria Teresa Sheahan, Timothy P Schoggins, John W Barry, Walter T Dustin, Lynn B Trehan, Kartik Ploss, Alexander Bhatia, Sangeeta N Rice, Charles M Hepatology Viral Hepatitis Here we demonstrate that primary cultures of human fetal liver cells (HFLC) reliably support infection with laboratory strains of hepatitis C virus (HCV), although levels of virus replication vary significantly between different donor cell preparations and frequently decline in a manner suggestive of active viral clearance. To investigate possible contributions of the interferon (IFN) system to control HCV infection in HFLC, we exploited the well-characterized ability of paramyxovirus (PMV) V proteins to counteract both IFN induction and antiviral signaling. The V proteins of measles virus (MV) and parainfluenza virus 5 (PIV5) were introduced into HFLC using lentiviral vectors encoding a fluorescent reporter for visualization of HCV-infected cells. V protein-transduced HFLC supported enhanced (10 to 100-fold) levels of HCV infection relative to untransduced or control vector-transduced HFLC. Infection was assessed by measurement of virus-driven luciferase, by assays for infectious HCV and viral RNA, and by direct visualization of HCV-infected hepatocytes. Live cell imaging between 48 and 119 hours postinfection demonstrated little or no spread of infection in the absence of PMV V protein expression. In contrast, V protein-transduced HFLC showed numerous HCV infection events. V protein expression efficiently antagonized the HCV-inhibitory effects of added IFNs in HFLC. In addition, induction of the type III IFN, IL29, following acute HCV infection was inhibited in V protein-transduced cultures. Conclusion: These studies suggest that the cellular IFN response plays a significant role in limiting the spread of HCV infection in primary hepatocyte cultures. Strategies aimed at dampening this response may be key to further development of robust HCV culture systems, enabling studies of virus pathogenicity and the mechanisms by which HCV spreads in its natural host cell population. (Hepatology 2011;54:1901-1912) Wiley Subscription Services, Inc., A Wiley Company 2011-12 2011-12-02 /pmc/articles/PMC3233237/ /pubmed/22144107 http://dx.doi.org/10.1002/hep.24557 Text en Copyright © 2011 American Association for the Study of Liver Diseases http://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Viral Hepatitis
Andrus, Linda
Marukian, Svetlana
Jones, Christopher T
Catanese, Maria Teresa
Sheahan, Timothy P
Schoggins, John W
Barry, Walter T
Dustin, Lynn B
Trehan, Kartik
Ploss, Alexander
Bhatia, Sangeeta N
Rice, Charles M
Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells
title Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells
title_full Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells
title_fullStr Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells
title_full_unstemmed Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells
title_short Expression of Paramyxovirus V Proteins Promotes Replication and Spread of Hepatitis C Virus in Cultures of Primary Human Fetal Liver Cells
title_sort expression of paramyxovirus v proteins promotes replication and spread of hepatitis c virus in cultures of primary human fetal liver cells
topic Viral Hepatitis
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3233237/
https://www.ncbi.nlm.nih.gov/pubmed/22144107
http://dx.doi.org/10.1002/hep.24557
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