EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy

J Lupberger; MB Zeisel; F Xiao; C Thumann; I Fofana; L Zona; Christopher Davis; Christopher Mee; M Turek; S Gorke; C Royer; B Fischer; MN Zahid; D Lavillette; J Fresquet; FL Cosset; SM Rothenberg; T Pietschmann; AH Patel; P Pessaux; M Doffoel; W Raffelsberger; O Poch; Jane McKeating; L Brino; TF Baumert

doi:10.1038/nm.2341

EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy

J Lupberger, MB Zeisel, F Xiao, C Thumann, I Fofana, L Zona, Christopher Davis, Christopher Mee, M Turek, S Gorke, C Royer, B Fischer, MN Zahid, D Lavillette, J Fresquet, FL Cosset, SM Rothenberg, T Pietschmann, AH Patel, P PessauxM Doffoel, W Raffelsberger, O Poch, Jane McKeating, L Brino, TF Baumert

Immunology and Immunotherapy

Research output: Contribution to journal › Article

499 Citations (Scopus)

Abstract

Hepatitis C virus (HCV) is a major cause of liver disease, but therapeutic options are limited and there are no prevention strategies. Viral entry is the first step of infection and requires the cooperative interaction of several host cell factors. Using a functional RNAi kinase screen, we identified epidermal growth factor receptor and ephrin receptor A2 as host cofactors for HCV entry. Blocking receptor kinase activity by approved inhibitors broadly impaired infection by all major HCV genotypes and viral escape variants in cell culture and in a human liver chimeric mouse model in vivo. The identified receptor tyrosine kinases (RTKs) mediate HCV entry by regulating CD81-claudin-1 co-receptor associations and viral glycoprotein-dependent membrane fusion. These results identify RTKs as previously unknown HCV entry cofactors and show that tyrosine kinase inhibitors have substantial antiviral activity. Inhibition of RTK function may constitute a new approach for prevention and treatment of HCV infection.

Original language	English
Pages (from-to)	589-U109
Journal	Nature Medicine
Volume	17
Issue number	5
DOIs	https://doi.org/10.1038/nm.2341
Publication status	Published - 1 May 2011

UN SDGs

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

Access to Document

10.1038/nm.2341

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

Lupberger, J., Zeisel, MB., Xiao, F., Thumann, C., Fofana, I., Zona, L., Davis, C., Mee, C., Turek, M., Gorke, S., Royer, C., Fischer, B., Zahid, MN., Lavillette, D., Fresquet, J., Cosset, FL., Rothenberg, SM., Pietschmann, T., Patel, AH., ... Baumert, TF. (2011). EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy. Nature Medicine, 17(5), 589-U109. https://doi.org/10.1038/nm.2341

@article{03fcc67cef414dd4a646c6a8c0596cd4,

title = "EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy",

abstract = "Hepatitis C virus (HCV) is a major cause of liver disease, but therapeutic options are limited and there are no prevention strategies. Viral entry is the first step of infection and requires the cooperative interaction of several host cell factors. Using a functional RNAi kinase screen, we identified epidermal growth factor receptor and ephrin receptor A2 as host cofactors for HCV entry. Blocking receptor kinase activity by approved inhibitors broadly impaired infection by all major HCV genotypes and viral escape variants in cell culture and in a human liver chimeric mouse model in vivo. The identified receptor tyrosine kinases (RTKs) mediate HCV entry by regulating CD81-claudin-1 co-receptor associations and viral glycoprotein-dependent membrane fusion. These results identify RTKs as previously unknown HCV entry cofactors and show that tyrosine kinase inhibitors have substantial antiviral activity. Inhibition of RTK function may constitute a new approach for prevention and treatment of HCV infection.",

author = "J Lupberger and MB Zeisel and F Xiao and C Thumann and I Fofana and L Zona and Christopher Davis and Christopher Mee and M Turek and S Gorke and C Royer and B Fischer and MN Zahid and D Lavillette and J Fresquet and FL Cosset and SM Rothenberg and T Pietschmann and AH Patel and P Pessaux and M Doffoel and W Raffelsberger and O Poch and Jane McKeating and L Brino and TF Baumert",

