Negotiation of the T Lineage Fate Decision by Transcription-Factor Interplay and Microenvironmental Signals
- Creators
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Rothenberg, Ellen V.
Abstract
Notch-Delta signaling of hematopoietic precursors sets in motion a train of events that activates expression of T lineage genes. Even so, through many cell generations the pro-T cells remain uncommitted to the T cell fate, preserving alternative potentials as divergent as monocyte or dendritic cell fates. This plasticity can be explained by the tenacious expression of stem- and progenitor-associated regulatory genes in the cells, and by the combinatorial coding of T cell identity by factors that are not intrinsically T lineage specific in their spectra of activity. T lineage developmental success depends on precise temporal and quantitative regulation of these factors and on the continuing modulating influence of Notch-Delta signals that buffer the cells against mechanisms promoting non-T outcomes. An additional mechanism, still not fully defined, is required just prior to T cell receptor-mediated selection to end plasticity and make T lineage commitment irreversible.
Additional Information
© 2007 Elsevier Inc. Available online 21 June 2007. The author owes both thanks and apologies to many authors whose work helped to develop the ideas in this review but could not be cited properly because of length limits. The review benefited greatly from illuminating discussions with W. Pear. Special thanks is due to D. Scripture-Adams for valuable preliminary discussions about this review. The author is also grateful to past and present members of her lab for permission to cite unpublished work. Related research in the author's lab was supported by NIH grants CA90233 and CA98925.Additional details
- Eprint ID
- 74073
- DOI
- 10.1016/j.immuni.2007.06.005
- Resolver ID
- CaltechAUTHORS:20170206-104749499
- CA90233
- NIH
- CA98925
- NIH
- Created
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2017-02-06Created from EPrint's datestamp field
- Updated
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2021-11-11Created from EPrint's last_modified field