Biological or pharmacological activation of protein kinase C alpha constrains hepatitis E virus replication

Wenshi Wang; Yijin Wang; Yannick Debing; Xinying Zhou; Yuebang Yin; Lei Xu; Elena Herrera Carrillo; Johannes H. Brandsma; Raymond A. Poot; Ben Berkhout; Johan Neyts; Maikel P. Peppelenbosch; Qiuwei Pan

doi:https://doi.org/10.1016/j.antiviral.2017.01.005

Biological or pharmacological activation of protein kinase C alpha constrains hepatitis E virus replication

Wenshi Wang, Yijin Wang, Yannick Debing, Xinying Zhou, Yuebang Yin, Lei Xu, Elena Herrera Carrillo, Johannes H. Brandsma, Raymond A. Poot, Ben Berkhout, Johan Neyts, Maikel P. Peppelenbosch, Qiuwei Pan

Research output: Contribution to journal › Article › Academic › peer-review

11 Citations (Scopus)

Abstract

Although hepatitis E has emerged as a global health issue, there is limited knowledge of its infection biology and no FDA-approved medication is available. Aiming to investigate the role of protein kinases in hepatitis E virus (HEV) infection and to identify potential antiviral targets, we screened a library of pharmacological kinase inhibitors in a cell culture model, a subgenomic HEV replicon containing luciferase reporter. We identified protein kinase C alpha (PKCα) as an essential cell host factor restricting HEV replication. Both specific inhibitor and shRNA-mediated knockdown of PKCα enhanced HEV replication. Conversely, over-expression of the activated form of PKCα or treatment with its pharmacological activator strongly inhibited HEV replication. Interestingly, upon the stimulation by its activator, PKCα efficiently activates its downstream Activator Protein 1 (AP-1) pathway, leading to the induction of antiviral interferon-stimulated genes (ISGs). This process is independent of the JAK-STAT machinery and interferon production. However, PKCα induced HEV inhibition appears independent of the AP1 cascade. The discovery that activated PKCα restricts HEV replication reveals new insight of HEV-host interactions and provides new target for antiviral drug development

Original language	English
Pages (from-to)	1-12
Journal	Antiviral Research
Volume	140
Early online date	2017
DOIs	https://doi.org/10.1016/j.antiviral.2017.01.005
Publication status	Published - 2017

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https://doi.org/10.1016/j.antiviral.2017.01.005

Cite this

@article{fc96c0c21d1d488dafed6379e13a403a,

title = "Biological or pharmacological activation of protein kinase C alpha constrains hepatitis E virus replication",

abstract = "Although hepatitis E has emerged as a global health issue, there is limited knowledge of its infection biology and no FDA-approved medication is available. Aiming to investigate the role of protein kinases in hepatitis E virus (HEV) infection and to identify potential antiviral targets, we screened a library of pharmacological kinase inhibitors in a cell culture model, a subgenomic HEV replicon containing luciferase reporter. We identified protein kinase C alpha (PKCα) as an essential cell host factor restricting HEV replication. Both specific inhibitor and shRNA-mediated knockdown of PKCα enhanced HEV replication. Conversely, over-expression of the activated form of PKCα or treatment with its pharmacological activator strongly inhibited HEV replication. Interestingly, upon the stimulation by its activator, PKCα efficiently activates its downstream Activator Protein 1 (AP-1) pathway, leading to the induction of antiviral interferon-stimulated genes (ISGs). This process is independent of the JAK-STAT machinery and interferon production. However, PKCα induced HEV inhibition appears independent of the AP1 cascade. The discovery that activated PKCα restricts HEV replication reveals new insight of HEV-host interactions and provides new target for antiviral drug development",

author = "Wenshi Wang and Yijin Wang and Yannick Debing and Xinying Zhou and Yuebang Yin and Lei Xu and {Herrera Carrillo}, Elena and Brandsma, {Johannes H.} and Poot, {Raymond A.} and Ben Berkhout and Johan Neyts and Peppelenbosch, {Maikel P.} and Qiuwei Pan",

year = "2017",

doi = "https://doi.org/10.1016/j.antiviral.2017.01.005",

language = "English",

volume = "140",

pages = "1--12",

journal = "Antiviral Research",

issn = "0166-3542",

publisher = "Elsevier",

}

TY - JOUR

T1 - Biological or pharmacological activation of protein kinase C alpha constrains hepatitis E virus replication

AU - Wang, Wenshi

AU - Wang, Yijin

AU - Debing, Yannick

AU - Zhou, Xinying

AU - Yin, Yuebang

AU - Xu, Lei

AU - Herrera Carrillo, Elena

AU - Brandsma, Johannes H.

AU - Poot, Raymond A.

AU - Berkhout, Ben

AU - Neyts, Johan

AU - Peppelenbosch, Maikel P.

AU - Pan, Qiuwei

PY - 2017

Y1 - 2017

N2 - Although hepatitis E has emerged as a global health issue, there is limited knowledge of its infection biology and no FDA-approved medication is available. Aiming to investigate the role of protein kinases in hepatitis E virus (HEV) infection and to identify potential antiviral targets, we screened a library of pharmacological kinase inhibitors in a cell culture model, a subgenomic HEV replicon containing luciferase reporter. We identified protein kinase C alpha (PKCα) as an essential cell host factor restricting HEV replication. Both specific inhibitor and shRNA-mediated knockdown of PKCα enhanced HEV replication. Conversely, over-expression of the activated form of PKCα or treatment with its pharmacological activator strongly inhibited HEV replication. Interestingly, upon the stimulation by its activator, PKCα efficiently activates its downstream Activator Protein 1 (AP-1) pathway, leading to the induction of antiviral interferon-stimulated genes (ISGs). This process is independent of the JAK-STAT machinery and interferon production. However, PKCα induced HEV inhibition appears independent of the AP1 cascade. The discovery that activated PKCα restricts HEV replication reveals new insight of HEV-host interactions and provides new target for antiviral drug development

AB - Although hepatitis E has emerged as a global health issue, there is limited knowledge of its infection biology and no FDA-approved medication is available. Aiming to investigate the role of protein kinases in hepatitis E virus (HEV) infection and to identify potential antiviral targets, we screened a library of pharmacological kinase inhibitors in a cell culture model, a subgenomic HEV replicon containing luciferase reporter. We identified protein kinase C alpha (PKCα) as an essential cell host factor restricting HEV replication. Both specific inhibitor and shRNA-mediated knockdown of PKCα enhanced HEV replication. Conversely, over-expression of the activated form of PKCα or treatment with its pharmacological activator strongly inhibited HEV replication. Interestingly, upon the stimulation by its activator, PKCα efficiently activates its downstream Activator Protein 1 (AP-1) pathway, leading to the induction of antiviral interferon-stimulated genes (ISGs). This process is independent of the JAK-STAT machinery and interferon production. However, PKCα induced HEV inhibition appears independent of the AP1 cascade. The discovery that activated PKCα restricts HEV replication reveals new insight of HEV-host interactions and provides new target for antiviral drug development

U2 - https://doi.org/10.1016/j.antiviral.2017.01.005

DO - https://doi.org/10.1016/j.antiviral.2017.01.005

M3 - Article

C2 - 28077314

SN - 0166-3542

VL - 140

SP - 1

EP - 12

JO - Antiviral Research

JF - Antiviral Research

ER -