Publikation: Enolase represents a metabolic checkpoint controlling the differential exhaustion programmes of hepatitis virus-specific CD8+T cells
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Objective: Exhausted T cells with limited effector function are enriched in chronic hepatitis B and C virus (HBV and HCV) infection. Metabolic regulation contributes to exhaustion, but it remains unclear how metabolism relates to different exhaustion states, is impacted by antiviral therapy, and if metabolic checkpoints regulate dysfunction.
Design: Metabolic state, exhaustion and transcriptome of virus-specific CD8+ T cells from chronic HBV-infected (n=31) and HCV-infected patients (n=52) were determined ex vivo and during direct-acting antiviral (DAA) therapy. Metabolic flux and metabolic checkpoints were tested in vitro. Intrahepatic virus-specific CD8+ T cells were analysed by scRNA-Seq in a HBV-replicating murine in vivo model of acute and chronic infection.
Results: HBV-specific (core18-27, polymerase455-463) and HCV-specific (NS31073-1081, NS31406-1415, NS5B2594-2602) CD8+ T cell responses exhibit heterogeneous metabolic profiles connected to their exhaustion states. The metabolic state was connected to the exhaustion profile rather than the aetiology of infection. Mitochondrial impairment despite intact glucose uptake was prominent in severely exhausted T cells linked to elevated liver inflammation in chronic HCV infection and in HBV polymerase455-463 -specific CD8+ T cell responses. In contrast, relative metabolic fitness was observed in HBeAg-negative HBV infection in HBV core18-27-specific responses. DAA therapy partially improved mitochondrial programmes in severely exhausted HCV-specific T cells and enriched metabolically fit precursors. We identified enolase as a metabolic checkpoint in exhausted T cells. Metabolic bypassing improved glycolysis and T cell effector function. Similarly, enolase deficiency was observed in intrahepatic HBV-specific CD8+ T cells in a murine model of chronic infection.
Conclusion: Metabolism of HBV-specific and HCV-specific T cells is strongly connected to their exhaustion severity. Our results highlight enolase as metabolic regulator of severely exhausted T cells. They connect differential bioenergetic fitness with distinct exhaustion subtypes and varying liver disease, with implications for therapeutic strategies.
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WINKLER, Frances, Anna V. HIPP, Carlos RAMIREZ, Bianca MARTIN, Matteo VILLA, Emilia NEUWIRT, Oliver GORKA, Jeroen AERSSENS, Kathrin SCHUMANN, Bertram BENGSCH, 2023. Enolase represents a metabolic checkpoint controlling the differential exhaustion programmes of hepatitis virus-specific CD8+T cells. In: Gut (eGut). BMJ. 2023, 72(10), S. 1971-1984. ISSN 0017-5749. eISSN 1468-3288. Verfügbar unter: doi: 10.1136/gutjnl-2022-328734BibTex
@article{Winkler2023-10Enola-75101,
title={Enolase represents a metabolic checkpoint controlling the differential exhaustion programmes of hepatitis virus-specific CD8<sup>+</sup>T cells},
year={2023},
doi={10.1136/gutjnl-2022-328734},
number={10},
volume={72},
issn={0017-5749},
journal={Gut (eGut)},
pages={1971--1984},
author={Winkler, Frances and Hipp, Anna V. and Ramirez, Carlos and Martin, Bianca and Villa, Matteo and Neuwirt, Emilia and Gorka, Oliver and Aerssens, Jeroen and Schumann, Kathrin and Bengsch, Bertram}
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<dcterms:abstract>Objective: Exhausted T cells with limited effector function are enriched in chronic hepatitis B and C virus (HBV and HCV) infection. Metabolic regulation contributes to exhaustion, but it remains unclear how metabolism relates to different exhaustion states, is impacted by antiviral therapy, and if metabolic checkpoints regulate dysfunction.
Design: Metabolic state, exhaustion and transcriptome of virus-specific CD8<sup>+</sup> T cells from chronic HBV-infected (n=31) and HCV-infected patients (n=52) were determined ex vivo and during direct-acting antiviral (DAA) therapy. Metabolic flux and metabolic checkpoints were tested in vitro. Intrahepatic virus-specific CD8<sup>+</sup> T cells were analysed by scRNA-Seq in a HBV-replicating murine in vivo model of acute and chronic infection.
Results: HBV-specific (core<sub>18-27</sub>, polymerase<sub>455-463</sub>) and HCV-specific (NS3<sub>1073-1081</sub>, NS3<sub>1406-1415</sub>, NS5B<sub>2594-2602</sub>) CD8<sup>+</sup> T cell responses exhibit heterogeneous metabolic profiles connected to their exhaustion states. The metabolic state was connected to the exhaustion profile rather than the aetiology of infection. Mitochondrial impairment despite intact glucose uptake was prominent in severely exhausted T cells linked to elevated liver inflammation in chronic HCV infection and in HBV polymerase<sub>455-463</sub> -specific CD8<sup>+</sup> T cell responses. In contrast, relative metabolic fitness was observed in HBeAg-negative HBV infection in HBV core<sub>18-27</sub>-specific responses. DAA therapy partially improved mitochondrial programmes in severely exhausted HCV-specific T cells and enriched metabolically fit precursors. We identified enolase as a metabolic checkpoint in exhausted T cells. Metabolic bypassing improved glycolysis and T cell effector function. Similarly, enolase deficiency was observed in intrahepatic HBV-specific CD8<sup>+</sup> T cells in a murine model of chronic infection.
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