Literature DB >> 21317429

Transient-state kinetic analysis of transcriptional activator·DNA complexes interacting with a key coactivator.

Amberlyn M Wands1, Ningkun Wang, Jenifer K Lum, John Hsieh, Carol A Fierke, Anna K Mapp.   

Abstract

Several lines of evidence suggest that the prototypical amphipathic transcriptional activators Gal4, Gcn4, and VP16 interact with the key coactivator Med15 (Gal11) during transcription initiation despite little sequence homology. Recent cross-linking data further reveal that at least two of the activators utilize the same binding surface within Med15 for transcriptional activation. To determine whether these three activators use a shared binding mechanism for Med15 recruitment, we characterized the thermodynamics and kinetics of Med15·activator·DNA complex formation by fluorescence titration and stopped-flow techniques. Combination of each activator·DNA complex with Med15 produced biphasic time courses. This is consistent with a minimum two-step binding mechanism composed of a bimolecular association step limited by diffusion, followed by a conformational change in the Med15·activator·DNA complex. Furthermore, the equilibrium constant for the conformational change (K(2)) correlates with the ability of an activator to stimulate transcription. VP16, the most potent of the activators, has the largest K(2) value, whereas Gcn4, the least potent, has the smallest value. This correlation is consistent with a model in which transcriptional activation is regulated at least in part by the rearrangement of the Med15·activator·DNA ternary complex. These results are the first detailed kinetic characterization of the transcriptional activation machinery and provide a framework for the future design of potent transcriptional activators.

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Year:  2011        PMID: 21317429      PMCID: PMC3091231          DOI: 10.1074/jbc.M110.207589

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  47 in total

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6.  Evidence that Gal11 protein is a target of the Gal4 activation domain in the mediator.

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  12 in total

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4.  Caught in the act: covalent cross-linking captures activator-coactivator interactions in vivo.

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7.  Discovery of Enzymatic Targets of Transcriptional Activators via in Vivo Covalent Chemical Capture.

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10.  DNA Methylation at the Novel CpG Sites in the Promoter of MED15/PCQAP Gene as a Biomarker for Head and Neck Cancers.

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