| Literature DB >> 18274628 |
Eimear M Mullen1, Peili Gu, Austin J Cooney.
Abstract
Embryonic stem (ES) cells have great therapeutic potential because they are capable of indefinite self-renewal and have the potential to differentiate into over 200 different cell types that compose the human body. The switch from the pluripotent phenotype to a differentiated cell involves many complex signaling pathways including those involving LIF/Stat3 and the transcription factors Sox2, Nanog and Oct-4. Many nuclear receptors play an important role in the maintenance of pluripotence (ERRbeta, SF-1, LRH-1, DAX-1) repression of the ES cell phenotype (RAR, RXR, GCNF) and also the differentiation of ES cells (PPARgamma). Here we review the roles of the nuclear receptors involved in regulating these important processes in ES cells.Entities:
Year: 2007 PMID: 18274628 PMCID: PMC2233893 DOI: 10.1155/2007/61563
Source DB: PubMed Journal: PPAR Res Impact factor: 4.964
Figure 1Yin-yang regulation of Oct-4 expression during ES cell differentiation by LRH-1 and GCNF, which compete for the same element. In undifferentiated ES cells LRH-1 binds to elements in the Oct-4 proximal enhancer and proximal promoter to maintain its expression during the very earliest stages of differentiation. As differentiation progresses LRH-1 expression decreases and GCNF expression is induced. At an intermediate point GCNF displaces LRH-1 and represses Oct-4 by recruiting the DNA methylation machinery that ultimately leads to the silencing of Oct-4 expression in somatic cells.
Summary of involvement of nuclear receptors in mouse ES cell pluripotency and differentiation.
| Nuclear receptor | Function |
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| ERR | Maintenance of pluripotency and repression of differentiation. |
| Repression of differentiation along specific cell lineages | |
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| SF-1 | Maintenance of Oct-4 expression in embryonic carcinoma cells |
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| LRH-1 | Maintenance of Oct-4 expression in ES cells. |
| Interaction with
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| DAX-1 | May act as a repressor of SF-1, LRH-1, ER, AR, and PR. |
| Conditional KO causes loss of pluripotency and differentiation | |
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| RAR | Down regulation of Oct-4. |
| Upregulation of GCNF. Neuronal differentiation | |
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| RXR | May play role in differentiation of cardiomyocytes |
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| GCNF | GCNF required for repression of Oct-4, Nanog, and Sox2 upon differentiation with RA. |
| Repression of ES cell phenotype | |
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| PPAR | Required in the early stages of adipose differentiation. |
| Differentiation down osteogenic lineage in siRNA experiments. | |
| PPAR | |