Transduction of human T cells with a novel T-cell receptor confers anti-HCV reactivity

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Abstract

Hepatitis C Virus (HCV) is a major public health concern, with no effective vaccines currently available and 3% of the world's population being infected. Despite the existence of both B- and T-cell immunity in HCV-infected patients, chronic viral infection and HCV-related malignancies progress. Here we report the identification of a novel HCV TCR from an HLA-A2-restricted, HCV NS3:1073-1081-reactive CTL clone isolated from a patient with chronic HCV infection. We characterized this HCV TCR by expressing it in human T cells and analyzed the function of the resulting HCV TCR-transduced cells. Our results indicate that both the HCV TCR-transduced CD4+ and CD8+ T cells recognized the HCV NS3:1073-1081 peptide-loaded targets and HCV+ hepatocellular carcinoma cells (HCC) in a polyfunctional manner with cytokine (IFN-c, IL-2, and TNF-a) production as well as cytotoxicity. Tumor cell recognition by HCV TCR transduced CD82 Jurkat cells and CD4+ PBL-derived T cells indicated this TCR was CD8-independent, a property consistent with other high affinity TCRs. HCV TCR-transduced T cells may be promising for the treatment of patients with chronic HCV infections. © 2010 Zhang et al.

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Zhang, Y., Liu, Y., Moxley, K. M., Golden-Mason, L., Hughes, M. G., Liu, T., … Nishimura, M. I. (2010). Transduction of human T cells with a novel T-cell receptor confers anti-HCV reactivity. PLoS Pathogens, 6(7), 1–13. https://doi.org/10.1371/journal.ppat.1001018

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