Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation

Anggakusuma; Inés Romero-Brey; Carola Berger; Che C. Colpitts; Tujana Boldanova; Michael Engelmann; Daniel Todt; Paula Monteiro Perin; Patrick Behrendt; Florian W.R. Vondran; Shuting Xu; Christine Goffinet; Luis M. Schang; Markus H. Heim; Ralf Bartenschlager; Thomas Pietschmann; Eike Steinmann

doi:10.1002/hep.27913

Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation

Anggakusuma, Inés Romero-Brey, Carola Berger, Che C. Colpitts, Tujana Boldanova, Michael Engelmann, Daniel Todt, Paula Monteiro Perin, Patrick Behrendt, Florian W.R. Vondran, Shuting Xu, Christine Goffinet, Luis M. Schang, Markus H. Heim, Ralf Bartenschlager, Thomas Pietschmann, Eike Steinmann

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Abstract

Hepatitis C virus (HCV) is a positive-strand RNA virus that primarily infects human hepatocytes. Infections with HCV constitute a global health problem, with 180 million people currently chronically infected. Recent studies have reported that cholesterol 25-hydroxylase (CH25H) is expressed as an interferon-stimulated gene and mediates antiviral activities against different enveloped viruses through the production of 25-hydroxycholesterol (25HC). However, the intrinsic regulation of human CH25H (hCH25H) expression within the liver as well as its mechanistic effects on HCV infectivity remain elusive. In this study, we characterized the expression of hCH25H using liver biopsies and primary human hepatocytes. In addition, the antiviral properties of this protein and its enzymatic product, 25HC, were further characterized against HCV in tissue culture. Levels of hCH25H messenger RNA were significantly up-regulated both in HCV-positive liver biopsies and in HCV-infected primary human hepatocytes. The expression of hCH25H in primary human hepatocytes was primarily and transiently induced by type I interferon. Transient expression of hCH25H in human hepatoma cells restricted HCV infection in a genotype-independent manner. This inhibition required the enzymatic activity of CH25H. We observed an inhibition of viral membrane fusion during the entry process by 25HC, which was not due to a virucidal effect. Yet the primary effect by 25HC on HCV was at the level of RNA replication, which was observed using subgenomic replicons of two different genotypes. Further analysis using electron microscopy revealed that 25HC inhibited formation of the membranous web, the HCV replication factory, independent of RNA replication. Conclusion: Infection with HCV causes up-regulation of interferon-inducible CH25H in vivo, and its product, 25HC, restricts HCV primarily at the level of RNA replication by preventing formation of the viral replication factory.

Original language	English
Pages (from-to)	702-714
Number of pages	13
Journal	Hepatology
Volume	62
Issue number	3
DOIs	https://doi.org/10.1002/hep.27913
Publication status	Published - 1 Sept 2015
Externally published	Yes

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Anggakusuma, Romero-Brey, I., Berger, C., Colpitts, C. C., Boldanova, T., Engelmann, M., Todt, D., Perin, P. M., Behrendt, P., Vondran, F. W. R., Xu, S., Goffinet, C., Schang, L. M., Heim, M. H., Bartenschlager, R., Pietschmann, T., & Steinmann, E. (2015). Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation. Hepatology, 62(3), 702-714. https://doi.org/10.1002/hep.27913

@article{b4a61c05c2ff4c46ad4ed13d132482a9,

title = "Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation",

abstract = "Hepatitis C virus (HCV) is a positive-strand RNA virus that primarily infects human hepatocytes. Infections with HCV constitute a global health problem, with 180 million people currently chronically infected. Recent studies have reported that cholesterol 25-hydroxylase (CH25H) is expressed as an interferon-stimulated gene and mediates antiviral activities against different enveloped viruses through the production of 25-hydroxycholesterol (25HC). However, the intrinsic regulation of human CH25H (hCH25H) expression within the liver as well as its mechanistic effects on HCV infectivity remain elusive. In this study, we characterized the expression of hCH25H using liver biopsies and primary human hepatocytes. In addition, the antiviral properties of this protein and its enzymatic product, 25HC, were further characterized against HCV in tissue culture. Levels of hCH25H messenger RNA were significantly up-regulated both in HCV-positive liver biopsies and in HCV-infected primary human hepatocytes. The expression of hCH25H in primary human hepatocytes was primarily and transiently induced by type I interferon. Transient expression of hCH25H in human hepatoma cells restricted HCV infection in a genotype-independent manner. This inhibition required the enzymatic activity of CH25H. We observed an inhibition of viral membrane fusion during the entry process by 25HC, which was not due to a virucidal effect. Yet the primary effect by 25HC on HCV was at the level of RNA replication, which was observed using subgenomic replicons of two different genotypes. Further analysis using electron microscopy revealed that 25HC inhibited formation of the membranous web, the HCV replication factory, independent of RNA replication. Conclusion: Infection with HCV causes up-regulation of interferon-inducible CH25H in vivo, and its product, 25HC, restricts HCV primarily at the level of RNA replication by preventing formation of the viral replication factory.",

author = "Anggakusuma and In{\'e}s Romero-Brey and Carola Berger and Colpitts, \{Che C.\} and Tujana Boldanova and Michael Engelmann and Daniel Todt and Perin, \{Paula Monteiro\} and Patrick Behrendt and Vondran, \{Florian W.R.\} and Shuting Xu and Christine Goffinet and Schang, \{Luis M.\} and Heim, \{Markus H.\} and Ralf Bartenschlager and Thomas Pietschmann and Eike Steinmann",

