Programming for T-lymphocyte fates: modularity and mechanisms
- Creators
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Rothenberg, Ellen V.
Abstract
T-cell development in mammals is a model for lineage choice and differentiation from multipotent stem cells. Although T-cell fate choice is promoted by signaling in the thymus through one dominant pathway, the Notch pathway, it entails a complex set of gene regulatory network and chromatin state changes even before the cells begin to express their signature feature, the clonal-specific T-cell receptors (TCRs) for antigen. This review distinguishes three developmental modules for T-cell development, which correspond to cell type specification, TCR expression and selection, and the assignment of cells to different effector types. The first is based on transcriptional regulatory network events, the second is dominated by somatic gene rearrangement and mutation and cell selection, and the third corresponds to establishing a poised state of latent regulator priming through an unknown mechanism. Interestingly, in different lineages, the third module can be deployed at variable times relative to the completion of the first two modules. This review focuses on the gene regulatory network and chromatin-based kinetic constraints that determine activities of transcription factors TCF1, GATA3, PU.1, Bcl11b, Runx1, and E proteins in the primary establishment of T-cell identity.
Additional Information
© 2019 Rothenberg; Published by Cold Spring Harbor Laboratory Press. This article is distributed exclusively by Cold Spring Harbor Laboratory Press for the first six months after the full-issue publication date (see http://genesdev.cshlp.org/site/misc/terms.xhtml). After six months, it is available under a Creative Commons License (Attribution-NonCommercial 4.0 International), as described at http://creativecommons.org/licenses/by-nc/4.0/. The ideas in this review were greatly enriched by discussions with Avinash Bhandoola, Max D. Cooper, James Di Santo, Hao Yuan Kueh, Cornelis Murre, John J. O'Shea, and Ichiro Taniuchi. I am very grateful to Mary A. Yui for valuable critical reading and comments, and to current and recent members of my research group for stimulating discoveries and shared ideas. Relevant work in E.V.R.'s laboratory was supported by grants from the U.S. Public Health Service (R01AI083514, R01AI095943, R01AI135200, R01HD076915, and R01HL119102) and by the Albert Billings Ruddock Professorship in Biology.Attached Files
Published - Genes_Dev.-2019-Rothenberg-1117-35.pdf
Supplemental Material - Supplemental_Material_Figure1_and_Legend_.pdf
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Additional details
- PMCID
- PMC6719619
- Eprint ID
- 98871
- Resolver ID
- CaltechAUTHORS:20190926-101246969
- R01AI083514
- NIH
- R01AI095943
- NIH
- R01AI135200
- NIH
- R01HD076915
- NIH
- R01HL119102
- NIH
- Albert Billings Ruddock Professorship
- Created
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2019-09-26Created from EPrint's datestamp field
- Updated
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2021-11-16Created from EPrint's last_modified field