Increased level of E protein activity during invariant NKT development promotes differentiation of invariant NKT2 and invariant NKT17 subsets

在恒定 NKT 发育过程中,E 蛋白活性水平的提高促进了恒定 NKT2 和恒定 NKT17 亚群的分化

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作者:Taishan Hu, Hongcheng Wang, Amie Simmons, Sandra Bajaña, Ying Zhao, Susan Kovats, Xiao-Hong Sun, Jose Alberola-Ila

Abstract

E protein transcription factors and their natural inhibitors, Id proteins, play critical and complex roles during lymphoid development. In this article, we report that partial maintenance of E protein activity during positive selection results in a change in the cell fate determination of developing iNKT cells, with a block in the development of iNKT1 cells and a parallel increase in the iNKT2 and iNKT17 subsets. Because the expression levels of the transcription factors that drive these alternative functional fates (GATA-3, RORγT, T-bet, and Runx-3) are not altered, our results suggest that E protein activity controls a novel checkpoint that regulates the number of iNKT precursors that choose each fate.

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