year = "2011",

month = may,

day = "1",

doi = "10.1038/nm.2341",

language = "English",

volume = "17",

pages = "589--U109",

journal = "Nature Medicine",

issn = "1546-170X",

publisher = "Nature Publishing Group",

number = "5",

}

Lupberger, J, Zeisel, MB, Xiao, F, Thumann, C, Fofana, I, Zona, L, Davis, C, Mee, C, Turek, M, Gorke, S, Royer, C, Fischer, B, Zahid, MN, Lavillette, D, Fresquet, J, Cosset, FL, Rothenberg, SM, Pietschmann, T, Patel, AH, Pessaux, P, Doffoel, M, Raffelsberger, W, Poch, O, McKeating, J, Brino, L & Baumert, TF 2011, 'EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy', Nature Medicine, vol. 17, no. 5, pp. 589-U109. https://doi.org/10.1038/nm.2341

TY - JOUR

T1 - EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy

AU - Lupberger, J

AU - Zeisel, MB

AU - Xiao, F

AU - Thumann, C

AU - Fofana, I

AU - Zona, L

AU - Davis, Christopher

AU - Mee, Christopher

AU - Turek, M

AU - Gorke, S

AU - Royer, C

AU - Fischer, B

AU - Zahid, MN

AU - Lavillette, D

AU - Fresquet, J

AU - Cosset, FL

AU - Rothenberg, SM

AU - Pietschmann, T

AU - Patel, AH

AU - Pessaux, P

AU - Doffoel, M

AU - Raffelsberger, W

AU - Poch, O

AU - McKeating, Jane

AU - Brino, L

AU - Baumert, TF

PY - 2011/5/1

Y1 - 2011/5/1

N2 - Hepatitis C virus (HCV) is a major cause of liver disease, but therapeutic options are limited and there are no prevention strategies. Viral entry is the first step of infection and requires the cooperative interaction of several host cell factors. Using a functional RNAi kinase screen, we identified epidermal growth factor receptor and ephrin receptor A2 as host cofactors for HCV entry. Blocking receptor kinase activity by approved inhibitors broadly impaired infection by all major HCV genotypes and viral escape variants in cell culture and in a human liver chimeric mouse model in vivo. The identified receptor tyrosine kinases (RTKs) mediate HCV entry by regulating CD81-claudin-1 co-receptor associations and viral glycoprotein-dependent membrane fusion. These results identify RTKs as previously unknown HCV entry cofactors and show that tyrosine kinase inhibitors have substantial antiviral activity. Inhibition of RTK function may constitute a new approach for prevention and treatment of HCV infection.

AB - Hepatitis C virus (HCV) is a major cause of liver disease, but therapeutic options are limited and there are no prevention strategies. Viral entry is the first step of infection and requires the cooperative interaction of several host cell factors. Using a functional RNAi kinase screen, we identified epidermal growth factor receptor and ephrin receptor A2 as host cofactors for HCV entry. Blocking receptor kinase activity by approved inhibitors broadly impaired infection by all major HCV genotypes and viral escape variants in cell culture and in a human liver chimeric mouse model in vivo. The identified receptor tyrosine kinases (RTKs) mediate HCV entry by regulating CD81-claudin-1 co-receptor associations and viral glycoprotein-dependent membrane fusion. These results identify RTKs as previously unknown HCV entry cofactors and show that tyrosine kinase inhibitors have substantial antiviral activity. Inhibition of RTK function may constitute a new approach for prevention and treatment of HCV infection.

U2 - 10.1038/nm.2341

DO - 10.1038/nm.2341

M3 - Article

SN - 1546-170X

VL - 17

SP - 589-U109

JO - Nature Medicine

JF - Nature Medicine

IS - 5

ER -

EGFR and EphA2 are host factors for hepatitis C virus entry and possible targets for antiviral therapy

Abstract

UN SDGs

Access to Document

Fingerprint

Projects

Mechanisms of Hepatitis C Virus Induced Hepatocyte Injury

Cite this