| Literature DB >> 23287858 |
Marcos E García-Ojeda1, Roel G J Klein Wolterink, Fabrice Lemaître, Odile Richard-Le Goff, Milena Hasan, Rudolf W Hendriks, Ana Cumano, James P Di Santo.
Abstract
Transcription factors orchestrate T-lineage differentiation in the thymus. One critical checkpoint involves Notch1 signaling that instructs T-cell commitment at the expense of the B-lineage program. While GATA-3 is required for T-cell specification, its mechanism of action is poorly understood. We show that GATA-3 works in concert with Notch1 to commit thymic progenitors to the T-cell lineage via 2 distinct pathways. First, GATA-3 orchestrates a transcriptional “repertoire” that is required for thymocyte maturation up to and beyond the pro-T-cell stage. Second, GATA-3 critically suppresses a latent B-cell potential in pro–T cells. As such, GATA-3 is essential to sealing in Notch-induced T-cell fate in early thymocyte precursors by promoting T-cell identity through the repression of alternative developmental options.Entities:
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Year: 2013 PMID: 23287858 DOI: 10.1182/blood-2012-06-440065
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113