Expanding the Host Range of Hepatitis C Virus through Viral Adaptation

Expanding the Host Range of Hepatitis C Virus through Viral Adaptation

ABSTRACT Hepatitis C virus (HCV) species tropism is incompletely understood. We have previously shown that at the level of entry, human CD81 and occludin (OCLN) comprise the minimal set of human factors needed for viral uptake into murine cells. As an alternative approach to genetic humanization, sp...

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Autores principales: Markus von Schaewen, Marcus Dorner, Kathrin Hueging, Lander Foquet, Sherif Gerges, Gabriela Hrebikova, Brigitte Heller, Julia Bitzegeio, Juliane Doerrbecker, Joshua A. Horwitz, Gisa Gerold, Sebastian Suerbaum, Charles M. Rice, Philip Meuleman, Thomas Pietschmann, Alexander Ploss
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Publicado: American Society for Microbiology 2016
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Microbiology
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spelling oai:doaj.org-article:1244794fd1604668930279a7182f76002021-11-15T15:50:14ZExpanding the Host Range of Hepatitis C Virus through Viral Adaptation10.1128/mBio.01915-162150-7511https://doaj.org/article/1244794fd1604668930279a7182f76002016-12-01T00:00:00Zhttps://journals.asm.org/doi/10.1128/mBio.01915-16https://doaj.org/toc/2150-7511ABSTRACT Hepatitis C virus (HCV) species tropism is incompletely understood. We have previously shown that at the level of entry, human CD81 and occludin (OCLN) comprise the minimal set of human factors needed for viral uptake into murine cells. As an alternative approach to genetic humanization, species barriers can be overcome by adapting HCV to use the murine orthologues of these entry factors. We previously generated a murine tropic HCV (mtHCV or Jc1/mCD81) strain harboring three mutations within the viral envelope proteins that allowed productive entry into mouse cell lines. In this study, we aimed to characterize the ability of mtHCV to enter and infect mouse hepatocytes in vivo and in vitro. Using a highly sensitive, Cre-activatable reporter, we demonstrate that mtHCV can enter mouse hepatocytes in vivo in the absence of any human cofactors. Viral entry still relied on expression of mouse CD81 and SCARB1 and was more efficient when mouse CD81 and OCLN were overexpressed. HCV entry could be significantly reduced in the presence of anti-HCV E2 specific antibodies, suggesting that uptake of mtHCV is dependent on viral glycoproteins. Despite mtHCV’s ability to enter murine hepatocytes in vivo, we did not observe persistent infection, even in animals with severely blunted type I and III interferon signaling and impaired adaptive immune responses. Altogether, these results establish proof of concept that the barriers limiting HCV species tropism can be overcome by viral adaptation. However, additional viral adaptations will likely be needed to increase the robustness of a murine model system for hepatitis C. IMPORTANCE At least 150 million individuals are chronically infected with HCV and are at risk of developing serious liver disease. Despite the advent of effective antiviral therapy, the frequency of chronic carriers has only marginally decreased. A major roadblock in developing a vaccine that would prevent transmission is the scarcity of animal models that are susceptible to HCV infection. It is poorly understood why HCV infects only humans and chimpanzees. To develop an animal model for hepatitis C, previous efforts focused on modifying the host environment of mice, for example, to render them more susceptible to HCV infection. Here, we attempted a complementary approach in which a laboratory-derived HCV variant was tested for its ability to infect mice. We demonstrate that this engineered HCV strain can enter mouse liver cells but does not replicate efficiently. Thus, additional adaptations are likely needed to construct a robust animal model for HCV.Markus von SchaewenMarcus DornerKathrin HuegingLander FoquetSherif GergesGabriela HrebikovaBrigitte HellerJulia BitzegeioJuliane DoerrbeckerJoshua A. HorwitzGisa GeroldSebastian SuerbaumCharles M. RicePhilip MeulemanThomas PietschmannAlexander PlossAmerican Society for MicrobiologyarticleMicrobiologyQR1-502ENmBio, Vol 7, Iss 6 (2016)
institution DOAJ
