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Immune-mediated effects targeting hepatitis C virus in a syngeneic replicon cell transplantation mouse model

Objective: HCV is characterised by its ability to establish chronic infection in hepatocytes and to replicate in the presence of an inflammation. We mimicked this situation in vivo in immune-competent mice by syngeneic transplantation of HCV replicon-containing mouse hepatoma cells. Design: A total...

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Bibliographic Details
Main Authors: Levander, Sepideh (Author) , Rupp, Daniel (Author) , Long, Gang (Author) , Bartenschlager, Ralf (Author)
Format: Article (Journal)
Language:English
Published: 2018
In: Gut
Year: 2017, Volume: 67, Issue: 8, Pages: 1525-1535
ISSN:1468-3288
DOI:10.1136/gutjnl-2016-313579
Online Access:Verlag, kostenfrei, Volltext: http://dx.doi.org/10.1136/gutjnl-2016-313579
Verlag, kostenfrei, Volltext: https://gut.bmj.com/content/67/8/1525
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Author Notes:Sepideh Levander, Fredrik Holmström, Lars Frelin, Gustaf Ahlén, Daniel Rupp, Gang Long, Ralf Bartenschlager, Matti Sällberg
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Summary:Objective: HCV is characterised by its ability to establish chronic infection in hepatocytes and to replicate in the presence of an inflammation. We mimicked this situation in vivo in immune-competent mice by syngeneic transplantation of HCV replicon-containing mouse hepatoma cells. Design: A total of 5 million H-2b positive Hep56.1D cells, carrying a subgenomic genotype (gt) 2a replicon (HCV replicon cells) or stably expressing comparable levels of the HCV NS3/4A protease/helicase complex (NS3/4A hepatoma cells), were injected subcutaneously into syngeneic H-2b-restricted mice. Kinetics of tumour growth, HCV RNA replication levels and HCV-specific immune responses were monitored. For immune monitoring, new H-2b-restricted cytotoxic T cell epitopes within the gt2a NS3/4A region were mapped. Immune mice were generated by DNA-based vaccination. Results: HCV replicon and NS3/4A hepatoma cells generated solid tumours in vivo. Similar to what is seen in human HCV infection did HCV RNA replicate in the presence of inflammation. NS3/4A-specific CD8+ T cells seemed to transiently reduce HCV RNA levels. Both CD4+ and CD8+ T cells were required for protection against tumour growth. Vaccine-induced NS3/4A(gt2a)-specific T cells protected against HCV replicon tumours in wild-type, but not in HCV NS3/4A(gt1a)-transgenic mice with dysfunctional HCV-specific T cells. Importantly, as in human HCV infection, HCV replicon cells neither primed nor boosted a strong NS3/4A-specific T cell response. Conclusion: Syngeneic transplantation of mouse HCV replicon cells into immune-competent animals mirrors many in vivo events in humans. This system is versatile and can be applied to any genetically modified H-2b-restricted mouse strain.
Item Description:First published June 23, 2017
Gesehen am 28.08.2018
Physical Description:Online Resource
ISSN:1468-3288
DOI:10.1136/gutjnl-2016-313579

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