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Literature DB >> 27717799

Reversed T Cell Receptor Docking on a Major Histocompatibility Class I Complex Limits Involvement in the Immune Response.

Stephanie Gras¹, Jesseka Chadderton², Claudia M Del Campo¹, Carine Farenc³, Florian Wiede³, Tracy M Josephs¹, Xavier Y X Sng², Michiko Mirams⁴, Katherine A Watson⁴, Tony Tiganis³, Kylie M Quinn², Jamie Rossjohn⁵, Nicole L La Gruta⁶.

Abstract

The anti-viral T cell response is drawn from the naive T cell repertoire. During influenza infection, the CD8+ T cell response to an H-2Db-restricted nucleoprotein epitope (NP366) is characterized by preferential expansion of T cells bearing TRBV13+ T cell receptors (TCRs) and avoidance of TRBV17+ T cells, despite the latter dominating the naive precursor repertoire. We found two TRBV17+ TCRs that bound H-2Db-NP366 with a 180° reversed polarity compared to the canonical TCR-pMHC-I docking. The TRBV17 β-chain dominated the interaction and, whereas the complementarity determining region-3 (CDR3) loops exclusively mediated contacts with the MHC-I, peptide specificity was attributable to germline-encoded recognition. Nevertheless, the TRBV17+ TCR exhibited moderate affinity toward H-2Db-NP366 and was capable of signal transduction. Thus, the naive CD8+ T cell pool can comprise TCRs adopting reversed pMHC-I docking modes that limit their involvement in the immune response.

Entities: Disease Gene

Keywords: T cell activation; T cell recruitment; TCR recognition of pMHCI; reversed TCR docking

Mesh：

Substances：

Year: 2016 PMID： 27717799 DOI： 10.1016/j.immuni.2016.09.007

Source DB: PubMed Journal: Immunity ISSN： 1074-7613 Impact factor: 31.745

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Cited

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