collection DOAJ
language EN
topic Microbiology
QR1-502
spellingShingle Microbiology
QR1-502
Markus von Schaewen
Marcus Dorner
Kathrin Hueging
Lander Foquet
Sherif Gerges
Gabriela Hrebikova
Brigitte Heller
Julia Bitzegeio
Juliane Doerrbecker
Joshua A. Horwitz
Gisa Gerold
Sebastian Suerbaum
Charles M. Rice
Philip Meuleman
Thomas Pietschmann
Alexander Ploss
Expanding the Host Range of Hepatitis C Virus through Viral Adaptation
description ABSTRACT Hepatitis C virus (HCV) species tropism is incompletely understood. We have previously shown that at the level of entry, human CD81 and occludin (OCLN) comprise the minimal set of human factors needed for viral uptake into murine cells. As an alternative approach to genetic humanization, species barriers can be overcome by adapting HCV to use the murine orthologues of these entry factors. We previously generated a murine tropic HCV (mtHCV or Jc1/mCD81) strain harboring three mutations within the viral envelope proteins that allowed productive entry into mouse cell lines. In this study, we aimed to characterize the ability of mtHCV to enter and infect mouse hepatocytes in vivo and in vitro. Using a highly sensitive, Cre-activatable reporter, we demonstrate that mtHCV can enter mouse hepatocytes in vivo in the absence of any human cofactors. Viral entry still relied on expression of mouse CD81 and SCARB1 and was more efficient when mouse CD81 and OCLN were overexpressed. HCV entry could be significantly reduced in the presence of anti-HCV E2 specific antibodies, suggesting that uptake of mtHCV is dependent on viral glycoproteins. Despite mtHCV’s ability to enter murine hepatocytes in vivo, we did not observe persistent infection, even in animals with severely blunted type I and III interferon signaling and impaired adaptive immune responses. Altogether, these results establish proof of concept that the barriers limiting HCV species tropism can be overcome by viral adaptation. However, additional viral adaptations will likely be needed to increase the robustness of a murine model system for hepatitis C. IMPORTANCE At least 150 million individuals are chronically infected with HCV and are at risk of developing serious liver disease. Despite the advent of effective antiviral therapy, the frequency of chronic carriers has only marginally decreased. A major roadblock in developing a vaccine that would prevent transmission is the scarcity of animal models that are susceptible to HCV infection. It is poorly understood why HCV infects only humans and chimpanzees. To develop an animal model for hepatitis C, previous efforts focused on modifying the host environment of mice, for example, to render them more susceptible to HCV infection. Here, we attempted a complementary approach in which a laboratory-derived HCV variant was tested for its ability to infect mice. We demonstrate that this engineered HCV strain can enter mouse liver cells but does not replicate efficiently. Thus, additional adaptations are likely needed to construct a robust animal model for HCV.
format article
author Markus von Schaewen
Marcus Dorner
Kathrin Hueging
Lander Foquet
Sherif Gerges
Gabriela Hrebikova
Brigitte Heller
Julia Bitzegeio
Juliane Doerrbecker
Joshua A. Horwitz
Gisa Gerold
Sebastian Suerbaum
Charles M. Rice
Philip Meuleman
Thomas Pietschmann
Alexander Ploss
author_facet Markus von Schaewen
Marcus Dorner
Kathrin Hueging
Lander Foquet
Sherif Gerges
Gabriela Hrebikova
Brigitte Heller
Julia Bitzegeio
Juliane Doerrbecker
Joshua A. Horwitz
Gisa Gerold
Sebastian Suerbaum
Charles M. Rice
Philip Meuleman
Thomas Pietschmann
Alexander Ploss
author_sort Markus von Schaewen
title Expanding the Host Range of Hepatitis C Virus through Viral Adaptation
title_short Expanding the Host Range of Hepatitis C Virus through Viral Adaptation
title_full Expanding the Host Range of Hepatitis C Virus through Viral Adaptation
title_fullStr Expanding the Host Range of Hepatitis C Virus through Viral Adaptation
title_full_unstemmed Expanding the Host Range of Hepatitis C Virus through Viral Adaptation
title_sort expanding the host range of hepatitis c virus through viral adaptation
publisher American Society for Microbiology
publishDate 2016
url https://doaj.org/article/1244794fd1604668930279a7182f7600
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