An HLA-B35-restricted epitope modified at an anchor residue results in an antagonist peptide

被引：44

作者：

Dong, T

Boyd, D

Rosenberg, W

Alp, N

Takiguchi, M

McMichael, A

RowlandJones, S

机构：

[1] JOHN RADCLIFFE HOSP,INST MOLEC MED,MOLEC IMMUNOL GRP,OXFORD OX3 9DU,ENGLAND

[2] JOHN RADCLIFFE HOSP,NUFFIELD DEPT MED,OXFORD OX3 9DU,ENGLAND

[3] UNIV TOKYO,INST MED SCI,DEPT TUMOR BIOL,TOKYO,JAPAN

来源：

EUROPEAN JOURNAL OF IMMUNOLOGY | 1996年 / 26卷 / 02期

关键词：

cytotoxic T lymphocyte; epitope; anchor residue; HLA-B35; antagonist peptide;

D O I：

10.1002/eji.1830260210

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Peptides associated with HLA-B35 commonly have a proline or occasionally a serine residue in the P2 anchor position of the peptide. with a tyrosine at the C terminus. Based on this motif, we identified an octamer epitope from influenza A matrix protein which is presented by HLA-B35. The requirements for MHC binding and T cell receptor contact have been analyzed using analogs of this peptide with substitutions at positions 1. 2. 4. 7 and 8. The natural epitope contains a serine residue at P2 of the peptide. Substitution of this residue with proline (the favored amino acid in this position in B35-associated peptides) considerably enhances binding to HLA-B35 in thc T2-B35 cell line, but the peptide is not recognized by the majority of CTL clones and can antagonize recognition of the index peptide. This suggests that a conservative substitution at the P2 anchor position results in a conformational change in the peptide-MHC surface exposed to the T cell receptor.

引用

页码：335 / 339

页数：5

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