In chronic

In chronic this website hepatitis C (CHC) infection, the immune response is a key determinant to outcome of the antiviral therapy.

In this study we hypothesised that impaired T cell glucose metabolism occurs in HCV infection and will impact response to antiviral therapy. Methods: Longitudinal peripheral blood mononuclear cells (PBMCs) from patients with CHC (n = 21) were examined at baseline -prior to standard antiviral therapy and post-treatment, which includes 13 responders to treatment and 8 non-responders. As a control group, PBMCs from 10 healthy controls were also examined. PBMCs from subjects were stimulated with HCV peptides and CD3/CD28 Dynabeads for 44 hrs. Flow cytometry was used to measure specific metabolic markers such as pAkt (a key molecule in glucose transport and metabolism and a marker for T cell energy) and glucose transporter-1 as well as a marker of exhaustion (PD-1) in T-cell subpopulations (CD4/CD8/T selleck inhibitor reg/naive/central and effector memory

& terminally differentiated). As a measure of functionality, cytokine multiplex assays will be employed to detect TH-1 and TH-2 cytokines produced by PBMCs. Results: Compared to normal subjects, patients with CHC had impaired T cell MCE公司 (CD4 & CD8) glucose metabolism as assessed by pAkt and glucose uptake (p < 0.05). Clearance of HCV with antiviral therapy restored pAkt and glucose uptake to levels of healthy controls (p < 0.05). Active T cell populations (central and effector memory, terminally differentiated and T regulatory cells) in patients with CHC had significantly higher metabolic

activity (p < 0.05) as reflected by pAkt levels when compared to quiescent populations (naive cells). Compared to responders to antiviral therapy, non-responders had significantly reduced expression of pAkt (p < 0.05) in all CD8 T cell subpopulations. This significant reduction was found at both baseline and post-treatment time points. Low pAKT levels correlated with an exhausted T cell profile (increased PD-1) (p = 0.009, R2 = 0.52). Conclusions: The current study identifies for the first time a glucose metabolic defect (pAkt and glucose uptake) within T cells of patients with CHC when compared to healthy controls. This metabolic defect is found to recover after viral clearance, which could suggest a virus driven effect. Secondly, a decrease in metabolic activity is found in all T cell subpopulations in those who do not respond to treatment when compared to responders of treatment.

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