Autotaxin-lysophosphatidic acid receptor signalling regulates hepatitis C virus replication

Michelle J. Farquhar; Isla S. Humphreys; Simon A. Rudge; Garrick K. Wilson; Bishnupriya Bhattacharya; Maria Ciaccia; Ke Hu; Qifeng Zhang; Laurent Mailly; Gary M. Reynolds; Margaret Ashcroft; Peter Balfe; Thomas F. Baumert; Stephanie Roessler; Michael J.O. Wakelam; Jane A. McKeating

doi:10.1016/j.jhep.2017.01.009

Autotaxin-lysophosphatidic acid receptor signalling regulates hepatitis C virus replication

Michelle J. Farquhar, Isla S. Humphreys, Simon A. Rudge, Garrick K. Wilson, Bishnupriya Bhattacharya, Maria Ciaccia, Ke Hu, Qifeng Zhang, Laurent Mailly, Gary M. Reynolds, Margaret Ashcroft, Peter Balfe, Thomas F. Baumert, Stephanie Roessler, Michael J.O. Wakelam, Jane A. McKeating

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Abstract

Background & AimsChronic hepatitis C is a global health problem with an estimated 170 million hepatitis C virus (HCV) infected individuals at risk of progressive liver disease and hepatocellular carcinoma (HCC). Autotaxin (ATX, gene name: ENPP2) is a phospholipase with diverse roles in the physiological and pathological processes including inflammation and oncogenesis. Clinical studies have reported increased ATX expression in chronic hepatitis C, however, the pathways regulating ATX and its role in the viral life cycle are not well understood.
Methods: In vitro hepatocyte and ex vivo liver culture systems along with chimeric humanized liver mice and HCC tissue enabled us to assess the interplay between ATX and the HCV life cycle.
Results: HCV infection increased hepatocellular ATX RNA and protein expression. HCV infection stabilizes hypoxia inducible factors (HIFs) and we investigated a role for these transcription factors to regulate ATX. In vitro studies show that low oxygen increases hepatocellular ATX expression and transcriptome analysis showed a positive correlation between ATX mRNA levels and hypoxia gene score in HCC tumour tissue associated with HCV and other aetiologies. Importantly, inhibiting ATX-lysophosphatidic acid (LPA) signalling reduced HCV replication, demonstrating a positive role for this phospholipase in the viral life cycle. LPA activates phosphoinositide-3-kinase that stabilizes HIF-1α and inhibiting the HIF signalling pathway abrogates the pro-viral activity of LPA.
Conclusions: Our data support a model where HCV infection increases ATX expression which supports viral replication and HCC progression.
Lay summary: Chronic hepatitis C is a global health problem with infected individuals at risk of developing liver disease that can progress to hepatocellular carcinoma. Autotaxin generates the biologically active lipid lysophosphatidic acid that has been reported to play a tumorigenic role in a wide number of cancers. In this study we show that hepatitis C virus infection increases autotaxin expression via hypoxia inducible transcription factor and provides an environment in the liver that promotes fibrosis and liver injury. Importantly, we show a new role for lysophosphatidic acid in positively regulating hepatitis C virus replication.

Original language	English
Journal	Journal of Hepatology
Early online date	23 Jan 2017
DOIs	https://doi.org/10.1016/j.jhep.2017.01.009
Publication status	E-pub ahead of print - 23 Jan 2017

Keywords

Autotaxin
Lipid signalling
Hepatitis C virus
Hypoxia
Hypoxia-Inducible Factor 1
alpha subunit
Lysophosphatidic acid

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Farquhar_et_al_Autotaxin-lysophosphatidic_acid_Journal_of_Hepatology_20Accepted author manuscript, 1.48 MBLicence: Creative Commons: Attribution-NonCommercial-NoDerivs (CC BY-NC-ND)

http://www.sciencedirect.com/science/article/pii/S0168827817300132Licence: None: All rights reserved

The Role of Hepatitis C Virus Glycoprotein-Receptor Polymorphism in Viral Pathogenesis
McKeating, J.
Medical Research Council
1/01/12 → 30/06/17
Project: Research Councils
Mechanisms of Hepatitis C Virus Induced Hepatocyte Injury
McKeating, J. & Balfe, P.
Medical Research Council
1/10/09 → 30/09/12
Project: Research Councils

