CGC Bibliography Paper 5042
A POP-1 repressor complex restricts inappropriate cell type-specific gene transcription during Caenorhabditis elegans embryogenesis.
Calvo D,
Victor M,
Gay F,
Sui G,
Luke MPS,
Dufourcq P,
Wen G,
Maduro M,
Rothman J,
Shi Y
- Medline:
- 11742996
- Citation:
- EMBO Journal 20: 7197-7208 2001
- Type:
- ARTICLE
- Genes:
- cbp-1 end-1 hda-1 hda-3 pop-1 unc-37
- Abstract:
- In Caenorhabditis elegans, histone acetyltransferase CBP-1 counteracts the repressive activity of the histone deacetylase HDA-1 to allow endoderm differentiation, which is specified by the E cell. In the sister MS cell, the endoderm fate is prevented by the action of an HMG box-containing protein, POP-1, through an unknown mechanism. In this study, we show that CBP-1, HDA-1 and POP-1 converge on end-1, an initial endoderm-determining gene. In the E lineage, an essential function of CBP-1 appears to be the activation of end-1 transcription. We further identify a molecular mechanism for the endoderm-suppressive effect of POP-1 in the MS lineage by demonstrating that POP-1 functions as a transcriptional repressor that inhibits inappropriate end-1 transcription. We provide evidence that POP-1 represses transcription via the recruitment of HDA-1 and UNC-37, the C.elegans homolog of the co-repressor Groucho. These findings demonstrate the importance of the interplay between acetyltransferases and deacetylases in the regulation of a critical cell fate-determining gene during development. Furthermore, they identify a strategy by which concerted actions of historic deacetylases and other co-repressors ensure maximal repression of inappropriate cell type-specific gene