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A naturally selected αβ T cell receptor binds HLA-DQ2 molecules without co-contacting the presented peptide

Nature Communications. 2025-04; 
Jia Jia Lim, Claerwen M. Jones, Tiing Jen Loh, Hien Thy Dao, Mai T. Tran, Jason A. Tye-Din, Nicole L. La Gruta & Jamie Rossjohn Monash University, Clayton
Products/Services Used Details Operation
Custom Vector Construction Selected P2A-linked TCRαβ gene constructs were custom ordered from Genscript and cloned into pMIGII (RRID: Addgene_52107; Get A Quote

摘要

αβ T cell receptors (TCR) co-recognise peptide (p) antigens that are presented by major histocompatibility complex (MHC) molecules. While marked variations in TCR-p-MHC docking topologies have been observed from structural studies, the co-recognition paradigm has held fast. Using HLA-DQ2.5-peptide tetramers, here we identify a TRAV12-1+-TRBV5-1+ G9 TCR from human peripheral blood that binds HLA-DQ2.5 in a peptide-agnostic manner. The crystal structures of TCR-HLA-DQ2.5-peptide complexes show that the G9 TCR binds HLA-DQ2.5 in a reversed docking topology without contacting the peptide, with the TCR contacting the β1 region of HLA-DQ2.5 and distal from the peptide antigen binding cleft. High-throughput screeni... More

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