Increased Cytotoxic T-Lymphocyte Epitope Variant Cross-Recognition and Functional Avidity Are Associated with Hepatitis C Virus Clearance

Daniel Yerly; David Heckerman; Todd M. Allen; John V. Chisholm III; Kellie Faircloth; Caitlyn H. Linde; Nicole Frahm; Joerg Timm; Werner J. Pichler; Andreas Cerny; Christian Brander

Increased Cytotoxic T-Lymphocyte Epitope Variant Cross-Recognition and Functional Avidity Are Associated with Hepatitis C Virus Clearance

Daniel Yerly ,
David Heckerman ,
Todd M. Allen ,
John V. Chisholm III ,
Kellie Faircloth ,
Caitlyn H. Linde ,
Nicole Frahm ,
Joerg Timm ,
Werner J. Pichler ,
Andreas Cerny ,
Christian Brander

Journal of Virology | October 2007 , Vol 82(6): pp. 3147-3153

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Hepatitis C virus (HCV) clearance has been associated with reduced viral evolution in targeted cytotoxic T-lymphocyte (CTL) epitopes, suggesting that HCV clearers may mount CTL responses with a superior ability to recognize epitope variants and prevent viral immune escape. Here, 40 HCV-infected subjects were tested with 406 10-mer peptides covering the vast majority of the sequence diversity spanning a 197-residue region of the NS3 protein. HCV clearers mounted significantly broader CTL responses of higher functional avidity and with wider variant cross-recognition capacity than nonclearers. These observations have important implications for vaccine approaches that may need to induce high-avidity responses in vivo.