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A TCRα framework–centered codon shapes a biased T cell repertoire through direct MHC and CDR3β interactions

Authors :
Elin Bergseng
Inger Sandlie
Knut E.A. Lundin
Lene Støkken Høydahl
Louise Fremgaard Risnes
M. Fleur du Pré
Shiva Dahal-Koirala
Ralf Stefan Neumann
Rahel Frick
Geir Åge Løset
Kristin Støen Gunnarsen
Bjørn Dalhus
Shuo-Wang Qiao
Terje Frigstad
Ludvig M. Sollid
Source :
JCI Insight. 2
Publication Year :
2017
Publisher :
American Society for Clinical Investigation, 2017.

Abstract

Selection of biased T cell receptor (TCR) repertoires across individuals is seen in both infectious diseases and autoimmunity, but the underlying molecular basis leading to these shared repertoires remains unclear. Celiac disease (CD) occurs primarily in HLA-DQ2.5+ individuals and is characterized by a CD4+ T cell response against gluten epitopes dominated by DQ2.5-glia-α1a and DQ2.5-glia-α2. The DQ2.5-glia-α2 response recruits a highly biased TCR repertoire composed of TRAV26-1 paired with TRBV7-2 harboring a semipublic CDR3β loop. We aimed to unravel the molecular basis for this signature. By variable gene segment exchange, directed mutagenesis, and cellular T cell activation studies, we found that TRBV7-3 can substitute for TRBV7-2, as both can contain the canonical CDR3β loop. Furthermore, we identified a pivotal germline-encoded MHC recognition motif centered on framework residue Y40 in TRAV26-1 engaging both DQB1*02 and the canonical CDR3β. This allowed prediction of expanded DQ2.5-glia-α2–reactive TCR repertoires, which were confirmed by single-cell sorting and TCR sequencing from CD patient samples. Our data refine our understanding of how HLA-dependent biased TCR repertoires are selected in the periphery due to germline-encoded residues. This research was originally published in JCI Insight. © 2018 American Society for Clinical Investigation

Details

ISSN :
23793708
Volume :
2
Database :
OpenAIRE
Journal :
JCI Insight
Accession number :
edsair.doi.dedup.....a795ac939ebcb3eee73f3887f1d468f5