CD8+ T cells from patients with cirrhosis display a phenotype that may contribute to cirrhosis-associated immune dysfunctionResearch in context

Fanny Lebossé; Cathrin Gudd; Enes Tunc; Arjuna Singanayagam; Rooshi Nathwani; Evangelos Triantafyllou; Oltin Pop; Naveenta Kumar; Sujit Mukherjee; Tie Zheng Hou; Alberto Quaglia; Fabien Zoulim; Julia Wendon; Ameet Dhar; Mark Thursz; Charalambos G. Antoniades; Wafa Khamri

EBioMedicine (Nov 2019)

CD8+ T cells from patients with cirrhosis display a phenotype that may contribute to cirrhosis-associated immune dysfunctionResearch in context

Fanny Lebossé,
Cathrin Gudd,
Enes Tunc,
Arjuna Singanayagam,
Rooshi Nathwani,
Evangelos Triantafyllou,
Oltin Pop,
Naveenta Kumar,
Sujit Mukherjee,
Tie Zheng Hou,
Alberto Quaglia,
Fabien Zoulim,
Julia Wendon,
Ameet Dhar,
Mark Thursz,
Charalambos G. Antoniades,
Wafa Khamri

Affiliations

Fanny Lebossé: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom; INSERM U1052- Cancer Research Centre of Lyon (CRCL), 69003 Lyon, France
Cathrin Gudd: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom
Enes Tunc: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom
Arjuna Singanayagam: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Rooshi Nathwani: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom
Evangelos Triantafyllou: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Oltin Pop: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Naveenta Kumar: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Sujit Mukherjee: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom
Tie Zheng Hou: Institute of Immunity and transplantation, University College London, United Kingdom
Alberto Quaglia: Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Fabien Zoulim: INSERM U1052- Cancer Research Centre of Lyon (CRCL), 69003 Lyon, France
Julia Wendon: Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Ameet Dhar: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom
Mark Thursz: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom
Charalambos G. Antoniades: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Institute of Liver Studies, King's College Hospital, King's College London, United Kingdom
Wafa Khamri: Division of Integrative Systems Medicine and Digestive Diseases, Department of Surgery and Cancer, St. Mary's Campus Imperial College London, London, United Kingdom; Corresponding author: Dr Wafa Khamri, Imperial College, Liver Immunology Laboratory, Division of Integrative Systems Medicine and Digestive Disease, Department of Surgery and Cancer, 10th Floor QEQM Wing, St Mary's Campus, South Warf Road, W2 1NY London, UK.

Journal volume & issue: Vol. 49
pp. 258 – 268

Abstract

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ABSTRACT: Background: Cirrhosis-associated immune dysfunction (CAID) contributes to high sepsis risk in patients with chronic liver disease. Various innate and; to a lesser extent; adaptive immune dysfunctions have been described as contributors to CAID leading to immune-paresis and impaired anti-microbial response in cirrhosis. In this study, we examined the phenotype of CD8+ T cells in chronic liver disease with the aim to evaluate changes that might contribute to impaired immune responses. Methods: Sixty patients with cirrhosis were prospectively recruited for this study. CD8+ T cells from peripheral blood, ascites and liver explants were characterized using flow cytometry and immunohistochemistry, respectively. The transcriptional signature of flow-sorted HLA-DR+CD8+ T cells was performed using Nanostring™ technology. HLA-DR+CD8+ T cells interactions with PBMCs and myeloid cells were tested in vitro. Findings: Peripheral CD8+ T cells from cirrhotic patients displayed an altered phenotype characterized by high HLA-DR and TIM-3 surface expression associated with concomitant infections and disease severity, respectively. Paired peritoneal CD8+ T cells expressed more pronounced levels of HLA-DR and PD-1 compared to peripheral CD8+ T cells. HLA-DR+CD8+ T cells were enriched in cirrhotic livers compared to controls. TIM-3, CTLA-4 and PD-1 levels were highly expressed on HLA-DR+CD8+ T cells and co-expression of HLA-DR and PD1 was higher in patients with poor disease outcomes. Genes involved in cytokines production and intracellular signalling pathways were strongly down-regulated in HLA-DR+CD8+ T cells. In comparison to their HLA-DR− counterparts, HLA-DR+CD8+ T cells promoted less proliferation of PBMCs and induced phenotypic and functional dysfunctions in monocytes and neutrophils in vitro. Interpretation: In patients with cirrhosis, CD8+ T cells display a phenotypic, functional and transcriptional profile which may contribute to CAID. Fund: This work was supported by Medical Research Council, the Rosetrees Charitable Trust, Robert Tournut 2016 grant (Sociéte Nationale Française de GastroEntérologie), Gilead® sciences, and NIHR Imperial Biomedical Research Centre. Keywords: Cirrhosis-associated immune dysfunction, CD8+ T cells, Chronic liver disease

Published in EBioMedicine

ISSN: 2352-3964 (Online)
Publisher: Elsevier
Country of publisher: Netherlands
LCC subjects: Medicine: Medicine (General)
Website: http://www.journals.elsevier.com/ebiomedicine/

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