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Distinct phenotype and function of circulating Vδ1+ and Vδ2+ γδT-cells in acute and chronic hepatitis B. | LitMetric

AI Article Synopsis

  • Hepatitis B virus (HBV) infection leads to dysfunction in virus-specific T-cells, exhibiting different immune responses in chronic (CHB) and acute (AHB) cases compared to uninfected individuals.
  • A study involving diverse clinical cohorts showed that Vδ2+γδT-cells were more prevalent among Asian Americans and exhibited altered expression of immune markers based on infection status, but not in the frequency of γδT-cell populations across groups.
  • Effector functions of Vδ2+γδT-cells varied, indicating that their ability to respond to stimuli was weaker during AHB yet better preserved in CHB; these immune responses could also correlate with the severity of liver inflammation during hepatitis flares.

Article Abstract

Hepatitis B virus (HBV) persists with global and virus-specific T-cell dysfunction, without T-cell based correlates of outcomes. To determine if γδT-cells are altered in HBV infection relative to clinical status, we examined the frequency, phenotype and function of peripheral blood Vδ1+ and Vδ2+γδT-cells by multi-parameter cytometry in a clinically diverse North American cohort of chronic hepatitis B (CHB), acute hepatitis B (AHB) and uninfected control subjects. We show that circulating γδT-cells were comprised predominantly of CD3hiCD4- Vδ2+γδT-cells with frequencies that were 2-3 fold higher among Asian than non-Asian Americans and inversely correlated with age, but without differences between CHB, AHB and control subjects. However, compared to control subjects, CHB was associated with increased TbethiEomesdim phenotype in Vδ2+γδT-cells whereas AHB was associated with increased TbethiEomesdim phenotype in Vδ1+γδT-cells, with significant correlations between Tbet/Eomes expression in γδT-cells with their expression of NK and T-cell activation and regulatory markers. As for effector functions, IFNγ/TNF responses to phosphoantigens or PMA/Ionomycin in Vδ2+γδT-cells were weaker in AHB but preserved in CHB, without significant differences for Vδ1+γδT-cells. Furthermore, early IFNγ/TNF responses in Vδ2+ γδT-cells to brief PMA/Ionomycin stimulation correlated inversely with serum ALT but not HBV DNA. Accordingly, IFNγ/TNF responses in Vδ2+γδT-cells were weaker in patients with CHB with hepatitis flare compared to those without hepatitis flares, and this functional deficit persisted beyond clinical resolution of CHB flare. We conclude that circulating γδT-cells show distinct activation and differentiatiation in acute and chronic HBV infection as part of lymphoid stress surveillance with potential role in clinical outcomes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6490945PMC
http://dx.doi.org/10.1371/journal.ppat.1007715DOI Listing

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