Cite this

Farquhar, M. J., Humphreys, I. S., Rudge, S. A., Wilson, G. K., Bhattacharya, B., Ciaccia, M., Hu, K., Zhang, Q., Mailly, L., Reynolds, G. M., Ashcroft, M., Balfe, P., Baumert, T. F., Roessler, S., Wakelam, M. J. O., & McKeating, J. A. (2017). Autotaxin-lysophosphatidic acid receptor signalling regulates hepatitis C virus replication. Journal of Hepatology. Advance online publication. https://doi.org/10.1016/j.jhep.2017.01.009

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title = "Autotaxin-lysophosphatidic acid receptor signalling regulates hepatitis C virus replication",

abstract = "Background & AimsChronic hepatitis C is a global health problem with an estimated 170 million hepatitis C virus (HCV) infected individuals at risk of progressive liver disease and hepatocellular carcinoma (HCC). Autotaxin (ATX, gene name: ENPP2) is a phospholipase with diverse roles in the physiological and pathological processes including inflammation and oncogenesis. Clinical studies have reported increased ATX expression in chronic hepatitis C, however, the pathways regulating ATX and its role in the viral life cycle are not well understood.Methods: In vitro hepatocyte and ex vivo liver culture systems along with chimeric humanized liver mice and HCC tissue enabled us to assess the interplay between ATX and the HCV life cycle.Results: HCV infection increased hepatocellular ATX RNA and protein expression. HCV infection stabilizes hypoxia inducible factors (HIFs) and we investigated a role for these transcription factors to regulate ATX. In vitro studies show that low oxygen increases hepatocellular ATX expression and transcriptome analysis showed a positive correlation between ATX mRNA levels and hypoxia gene score in HCC tumour tissue associated with HCV and other aetiologies. Importantly, inhibiting ATX-lysophosphatidic acid (LPA) signalling reduced HCV replication, demonstrating a positive role for this phospholipase in the viral life cycle. LPA activates phosphoinositide-3-kinase that stabilizes HIF-1α and inhibiting the HIF signalling pathway abrogates the pro-viral activity of LPA.Conclusions: Our data support a model where HCV infection increases ATX expression which supports viral replication and HCC progression.Lay summary: Chronic hepatitis C is a global health problem with infected individuals at risk of developing liver disease that can progress to hepatocellular carcinoma. Autotaxin generates the biologically active lipid lysophosphatidic acid that has been reported to play a tumorigenic role in a wide number of cancers. In this study we show that hepatitis C virus infection increases autotaxin expression via hypoxia inducible transcription factor and provides an environment in the liver that promotes fibrosis and liver injury. Importantly, we show a new role for lysophosphatidic acid in positively regulating hepatitis C virus replication.",

keywords = "Autotaxin , Lipid signalling , Hepatitis C virus , Hypoxia , Hypoxia-Inducible Factor 1 , alpha subunit , Lysophosphatidic acid",

author = "Farquhar, {Michelle J.} and Humphreys, {Isla S.} and Rudge, {Simon A.} and Wilson, {Garrick K.} and Bishnupriya Bhattacharya and Maria Ciaccia and Ke Hu and Qifeng Zhang and Laurent Mailly and Reynolds, {Gary M.} and Margaret Ashcroft and Peter Balfe and Baumert, {Thomas F.} and Stephanie Roessler and Wakelam, {Michael J.O.} and McKeating, {Jane A.}",

year = "2017",

month = jan,

day = "23",

doi = "10.1016/j.jhep.2017.01.009",

language = "English",

journal = "Journal of Hepatology",

issn = "0168-8278",

publisher = "Elsevier",

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TY - JOUR

T1 - Autotaxin-lysophosphatidic acid receptor signalling regulates hepatitis C virus replication

AU - Farquhar, Michelle J.

AU - Humphreys, Isla S.

AU - Rudge, Simon A.

AU - Wilson, Garrick K.

AU - Bhattacharya, Bishnupriya

AU - Ciaccia, Maria

AU - Hu, Ke

AU - Zhang, Qifeng

AU - Mailly, Laurent

AU - Reynolds, Gary M.

AU - Ashcroft, Margaret

AU - Balfe, Peter

AU - Baumert, Thomas F.

AU - Roessler, Stephanie

AU - Wakelam, Michael J.O.

AU - McKeating, Jane A.

