Transcriptional regulation of lymphocyte lineage commitment
Abstract
The development of T cells and B cells from pluripotent hematopoietic precursors occurs through a stepwise narrowing of developmental potential that ends in lineage commitment. During this process, lineage-specific genes are activated asynchronously, and lineage-inappropriate genes, although initially expressed, are asynchronously turned off. These complex gene expression events are the outcome of the changes in expression of multiple transcription factors with partially overlapping roles in early lymphocyte and myeloid cell development. Key transcription factors promoting B-cell development and candidates for this role in T-cell development are discussed in terms of their possible modes of action in fate determination. We discuss how a robust, stable, cell-type–specific gene expression pattern may be established in part by the interplay between endogenous transcription factors and signals transduced by cytokine receptors, and in part by the network of effects of particular transcription factors on each other.
Additional Information
© 1999 John Wiley & Sons, Inc. Issue online: 25 August 1999; Version of record online: 25 August 1999. Funding agencies: Stowers Institute for Medical Research; USPHS; Grant numbers: AI34041; AG13108. We apologize to the many colleagues whose important work could not be cited due to space constraints. The authors gratefully acknowledge the valuable criticism of Drs. Eric Davidson and Jonathan Rast, and helpful discussions with other members of the Rothenberg laboratory.Additional details
- Eprint ID
- 74178
- Resolver ID
- CaltechAUTHORS:20170208-155733709
- Stowers Institute for Medical Research
- AI34041
- NIH
- AG13108
- NIH
- Created
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2017-02-09Created from EPrint's datestamp field
- Updated
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2021-11-11Created from EPrint's last_modified field