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Cutting Edge: Dual TCR? Expression Poses an Autoimmune Hazard by Limiting Regulatory T Cell Generation.


ABSTRACT: Despite accounting for 10-30% of the T cell population in mice and humans, the role of dual TCR-expressing T cells in immunity remains poorly understood. It has been hypothesized that dual TCR T cells pose an autoimmune hazard by allowing self-reactive TCRs to escape thymic selection. We revisited this hypothesis using the NOD murine model of type 1 diabetes. We bred NOD mice hemizygous at both TCR? and ? (TCR?+/- ?+/-) loci, rendering them incapable of producing dual TCR T cells. We found that the lack of dual TCR? expression skewed the insulin-specific thymocyte population toward greater regulatory T (Treg) cell commitment, resulting in a more tolerogenic Treg to conventional T cell ratio and protection from diabetes. These data support a novel hypothesis by which dual TCR expression can promote autoimmunity by limiting agonist selection of self-reactive thymocytes into the Treg cell lineage.

SUBMITTER: Schuldt NJ 

PROVIDER: S-EPMC5501482 | biostudies-literature | 2017 Jul

REPOSITORIES: biostudies-literature

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Cutting Edge: Dual TCRα Expression Poses an Autoimmune Hazard by Limiting Regulatory T Cell Generation.

Schuldt Nathaniel J NJ   Auger Jennifer L JL   Spanier Justin A JA   Martinov Tijana T   Breed Elise R ER   Fife Brian T BT   Hogquist Kristin A KA   Binstadt Bryce A BA  

Journal of immunology (Baltimore, Md. : 1950) 20170524 1


Despite accounting for 10-30% of the T cell population in mice and humans, the role of dual TCR-expressing T cells in immunity remains poorly understood. It has been hypothesized that dual TCR T cells pose an autoimmune hazard by allowing self-reactive TCRs to escape thymic selection. We revisited this hypothesis using the NOD murine model of type 1 diabetes. We bred NOD mice hemizygous at both TCRα and β (TCRα<sup>+/-</sup> β<sup>+/-</sup>) loci, rendering them incapable of producing dual TCR T  ...[more]

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