PY - 2017/1/23

Y1 - 2017/1/23

N2 - Background & AimsChronic hepatitis C is a global health problem with an estimated 170 million hepatitis C virus (HCV) infected individuals at risk of progressive liver disease and hepatocellular carcinoma (HCC). Autotaxin (ATX, gene name: ENPP2) is a phospholipase with diverse roles in the physiological and pathological processes including inflammation and oncogenesis. Clinical studies have reported increased ATX expression in chronic hepatitis C, however, the pathways regulating ATX and its role in the viral life cycle are not well understood.Methods: In vitro hepatocyte and ex vivo liver culture systems along with chimeric humanized liver mice and HCC tissue enabled us to assess the interplay between ATX and the HCV life cycle.Results: HCV infection increased hepatocellular ATX RNA and protein expression. HCV infection stabilizes hypoxia inducible factors (HIFs) and we investigated a role for these transcription factors to regulate ATX. In vitro studies show that low oxygen increases hepatocellular ATX expression and transcriptome analysis showed a positive correlation between ATX mRNA levels and hypoxia gene score in HCC tumour tissue associated with HCV and other aetiologies. Importantly, inhibiting ATX-lysophosphatidic acid (LPA) signalling reduced HCV replication, demonstrating a positive role for this phospholipase in the viral life cycle. LPA activates phosphoinositide-3-kinase that stabilizes HIF-1α and inhibiting the HIF signalling pathway abrogates the pro-viral activity of LPA.Conclusions: Our data support a model where HCV infection increases ATX expression which supports viral replication and HCC progression.Lay summary: Chronic hepatitis C is a global health problem with infected individuals at risk of developing liver disease that can progress to hepatocellular carcinoma. Autotaxin generates the biologically active lipid lysophosphatidic acid that has been reported to play a tumorigenic role in a wide number of cancers. In this study we show that hepatitis C virus infection increases autotaxin expression via hypoxia inducible transcription factor and provides an environment in the liver that promotes fibrosis and liver injury. Importantly, we show a new role for lysophosphatidic acid in positively regulating hepatitis C virus replication.

AB - Background & AimsChronic hepatitis C is a global health problem with an estimated 170 million hepatitis C virus (HCV) infected individuals at risk of progressive liver disease and hepatocellular carcinoma (HCC). Autotaxin (ATX, gene name: ENPP2) is a phospholipase with diverse roles in the physiological and pathological processes including inflammation and oncogenesis. Clinical studies have reported increased ATX expression in chronic hepatitis C, however, the pathways regulating ATX and its role in the viral life cycle are not well understood.Methods: In vitro hepatocyte and ex vivo liver culture systems along with chimeric humanized liver mice and HCC tissue enabled us to assess the interplay between ATX and the HCV life cycle.Results: HCV infection increased hepatocellular ATX RNA and protein expression. HCV infection stabilizes hypoxia inducible factors (HIFs) and we investigated a role for these transcription factors to regulate ATX. In vitro studies show that low oxygen increases hepatocellular ATX expression and transcriptome analysis showed a positive correlation between ATX mRNA levels and hypoxia gene score in HCC tumour tissue associated with HCV and other aetiologies. Importantly, inhibiting ATX-lysophosphatidic acid (LPA) signalling reduced HCV replication, demonstrating a positive role for this phospholipase in the viral life cycle. LPA activates phosphoinositide-3-kinase that stabilizes HIF-1α and inhibiting the HIF signalling pathway abrogates the pro-viral activity of LPA.Conclusions: Our data support a model where HCV infection increases ATX expression which supports viral replication and HCC progression.Lay summary: Chronic hepatitis C is a global health problem with infected individuals at risk of developing liver disease that can progress to hepatocellular carcinoma. Autotaxin generates the biologically active lipid lysophosphatidic acid that has been reported to play a tumorigenic role in a wide number of cancers. In this study we show that hepatitis C virus infection increases autotaxin expression via hypoxia inducible transcription factor and provides an environment in the liver that promotes fibrosis and liver injury. Importantly, we show a new role for lysophosphatidic acid in positively regulating hepatitis C virus replication.

KW - Autotaxin

KW - Lipid signalling

KW - Hepatitis C virus

KW - Hypoxia

KW - Hypoxia-Inducible Factor 1

KW - alpha subunit

KW - Lysophosphatidic acid

U2 - 10.1016/j.jhep.2017.01.009

DO - 10.1016/j.jhep.2017.01.009

M3 - Article

SN - 0168-8278

JO - Journal of Hepatology

JF - Journal of Hepatology

ER -

Autotaxin-lysophosphatidic acid receptor signalling regulates hepatitis C virus replication

Abstract

Keywords

UN SDGs

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Projects

The Role of Hepatitis C Virus Glycoprotein-Receptor Polymorphism in Viral Pathogenesis

Mechanisms of Hepatitis C Virus Induced Hepatocyte Injury

Cite this