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Molecular and Cellular Biology Volume 20, 2000 - Issue 1
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Transcriptional Regulation

Auto-Inhibition of Ets-1 Is Counteracted by DNA Binding Cooperativity with Core-Binding Factor α2

Tamara L. Goetz1 Huntsman Cancer Institute, University of Utah, Salt Lake City, Utah84112-5550
,
Ting-Lei Gu2 Department of Biochemistry, Dartmouth Medical School, Hanover, New Hampshire03755
,
Nancy A. Speck2 Department of Biochemistry, Dartmouth Medical School, Hanover, New Hampshire03755
&
Barbara J. Graves1 Huntsman Cancer Institute, University of Utah, Salt Lake City, Utah84112-5550Correspondence[email protected]
Pages 81-90 | Received 15 Jun 1999, Accepted 04 Oct 1999, Published online: 28 Mar 2023
 
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Abstract

Auto-inhibition is a common transcriptional control mechanism that is well characterized in the regulatory transcription factor Ets-1. Autoinhibition of Ets-1 DNA binding works through an inhibitory module that exists in two conformations. DNA binding requires a change in the inhibitory module from the packed to disrupted conformation. This structural switch provides a mechanism to tightly regulate Ets-1 DNA binding. We report that the Ets-1 partner protein core-binding factor α2 (CBFα2; also known as AML1 or PEBP2) stimulates Ets-1 DNA binding and counteracts auto-inhibition. Support for this conclusion came from three observations. First, the level of cooperative DNA binding (10-fold) was similar to the level of repression by auto-inhibition (10- to 20-fold). Next, a region necessary for cooperative DNA binding mapped to the inhibitory module. Third, an Ets-1 mutant with a constitutively disrupted inhibitory module did not bind DNA cooperatively with CBFα2. Furthermore, two additional lines of evidence indicated that CBFα2 affects the structural switch by direct interactions with Ets-1. First, the retention of cooperative DNA binding on nicked duplexes eliminated a potential role of through-DNA effects. Second, cooperative DNA binding was observed on composite sites with altered spacing or reversed orientation. We suggest that only protein interactions can accommodate this observed flexibility. These findings provide a mechanism by which CBF relieves the auto-inhibition of Ets-1 and illustrates one strategy for the synergistic activity of regulatory transcription factors.

ACKNOWLEDGMENTS

We acknowledge research support from the National Institutes of Health to B.J.G. (GM38663) and training grant support for T.L.G. (CA090602). National Institutes of Health support to the Huntsman Cancer Institute (CA42014) is also acknowledged. N.A.S. was supported by National Institutes of Health grants CA58343 and CA75611.

We are grateful to Don Ayer, John Bushweller, and Lawrence McIntosh for critical comments on the manuscript.

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