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The checkpoint for agonist selection precedes conventional selection in human thymus.


ABSTRACT: The thymus plays a central role in self-tolerance, partly by eliminating precursors with a T cell receptor (TCR) that binds strongly to self-antigens. However, the generation of self-agonist-selected lineages also relies on strong TCR signaling. How thymocytes discriminate between these opposite outcomes remains elusive. Here, we identified a human agonist-selected PD-1+ CD8??+ subset of mature CD8??+ T cells that displays an effector phenotype associated with agonist selection. TCR stimulation of immature post-?-selection thymocyte blasts specifically gives rise to this innate subset and fixes early T cell receptor alpha variable (TRAV) and T cell receptor alpha joining (TRAJ) rearrangements in the TCR repertoire. These findings suggest that the checkpoint for agonist selection precedes conventional selection in the human thymus.

SUBMITTER: Verstichel G 

PROVIDER: S-EPMC5569900 | biostudies-literature | 2017 Feb

REPOSITORIES: biostudies-literature

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The thymus plays a central role in self-tolerance, partly by eliminating precursors with a T cell receptor (TCR) that binds strongly to self-antigens. However, the generation of self-agonist-selected lineages also relies on strong TCR signaling. How thymocytes discriminate between these opposite outcomes remains elusive. Here, we identified a human agonist-selected PD-1<sup>+</sup> CD8αα<sup>+</sup> subset of mature CD8αβ<sup>+</sup> T cells that displays an effector phenotype associated with ag  ...[more]

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