4.7 Article

Dynamic changes in E-protein activity regulate T reg cell development

Journal

JOURNAL OF EXPERIMENTAL MEDICINE
Volume 211, Issue 13, Pages 2651-2668

Publisher

ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20132681

Keywords

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Funding

  1. National Natural science Foundation of China [31270933]
  2. Ministry of Health of China [2013ZX10004608]
  3. Intramural Research Program of National Institute of Allergy and Infectious Diseases

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E-proteins are TCR-sensitive transcription factors essential for intrathymic T cell transitions. Here, we show that deletion of E-proteins leads to both enhanced peripheral TGF-beta-induced regulatory T (iT reg) cell and thymic naturally arising T reg cell (nT reg cell) differentiation. In contrast, deletion of Id proteins results in reduced nT reg cell differentiation. Mechanistic analysis indicated that decreased E-protein activity leads to de-repression of signaling pathways that are essential to Foxp3 expression. Decreased E-protein binding to an IL-2R alpha enhancer locus facilitated TCR-induced IL-2R alpha expression. Similarly, decreased E-protein activity facilitated TCR-induced NF-kappa B activation and generation of c-Rel. Consistent with this, microarray analysis indicated that cells with E-protein depletion that are not yet expressing Foxp3 exhibit activation of the IL-2 and NF-kappa B signaling pathways as well as enhanced expression of many of the genes associated with Foxp3 induction. Finally, studies using Nur77-GFP mice to monitor TCR signaling showed that TCR signaling strength sufficient to induce Foxp3 differentiation is accompanied by down-regulation of E-protein levels. Collectively, these data suggest that TCR stimulation acts in part through down-regulation of E-protein activity to induce T reg cell lineage development.

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