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Timing and duration of MHC I positive selection signals are adjusted in the thymus to prevent lineage errors.


ABSTRACT: Major histocompatibility complex class I (MHC I) positive selection of CD8+ T cells in the thymus requires that T cell antigen receptor (TCR) signaling end in time for cytokines to induce Runx3d, the CD8-lineage transcription factor. We examined the time required for these events and found that the overall duration of positive selection was similar for all CD8+ thymocytes in mice, despite markedly different TCR signaling times. Notably, prolonged TCR signaling times were counter-balanced by accelerated Runx3d induction by cytokines and accelerated differentiation into CD8+ T cells. Consequently, lineage errors did not occur except when MHC I-TCR signaling was so prolonged that the CD4-lineage-specifying transcription factor ThPOK was expressed, preventing Runx3d induction. Thus, our results identify a compensatory signaling mechanism that prevents lineage-fate errors by dynamically modulating Runx3d induction rates during MHC I positive selection.

SUBMITTER: Kimura MY 

PROVIDER: S-EPMC6691722 | biostudies-literature | 2016 Dec

REPOSITORIES: biostudies-literature

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Timing and duration of MHC I positive selection signals are adjusted in the thymus to prevent lineage errors.

Kimura Motoko Y MY   Thomas Julien J   Tai Xuguang X   Guinter Terry I TI   Shinzawa Miho M   Etzensperger Ruth R   Li Zhenhu Z   Love Paul P   Nakayama Toshinori T   Singer Alfred A  

Nature immunology 20160926 12


Major histocompatibility complex class I (MHC I) positive selection of CD8<sup>+</sup> T cells in the thymus requires that T cell antigen receptor (TCR) signaling end in time for cytokines to induce Runx3d, the CD8-lineage transcription factor. We examined the time required for these events and found that the overall duration of positive selection was similar for all CD8<sup>+</sup> thymocytes in mice, despite markedly different TCR signaling times. Notably, prolonged TCR signaling times were co  ...[more]

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