Longitudinal mapping of protective CD4+ T cell responses against HCV: Analysis of fluctuating dominant and subdominant HLA-DR11 restricted epitopes

G. C. Harcourt, M. Lucas, I. Sheridan, E. Barnes, R. Phillips, P. Klenerman

Research output: Contribution to journalArticlepeer-review

23 Citations (Scopus)

Abstract

Cellular immunity plays an important role in the control of persistent virus infections such as hepatitis C virus (HCV). Antiviral CD4+ T cell responses have been shown to accompany resolution of acute disease and there is also a consistent association between HLA Class II genes, notably HLADRB1*1101 (and the closely linked HLADQB1*0301) and disease resolution. We initially mapped longitudinal CD4+ T cell responses in an individual after spontaneous resolution of acute HCV, and identified three HLA-DR11-restricted responses which vary in immunodominance over time. Functional assays and HLA Class II tetramer staining revealed one to be a response to a commonly recognized epitope, NS31248-1261, although cytokine capture assays showed these specific cells to be at a very low frequency. In this patient, and in others reported, this most frequently recognized HLA-DR11 restricted epitope is not immunodominant. We analysed whether sequence variability within and between genotypes might account for differences in recognition of HLA-DR11 restricted epitopes. We found that a limited number, including NS31248-1261, showed extreme sequence conservation. Within NS3, the ability of peptides to accept amino acid substitutions was clearly related to the structure of the protein. Overall the data provide a deeper understanding of the relationship between protein structure and variability of HLA-DR11 restricted peptides and may explain the apparent dominance of responses to NS31248-1261 across studies but not within an individual immune response.

Original languageEnglish
Pages (from-to)324-331
Number of pages8
JournalJournal of Viral Hepatitis
Volume11
Issue number4
DOIs
Publication statusPublished - 1 Jul 2004
Externally publishedYes

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