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Article

Differential Gene Regulation by Selective Association of Transcriptional Coactivators and bZIP DNA-Binding Domains

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Pages 5969-5982 | Received 22 Apr 2006, Accepted 02 Jun 2006, Published online: 27 Mar 2023
 

Abstract

bZIP DNA-binding domains are targets for viral and cellular proteins that function as transcriptional coactivators. Here, we show that MBF1 and the related Chameau and HBO1 histone acetylases interact with distinct subgroups of bZIP proteins, whereas pX does not discriminate. Selectivity of Chameau and MBF1 for bZIP proteins is mediated by residues in the basic region that lie on the opposite surface from residues that contact DNA. Chameau functions as a specific coactivator for the AP-1 class of bZIP proteins via two arginine residues. A conserved glutamic acid/glutamine in the linker region underlies MBF1 specificity for a subgroup of bZIP factors. Chameau and MBF1 cannot synergistically coactivate transcription due to competitive interactions with the basic region, but either protein can synergistically coactivate with pX. Analysis of Jun derivatives that selectively interact with these coactivators reveals that MBF1 is crucial for the response to oxidative stress, whereas Chameau is important for the response to chemical and osmotic stress. Thus, the bZIP domain mediates selective interactions with coactivators and hence differential regulation of gene expression.

Supplemental material for this article may be found at http://mcb.asm.org/.

We are very grateful to A. Swaroop, J. Alam, A. Friedman, P. Johnson, J.-M. Mesnard, S. X. Hou, A. Sergeant, P. M. Lieberman, R. Prywes, S. Taylor, J. A. Goodrich, O. M. Andrisani, J. Auwerx, K. H. Klempnauer, P. Sassone-Corsi, and M. Safak for the different DNA plasmids they provide us. We also thank J. Pradel for the gift of the Chameau primary antibody and A. B. Lassar for the used of the Avoroskan Ascent F.L. luminometer.

This work was supported by grants to K.S. from the National Institutes of Health (GM30186).

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