year = "2015",

month = sep,

day = "1",

doi = "10.1002/hep.27913",

language = "English",

volume = "62",

pages = "702--714",

journal = "Hepatology",

issn = "0270-9139",

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Anggakusuma, Romero-Brey, I, Berger, C, Colpitts, CC, Boldanova, T, Engelmann, M, Todt, D, Perin, PM, Behrendt, P, Vondran, FWR, Xu, S, Goffinet, C, Schang, LM, Heim, MH, Bartenschlager, R, Pietschmann, T & Steinmann, E 2015, 'Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation', Hepatology, vol. 62, no. 3, pp. 702-714. https://doi.org/10.1002/hep.27913

TY - JOUR

T1 - Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation

AU - Anggakusuma, null

AU - Romero-Brey, Inés

AU - Berger, Carola

AU - Colpitts, Che C.

AU - Boldanova, Tujana

AU - Engelmann, Michael

AU - Todt, Daniel

AU - Perin, Paula Monteiro

AU - Behrendt, Patrick

AU - Vondran, Florian W.R.

AU - Xu, Shuting

AU - Goffinet, Christine

AU - Schang, Luis M.

AU - Heim, Markus H.

AU - Bartenschlager, Ralf

AU - Pietschmann, Thomas

AU - Steinmann, Eike

PY - 2015/9/1

Y1 - 2015/9/1

N2 - Hepatitis C virus (HCV) is a positive-strand RNA virus that primarily infects human hepatocytes. Infections with HCV constitute a global health problem, with 180 million people currently chronically infected. Recent studies have reported that cholesterol 25-hydroxylase (CH25H) is expressed as an interferon-stimulated gene and mediates antiviral activities against different enveloped viruses through the production of 25-hydroxycholesterol (25HC). However, the intrinsic regulation of human CH25H (hCH25H) expression within the liver as well as its mechanistic effects on HCV infectivity remain elusive. In this study, we characterized the expression of hCH25H using liver biopsies and primary human hepatocytes. In addition, the antiviral properties of this protein and its enzymatic product, 25HC, were further characterized against HCV in tissue culture. Levels of hCH25H messenger RNA were significantly up-regulated both in HCV-positive liver biopsies and in HCV-infected primary human hepatocytes. The expression of hCH25H in primary human hepatocytes was primarily and transiently induced by type I interferon. Transient expression of hCH25H in human hepatoma cells restricted HCV infection in a genotype-independent manner. This inhibition required the enzymatic activity of CH25H. We observed an inhibition of viral membrane fusion during the entry process by 25HC, which was not due to a virucidal effect. Yet the primary effect by 25HC on HCV was at the level of RNA replication, which was observed using subgenomic replicons of two different genotypes. Further analysis using electron microscopy revealed that 25HC inhibited formation of the membranous web, the HCV replication factory, independent of RNA replication. Conclusion: Infection with HCV causes up-regulation of interferon-inducible CH25H in vivo, and its product, 25HC, restricts HCV primarily at the level of RNA replication by preventing formation of the viral replication factory.

AB - Hepatitis C virus (HCV) is a positive-strand RNA virus that primarily infects human hepatocytes. Infections with HCV constitute a global health problem, with 180 million people currently chronically infected. Recent studies have reported that cholesterol 25-hydroxylase (CH25H) is expressed as an interferon-stimulated gene and mediates antiviral activities against different enveloped viruses through the production of 25-hydroxycholesterol (25HC). However, the intrinsic regulation of human CH25H (hCH25H) expression within the liver as well as its mechanistic effects on HCV infectivity remain elusive. In this study, we characterized the expression of hCH25H using liver biopsies and primary human hepatocytes. In addition, the antiviral properties of this protein and its enzymatic product, 25HC, were further characterized against HCV in tissue culture. Levels of hCH25H messenger RNA were significantly up-regulated both in HCV-positive liver biopsies and in HCV-infected primary human hepatocytes. The expression of hCH25H in primary human hepatocytes was primarily and transiently induced by type I interferon. Transient expression of hCH25H in human hepatoma cells restricted HCV infection in a genotype-independent manner. This inhibition required the enzymatic activity of CH25H. We observed an inhibition of viral membrane fusion during the entry process by 25HC, which was not due to a virucidal effect. Yet the primary effect by 25HC on HCV was at the level of RNA replication, which was observed using subgenomic replicons of two different genotypes. Further analysis using electron microscopy revealed that 25HC inhibited formation of the membranous web, the HCV replication factory, independent of RNA replication. Conclusion: Infection with HCV causes up-regulation of interferon-inducible CH25H in vivo, and its product, 25HC, restricts HCV primarily at the level of RNA replication by preventing formation of the viral replication factory.

U2 - 10.1002/hep.27913

DO - 10.1002/hep.27913

M3 - Article

SN - 0270-9139

VL - 62

SP - 702

EP - 714

JO - Hepatology

JF - Hepatology

IS - 3

ER -

Interferon-inducible cholesterol-25-hydroxylase restricts hepatitis C virus replication through blockage of membranous web formation

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