A single amino acid substitution in the Ak molecule fortuitously provokes an alloresponse

Abstract

We discovered by chance that the R28 T cell hybridoma has dual specificity. It responds to a peptide derived from ribonuclease presented by cells displaying A^k molecules and it reacts, in the absence of added antigen, to cells expressing A^k complexes with a single amino acid substitution at position 69 of the α chain. Modelling and functional studies suggest that residue 69 is a peptide contact residue, prompting the hypothesis that R28′s alloreactivity is a cross-reactive response to an unknown peptide bound in the ‘groove’ of the mutant A^k complex. In this report, we employ a competition assay to confirm that this alloresponse involves a groove-binding peptide, demonstrate that this peptide derives from or depends on fetal calf serum and exploit a panel of antigen-presenting cell lines – each displaying an A^k complex with a different position 69 substitution – to establish that the alloresponse is not just a heteroclitic response to ribonuclease, itself. We speculate that much of the alloreactivity against murine class II molecules that is revealed in vitro may prove to be directed at bovine serum-derived peptides, suggesting that in this context, alloreactivity is a misnomer.