AUTHOR=Erausquin Elena , Serra Pau , Parras Daniel , Santamaria Pere , López-Sagaseta Jacinto 

TITLE=Structural plasticity in I-Ag7 links autoreactivity to hybrid insulin peptides in type I diabetes

JOURNAL=Frontiers in Immunology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2022.924311

DOI=10.3389/fimmu.2022.924311

ISSN=1664-3224

ABSTRACT=<p>We recently provided evidence for promiscuous recognition of several different hybrid insulin peptides (HIPs) by the highly diabetogenic, I-A<sup>g7</sup>-restricted 4.1-T cell receptor (TCR). To understand the structural determinants of this phenomenon, we solved the structure of an agonistic HIP/I-A<sup>g7</sup> complex, both in isolation as well as bound to the 4.1-TCR. We find that HIP promiscuity of the 4.1-TCR is dictated, on the one hand, by an amino acid sequence pattern that ensures I-A<sup>g7</sup> binding and, on the other hand, by the presence of three acidic residues at positions P5, P7 and P8 that favor an optimal engagement by the 4.1-TCR’s complementary determining regions. Surprisingly, comparison of the TCR-bound and unbound HIP/I-A<sup>g7</sup> structures reveals that 4.1-TCR binding triggers several novel and unique structural motions in both the I-A<sup>g7</sup> molecule and the peptide that are essential for docking. This observation indicates that the type 1 diabetes-associated I-A<sup>g7</sup> molecule is structurally malleable and that this plasticity allows the recognition of multiple peptides by individual TCRs that would otherwise be unable to do so.</p>