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Transcriptional Regulation

CtBP-Independent Repression in the Drosophila Embryo

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Pages 3990-3999 | Received 16 Sep 2002, Accepted 21 Feb 2003, Published online: 27 Mar 2023
 

Abstract

There are three mechanisms of transcriptional repression in eukaryotes. The first is quenching, whereby repressors and activators co-occupy closely linked sites and then the repressor inhibits adjacent activators. The second is direct repression, in which repressors block the function of the core transcription complex. The third is competition, in which repressors compete with activators for a common DNA-binding site. Previous studies have shown that the Drosophila melanogaster CtBP corepressor (dCtBP) is essential for the quenching activity of three short-range sequence-specific repressors in the early Drosophila embryo: Krüppel, Knirps, and Snail. Here we demonstrate that dCtBP is dispensable for target enhancers that contain overlapping activator and repressor binding sites. However, it is essential when Krüppel and Knirps repressor sites do not overlap activator sites but are instead located adjacent to either activators or the core promoter. These findings provide evidence that competition is distinct from quenching and direct repression. Quenching and direct repression depend on dCtBP, whereas competition does not.

ACKNOWLEDGMENTS

We thank Kevin Wright for construction of the His-Dorsal vector and Stephen Small for providing the pPac Dorsal vector. We also thank Angelike Stathopoulos and Anna Di Gregorio for valuable advice.

Y.N. was supported by the Uehara Memorial Foundation. This work was funded by an NIH grant (GM 34431).

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