MHC class I H-2Kd-restricted antigenic peptides: additional constraints for the binding motif

Abstract

The previously defined binding motif of MHC class I H-2K^d-restricted antigenic peptides consists of a Y residue in position P2 and a hydrophobic residue with a large aliphatic side chain (L, I, or V) in position P9/P10 of optimal 9- or 10-mer peptides. We show now that the presence of a charged or a F residue in position P5 reduces the K^d-restricted competitor activity of several cytotoxic T lymphocyte (CTL) epitopes and model peptides, at a degree comparable to A substitutions for the P2 or the P9/P10 anchor residues. Various charged, polar, aromatic, and aliphatic amino acids were substituted for S256 in the CTL epitope Plasmodium berghel circumsporozoite (CS) 253–260 8-mer and in its CS 252–2609-mer form, whereas a more restricted panel of substitutions was tested in the CTL epitopes influenza nucleoprotein 147–155 9-mer and HLA-CW3 170–179 10-mer. Analysis of all the K^d-restricted epitopes so far defined also revealed an uncharged residue at this position. These additional structural constraints present in the K^d binding motif may thus improve the prediction of new epitopes recognized by T cells in the context of this MHC molecule.