Blockade of immunosuppressive cytokines restores NK cell antiviral function in chronic hepatitis B virus infection

NK cells are enriched in the liver, constituting around a third of intrahepatic lymphocytes. We have previously demonstrated that they upregulate the death ligand TRAIL in patients with chronic hepatitis B virus infection (CHB), allowing them to kill hepatocytes bearing TRAIL receptors. In this stud...

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Bibliographic Details
Published in:PLoS pathogens 2010-12, Vol.6 (12), p.e1001227-e1001227
Main Authors: Peppa, Dimitra, Micco, Lorenzo, Javaid, Alia, Kennedy, Patrick T F, Schurich, Anna, Dunn, Claire, Pallant, Celeste, Ellis, Gidon, Khanna, Pooja, Dusheiko, Geoffrey, Gilson, Richard J, Maini, Mala K
Format: Article
Language:English
Subjects:
Adult
Aged
Case-Control Studies
Cells
Cytokines
Cytokines - antagonists & inhibitors
Female
Gastroenterology and Hepatology/Gastrointestinal Infections
Hepatitis B
Hepatitis B, Chronic - immunology
Humans
Immune system
Immunology/Innate Immunity
Immunosuppression
Immunosuppressive Agents - antagonists & inhibitors
Infections
Infectious Diseases/Viral Infections
Interferon-gamma - biosynthesis
Interleukin-10 - analysis
Killer cells
Killer Cells, Natural - immunology
Killer Cells, Natural - virology
Ligands
Liver - immunology
Liver - virology
Male
Middle Aged
Physiological aspects
TNF-Related Apoptosis-Inducing Ligand - analysis
Virology/Host Antiviral Responses
Young Adult
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Summary:NK cells are enriched in the liver, constituting around a third of intrahepatic lymphocytes. We have previously demonstrated that they upregulate the death ligand TRAIL in patients with chronic hepatitis B virus infection (CHB), allowing them to kill hepatocytes bearing TRAIL receptors. In this study we investigated whether, in addition to their pathogenic role, NK cells have antiviral potential in CHB. We characterised NK cell subsets and effector function in 64 patients with CHB compared to 31 healthy controls. We found that, in contrast to their upregulated TRAIL expression and maintenance of cytolytic function, NK cells had a markedly impaired capacity to produce IFN-γ in CHB. This functional dichotomy of NK cells could be recapitulated in vitro by exposure to the immunosuppressive cytokine IL-10, which was induced in patients with active CHB. IL-10 selectively suppressed NK cell IFN-γ production without altering cytotoxicity or death ligand expression. Potent antiviral therapy reduced TRAIL-expressing CD56(bright) NK cells, consistent with the reduction in liver inflammation it induced; however, it was not able to normalise IL-10 levels or the capacity of NK cells to produce the antiviral cytokine IFN-γ. Blockade of IL-10 +/- TGF-β restored the capacity of NK cells from both the periphery and liver of patients with CHB to produce IFN-γ, thereby enhancing their non-cytolytic antiviral capacity. In conclusion, NK cells may be driven to a state of partial functional tolerance by the immunosuppressive cytokine environment in CHB. Their defective capacity to produce the antiviral cytokine IFN-γ persists in patients on antiviral therapy but can be corrected in vitro by IL-10+/- TGF-β blockade.
ISSN:1553-7374
1553-7366
1553-7374
DOI:10.1371/journal.ppat.1001227