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Hepatitis B Virus--Specific and Global T-Cell Dysfunction in Chronic Hepatitis B. | LitMetric

AI Article Synopsis

  • The study investigates the roles of T cells in chronic hepatitis B (CHB) and aims to correlate T-cell responses with clinical stages of the disease in a group of 200 CHB patients and 20 healthy controls.
  • Patients with CHB showed weak T-cell responses, with a notable increase in regulatory T cells and expression of inhibitory markers, suggesting immune dysfunction.
  • Although specific T-cell responses to the hepatitis B virus (HBV) were weaker in HBeAg-positive patients, the overall T-cell dysfunction did not clearly differentiate between the clinical stages of CHB.

Article Abstract

Background & Aims: T cells play a critical role in viral infection. We examined whether T-cell effector and regulatory responses can define clinical stages of chronic hepatitis B (CHB).

Methods: We enrolled 200 adults with CHB who participated in the National Institutes of Health-supported Hepatitis B Research Network from 2011 through 2013 and 20 uninfected individuals (controls). Peripheral blood lymphocytes from these subjects were analyzed for T-cell responses (proliferation and production of interferon gamma and interleukin 10) to overlapping hepatitis B virus (HBV) peptides (preS, S, preC, core, and reverse transcriptase), influenza matrix peptides, and lipopolysaccharide. T-cell expression of regulatory markers FOXP3, programmed death-1, and cytotoxic T lymphocyte-associated antigen-4 was examined by flow cytometry. Immune measures were compared with clinical parameters, including physician-defined immune-active, immune-tolerant, or inactive CHB phenotypes, in a blinded fashion.

Results: Compared with controls, patients with CHB had weak T-cell proliferative, interferon gamma, and interleukin 10 responses to HBV, with increased frequency of circulating FOXP3(+)CD127(-) regulatory T cells and CD4(+) T-cell expression of programmed death-1 and cytotoxic T lymphocyte-associated antigen-4. T-cell measures did not clearly distinguish between clinical CHB phenotypes, although the HBV core-specific T-cell response was weaker in hepatitis B e antigen (HBeAg)(+) than HBeAg(-) patients (percent responders: 3% vs 23%; P = .00008). Although in vitro blockade of programmed death-1 or cytotoxic T lymphocyte-associated antigen-4 increased T-cell responses to HBV, the effect was weaker in HBeAg(+) than HBeAg(-) patients. Furthermore, T-cell responses to influenza and lipopolysaccharide were weaker in CHB patients than controls.

Conclusions: HBV persists with virus-specific and global T-cell dysfunction mediated by multiple regulatory mechanisms, including circulating HBeAg, but without distinct T-cell-based immune signatures for clinical phenotypes. These findings suggest additional T-cell-independent or regulatory mechanisms of CHB pathogenesis that warrant further investigation.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4766024PMC
http://dx.doi.org/10.1053/j.gastro.2015.11.050DOI Listing

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