Literature DB >> 28494867

Essential Roles of SATB1 in Specifying T Lymphocyte Subsets.

Kiyokazu Kakugawa1, Satoshi Kojo1, Hirokazu Tanaka1, Wooseok Seo1, Takaho A Endo2, Yohko Kitagawa3, Sawako Muroi1, Mari Tenno1, Nighat Yasmin1, Yoshinori Kohwi4, Shimon Sakaguchi2, Terumi Kowhi-Shigematsu4, Ichiro Taniuchi5.   

Abstract

T cell receptor (TCR) signaling by MHC class I and II induces thymocytes to acquire cytotoxic and helper fates via the induction of Runx3 and ThPOK transcription factors, respectively. The mechanisms by which TCR signaling is translated into transcriptional programs for each cell fate remain elusive. Here, we show that, in post-selection thymocytes, a genome organizer, SATB1, activates genes for lineage-specifying factors, including ThPOK, Runx3, CD4, CD8, and Treg factor Foxp3, via regulating enhancers in these genes in a locus-specific manner. Indeed, SATB1-deficient thymocytes are partially re-directed into inappropriate T lineages after both MHC class I- and II-mediated selection, and they fail to generate NKT and Treg subsets. Despite its essential role in activating enhancers for the gene encoding ThPOK in TCR-signaled thymocytes, SATB1 becomes dispensable for maintaining ThPOK in CD4+ T cells. Collectively, our findings demonstrate that SATB1 shapes the primary T cell pool by directing lineage-specific transcriptional programs in the thymus.
Copyright © 2017 The Author(s). Published by Elsevier Inc. All rights reserved.

Entities:  

Keywords:  SATB1; T lymphocyte development; gene regulation; genome organizer; lineage specification

Mesh:

Substances:

Year:  2017        PMID: 28494867     DOI: 10.1016/j.celrep.2017.04.038

Source DB:  PubMed          Journal:  Cell Rep            Impact factor:   9.423


  31 in total

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