SummaryMutations that abrogate recognition of a viral epitope by class I-restricted cytotoxic T lymphocyte (CTL) can lead to viral escape if the CTL response against that epitope is crucial for viral clearance. The likelihood of this type of event is low when the CTL response is simultaneously directed against multiple viral epitopes, as has been recently reported for patients with acute self-limited hepatitis B virus (HBV) infection. The CTL response to HBV is usually quite weak, however, during chronic HBV infection, and it is generally acknowledged that this is a major determinant of viral persistence in this disease. If such individuals were to produce a mono-or oligospecific CTL response, however, negative selection of the corresponding mutant viruses might occur. We have recently studied two HLAoA2-positive patients with chronic hepatitis B who, atypically, developed a strong HLA-A2-restricted CTL response against an epitope (FLPSDFFPSV) that contains an HLA-A2-binding motif located between residues 18-27 of the viral nucleocapsid protein, hepatitis B core antigen (HBcAg). These patients failed, however, to respond to any of other HLA-A2-restricted HBV-derived peptides that are generally immunogenic in acutely infected patients who successfully clear the virus. Interestingly, DNA sequence analysis of HBV isolates from these two patients demonstrated alternative residues at position 27 (V --~ A and V --~ I) and position 21 (S --~ N, S --~ A, and S -'~ V) that reduced the HLA and T cell receptorbinding capacities of the variant sequences, respectively. Synthetic peptides containing these alternative sequences were poorly immunogenic compared to the prototype HBc18-27 sequence, and they could not be recognized by CTL clones specific for the prototype peptide. While we do not know if the two patients were originally infected by these variant viruses or if the variants emerged subsequent to infection because of immune selection, the results are most consistent with the latter hypothesis. If this is correct, the data suggest that negative selection of mutant viral genomes might contribute to viral persistence in a subset of patients with chronic HBV infection who express a narrow repertoire of anti-HBV CTL responses.H LA class I-restricted, anti-viral cytotoxic T cells recognize short viral peptides that are generated by the intracellular processing of endogenously synthesized viral antigen within infected cells (1, 2), and are expressed at the cell surface in the binding groove of selected HLA class I molecules (3-7). Peptide binding to HLA class I molecules is dependent on interactions between conserved MHC residues and main chain atoms at both peptide termini (8-13), as well as selective interactions between allele-specific MHC pockets, formed by polymorphic MHC residues, and side chains of peptide anchor residues, pointing towards the floor of the HLA groove (14-17). Residues of the MHC bound peptide particularly accessible to TCR recognition are located in the central portion of the antigenic sequence that ...
