Structural Diversity in p160/CREB-binding Protein Coactivator Complexes

Waters, Lorna C.; Yue, Baigong; Veverka, Václav; Renshaw, Philip S.; Bramham, Janice; Matsuda, Sachiko; Frenkiel, Thomas A.; Kelly, Geoffrey; Muskett, Frederick W.; Carr, Mark D.; Heery, David M.

doi:10.1074/jbc.m600237200

Cited by 70 publications

(66 citation statements)

References 50 publications

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“…Over the past 10 years, a combination of biochemical, genetic, and structural experiments has conclusively identified relevant targets for some mammalian and yeast activators (e.g., Stevens et al 2002;Yang et al 2004;Green 2005;Sampietro et al 2006;Waters et al 2006;Thakur et al 2009;Herbig et al 2010;Jedidi et al 2010). In general, these targets are located in coactivator complexes and chromatin-remodeling or -modifying factors rather than in subunits of the general transcription factors.…”

Section: Activator Targetsmentioning

confidence: 99%

Transcriptional Regulation inSaccharomyces cerevisiae: Transcription Factor Regulation and Function, Mechanisms of Initiation, and Roles of Activators and Coactivators

2011

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Here we review recent advances in understanding the regulation of mRNA synthesis in Saccharomyces cerevisiae. Many fundamental gene regulatory mechanisms have been conserved in all eukaryotes, and budding yeast has been at the forefront in the discovery and dissection of these conserved mechanisms. Topics covered include upstream activation sequence and promoter structure, transcription factor classification, and examples of regulated transcription factor activity. We also examine advances in understanding the RNA polymerase II transcription machinery, conserved coactivator complexes, transcription activation domains, and the cooperation of these factors in gene regulatory mechanisms. TABLE OF CONTENTS Abstract 705Introduction 706

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Section: Activator Targetsmentioning

confidence: 99%

Transcriptional Regulation inSaccharomyces cerevisiae: Transcription Factor Regulation and Function, Mechanisms of Initiation, and Roles of Activators and Coactivators

2011

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“…The NCBD:ACTR complex was the first documented example of an IDP that folds upon binding to another IDP in a process termed mutual synergistic folding (16). Structural studies of the complexes of NCBD and three of its ligands have shown that the complexes have fully compact and well defined globular structures, and that NCBD adopts at least two different ligand specific structures (16,19,20). This structural adaptability is a functional hallmark of the IDPs.…”

Section: Creb Binding Protein | Folding Upon Binding | Nmr Spectroscopymentioning

confidence: 99%

Conformational selection in the molten globule state of the nuclear coactivator binding domain of CBP

Kjærgaard

Teilum

Poulsen

2010

Proc. Natl. Acad. Sci. U.S.A.

153

242

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Native molten globules are the most folded kind of intrinsically disordered proteins. Little is known about the mechanism by which native molten globules bind to their cognate ligands to form fully folded complexes. The nuclear coactivator binding domain (NCBD) of CREB binding protein is particularly interesting in this respect as structural studies of its complexes have shown that NCBD folds into two remarkably different states depending on the ligand being ACTR or IRF-3. The ligand-free state of NCBD was characterized in order to understand the mechanism of folding upon ligand binding. Biophysical studies show that despite the molten globule nature of the domain, it contains a small cooperatively folded core. By NMR spectroscopy, we have demonstrated that the folded core of NCBD has a well ordered conformer with specific side chain packing. This conformer resembles the structure of the NCBD in complex with the protein ligand, ACTR, suggesting that ACTR binds to prefolded NCBD molecules from the ensemble of interconverting structures.CREB binding protein | folding upon binding | NMR spectroscopy T he protein structure-function paradigm has dominated structural and molecular biology over the past five decades. This paradigm has been challenged by the discovery of functional but intrinsically disordered proteins (IDPs) (1). IDPs are abundant in higher organisms and are necessary for many crucial biological functions such as cell cycle regulation, signal transduction, and regulation of transcription (2, 3). Structural studies of IDPs have shown that despite the high degree of disorder, these proteins are far from randomly structured and form transient, yet specific, secondary and tertiary structural elements (4, 5). The success of the structure-function paradigm in explaining the function of folded proteins suggests that the functions of the IDPs may also be understood by studying the transient structure of the disordered state.The molten globule was originally discovered as a partially folded state under mildly denaturing conditions and was shown to accumulate as an intermediate during protein folding reactions (6, 7). With the emergence of the IDPs, proteins were discovered where the molten globule is the functionally active state. Native molten globules are the most compact conformational state considered as IDPs (4). Molten globules have native-like secondary structure, but are believed to lack the well-defined tertiary interactions found in folded proteins. Most high resolution NMR studies of the molten globule state have focused on the secondary structure of the backbone as this is more readily accessible from secondary chemical shifts (8). The degree of side chain packing, however, is less well understood. Molten globules are believed to have dynamic hydrophobic cores due to the lack of signal in the near-UV CD spectrum and the broadening of NMR signals of aromatic groups (6, 7). Recent studies have shown that the side chains in the α-lactalbumin molten globule exchange between several well defined confor...

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“…Upon binding to its physiological partners, the NCBD folds to form a bundle of three helices that differ in their topological arrangements in complexes with intrinsically disordered targets, such as the p160 nuclear coactivators ACTR (coactivator for thyroid and retinoid receptors) and SRC-1 and the p53 activation domain (18,54,55), and in the complex with the stably folded interferon regulatory factor IRF-3 (56). Detailed NMR and computational studies suggest that in the unbound state, the NCBD is flexible and fluctuates over an ensemble of conformations that includes both the ACTR/SRC-1-bound conformation and the IRF-3-bound conformation (57-61).…”

Section: Ncbd Interactionsmentioning

confidence: 99%

Role of Intrinsic Protein Disorder in the Function and Interactions of the Transcriptional Coactivators CREB-binding Protein (CBP) and p300

Dyson

Wright

2016

Journal of Biological Chemistry

275

270

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The transcriptional coactivators CREB-binding protein (CBP) and p300 undergo a particularly rich set of interactions with disordered and partly ordered partners, as a part of their ubiquitous role in facilitating transcription of genes. CBP and p300 contain a number of small structured domains that provide scaffolds for the interaction of disordered transactivation domains from a wide variety of partners, including p53, hypoxiainducible factor 1␣ (HIF-1␣), NF-B, and STAT proteins, and are the targets for the interactions of disordered viral proteins that compete with cellular factors to disrupt signaling and subvert the cell cycle. The functional diversity of the CBP/p300 interactome provides an excellent example of the power of intrinsic disorder to facilitate the complexity of living systems.

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Structural Diversity in p160/CREB-binding Protein Coactivator Complexes

Cited by 70 publications

References 50 publications

Transcriptional Regulation inSaccharomyces cerevisiae: Transcription Factor Regulation and Function, Mechanisms of Initiation, and Roles of Activators and Coactivators

Transcriptional Regulation inSaccharomyces cerevisiae: Transcription Factor Regulation and Function, Mechanisms of Initiation, and Roles of Activators and Coactivators

Conformational selection in the molten globule state of the nuclear coactivator binding domain of CBP

Role of Intrinsic Protein Disorder in the Function and Interactions of the Transcriptional Coactivators CREB-binding Protein (CBP) and p300

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