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Structural interplay between germline interactions and adaptive recognition determines the bandwidth of TCR-peptide-MHC cross-reactivity.

Nat. Immunol.. 2019-01; 
AdamsJarrett J,NarayananSamanthi,BirnbaumMichael E,SidhuSachdev S,BlevinsSydney J,GeeMarvin H,SibenerLeah V,BakerBrian M,KranzDavid M,GarciaK Christo
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Peptide Synthesis To produce a closer mimic of H-2Ld for display, we reverted the peptide-proximal substitutions back to wild-type (Ile66 and Trp97) to produce an m31r variant with three peptide-distal, TCR-distal substitutions and synthesized the mini-MHC m31r-CP with a tethered QL9 peptide (Genscript). Get A Quote

摘要

The T cell antigen receptor (TCR)-peptide-major histocompatibility complex (MHC) interface is composed of conserved and diverse regions, yet the relative contribution of each in shaping recognition by T cells remains unclear. Here we isolated cross-reactive peptides with limited homology, which allowed us to compare the structural properties of nine peptides for a single TCR-MHC pair. The TCR's cross-reactivity was rooted in highly similar recognition of an apical 'hot-spot' position in the peptide with tolerance of sequence variation at ancillary positions. Furthermore, we found a striking structural convergence onto a germline-mediated interaction between the TCR CDR1α region and the MHC α2 helix in t... More

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