期刊
GUT
卷 64, 期 3, 页码 469-482出版社
BMJ PUBLISHING GROUP
DOI: 10.1136/gutjnl-2014-306767
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资金
- International Research Training Group 1273 - German Research Foundation (DFG)
- Federal Ministry of Education and Research (BMBF) [01Kl0788]
- Deutsches Zentrum fur Infektionsforschung
- Swedish Research Council
- Swedish Cancer Society
- Karolinska Institutet
- Swedish Society for Medical Research
- Stockholm County Council
- Alex and Eva Wallstrom Foundation
- Swedish Society of Medicine
- Jeansson Foundation
- Bengt Ihre Foundation
- Groschinsky Foundation
- Hedlunds Foundation
- Mag-tarmfonden
- Julin Foundation
- Novo Nordisk Fonden [NNF14OC0009347] Funding Source: researchfish
Objective Although hepatitis delta is considered an immune-mediated disease, adaptive immune responses to hepatitis delta virus (HDV) are hardly detectable. Thus, the role of other immune responses, including those mediated by natural killer (NK) cells, must be considered in HDV pathogenesis and in treatments with immune-stimulating agents such as interferon (IFN)alpha. However, the phenotype and function of NK cells in chronic HDV infection, or in HDV-infected individuals undergoing IFN alpha treatment, have not been extensively studied. Design We performed an extensive analysis of NK cells in chronically HDV-infected patients before and during treatment with IFN alpha, and compared the results with those for patients with HBV mono-infection as well as healthy controls. Results In untreated HDV-infected patients, a higher than normal frequency of NK cells was observed in peripheral blood with unaltered phenotypic NK cell differentiation status. In contrast, long-term IFN alpha treatment of HDV-infected patients caused a significant change in NK cell differentiation status, with selective loss of terminally differentiated NK cells and, in parallel, a relative enrichment in immature NK cell subsets. Treatment was associated with marked functional impairment of the NK cells, which was independent of the changes in NK cell differentiation status. Furthermore, treatment polarised NK cell IFN signalling from STAT4 towards STAT1 dependency. Strikingly, a high frequency of CD56(dim) NK cells at baseline was positively associated with IFN alpha treatment outcome in the patients. Conclusions We describe in detail how HDV infection, and IFN alpha treatment of this infection, affects the NK cell compartment and what consequences this has for the functional capacity of NK cells.
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