Publication | Open Access
Increased Level of E Protein Activity during Invariant NKT Development Promotes Differentiation of Invariant NKT2 and Invariant NKT17 Subsets
27
Citations
42
References
2013
Year
Lymphocyte DevelopmentImmune RegulationInkt CellsCellular PhysiologyTranscriptional RegulationSignaling PathwayCell RegulationInvariant Nkt2Germ Cell DevelopmentCell SignalingGene ExpressionCell BiologyGene FunctionCell LineageDevelopmental BiologyImmune Cell DevelopmentE Protein ActivityInvariant Nkt17 SubsetsCell Fate DeterminationTranscription FactorsMedicineCell Development
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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