Determination of amino acids on agretopes of pigeon cytochrome c‐related peptides specifically bound to I‐A allelic products

Abstract

In our prior study it was demonstrated that residues 46 and 54 on a synthetic peptide, AEGFSYTVANKNKGIT (50V), work as an agretope (site contacts with major histocompatibility complex molecules) and residues 50 and 52 function as an epitope (site contacts with T cell receptor), when tri-molecular complexes are formed among 50V, I-A^b and the T cell receptor. 50V was composed of residues 43 to 58 of pigeon cytochrome c (p43--58) except that the aspartic acid (D) at residue 50 was substituted by valine (V). Substitution of agretopic residues on 50V changed this I-A^b-binding peptide to an I-A^k-binding peptide, suggesting that positions 46 and 54 work as an agretope in I-A^k-restricted T cell responses. In the present study we examined whether residues 46 and 54 of 50V worked as agretopes in T cell responses restricted to other I-A haplotypes. The 50V-related peptides with phenylalanine (F) at position 46 and alanine (A) at position 54 bound tightly to I-A^b, I-A^d, I-A^q and I-A^s molecules and stimulated T cells most potently in mice bearing these I-A haplotypes. In contrast, 50V-related peptides carrying D at position 46 and A at position 54 bound most potently to I-A^k molecules, and the peptides with arginine (R) at position 46 and A at position 54 bound most efficiently to I-A^v molecules. The present findings, thus, demonstrate that the agretopic positions on the p43--58 related peptides are preserved in T cell responses restricted to each I-A haplotype studied, and that the specific amino acids on the agretopic positions exist a priori for each I-A allele-specific structure.