An alternate binding site for PPARγ ligands

Hughes, Travis S.; Giri, Pankaj K.; Vera, Ian Mitchelle S. de; Marciano, David; Kuruvilla, Dana S.; Shin, Youseung; Blayo, Anne‐Laure; Kamenecka, Theodore M.; Burris, Thomas P.; Griffin, Patrick R.; Kojetin, D.J.

doi:10.1038/ncomms4571

Cited by 167 publications

(227 citation statements)

References 65 publications

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“…One is CLBP with the predicted docking score of −34.72 kJ/mol, and the other is a second binding site with a docking score of −28.03 kJ/mol, indicating BVC occupied the CLBP with higher binding affinity. The second binding site for BVC was consistent with the alternative binding site (ABS), which was composed of H2′, Ω loop, H3 and β sheets [33]. In addition, if one BVC was docked to CLBP first (Fig.…”

Section: Lc 2 7 a 4 F G F 2 1 A D Ip O Q A C A C B P P A R -A C A D Mmentioning

confidence: 59%

“…PPAR senses ligands through ligandbinding sites in the LBD [43,44]. The PPAR-γ-LBD has shown two binding sites, CLBP and ABS; synthetic PPAR ligands are designed to bind to CLBP by mimicking endogenous ligands [33]. GW9662, a PPAR covalent antagonist, can compete for the CLBP of synthetic ligands to PPAR and block binding to CLBP.…”

Section: Discussionmentioning

confidence: 99%

“…These changes vary depending on the type of ligand that binds to the LBD. TZDs and fibrates induce direct stabilisation of AF-2 conformation through distinct interactions with helix 12 of the AF-2 domain, followed by the recruitment of coactivators, including PGC-1α and TRAP220 [33]. BVC does not recruit PGC-1α and TRAP220 during the transcriptional process-its unique binding mode results in indirect stabilisation of AF-2 mediated via an Ω loop and helix 3.…”

Section: Discussionmentioning

confidence: 99%

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Bavachinin, as a novel natural pan-PPAR agonist, exhibits unique synergistic effects with synthetic PPAR-γ and PPAR-α agonists on carbohydrate and lipid metabolism in db/db and diet-induced obese mice

Luo

et al. 2016

Diabetologia

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Section: Lc 2 7 a 4 F G F 2 1 A D Ip O Q A C A C B P P A R -A C A D Mmentioning

confidence: 59%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Bavachinin, as a novel natural pan-PPAR agonist, exhibits unique synergistic effects with synthetic PPAR-γ and PPAR-α agonists on carbohydrate and lipid metabolism in db/db and diet-induced obese mice

Luo

et al. 2016

Diabetologia

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“…In addition to a plethora of studies in the field of enzymology, where the phenomenon of allostery was first described (Monod et al, 1963(Monod et al, , 1965Koshland et al, 1966;Changeux, 2013), allosteric modulators have now been identified for all receptor superfamilies, including ligand-gated ion channels (Olsen et al, 2004;Taly et al, 2009;Traynelis et al, 2010), voltage-gated ion channels (Spedding et al, 1995;Catterall et al, 2007), nuclear hormone receptors (Estebanez-Perpina et al, 2007;Hughes et al, 2014), receptor tyrosine kinases (Bono et al, 2013;De Smet et al, 2014), and GPCRs. As a consequence, there exists a large body of literature in which the definition of the term "allosteric" and the description/classification of allosteric ligands can be quite varied and, in many instances, confusing (Colquhoun, 1998;Fenton, 2008;Nussinov and Tsai, 2013).…”

Section: Classification Of Allosteric Modulatorsmentioning

confidence: 99%

Advances in G Protein-Coupled Receptor Allostery: From Function to Structure

2014

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It is now widely accepted that G protein-coupled receptors (GPCRs) are highly dynamic proteins that adopt multiple active states linked to distinct functional outcomes. Furthermore, these states can be differentially stabilized not only by orthosteric ligands but also by allosteric ligands acting at spatially distinct binding sites. The key pharmacologic characteristics of GPCR allostery include improved selectivity due to either greater sequence divergence between receptor subtypes and/or subtype-selective cooperativity, a ceiling level to the effect, probe dependence (whereby the magnitude and direction of the allosteric effect change with the nature of the interacting ligands), and the potential for biased signaling.Recent chemical biology developments are beginning to demonstrate how the incorporation of analytical pharmacology and operational modeling into the experimental workflow can enrich structure-activity studies of allostery and bias, and have also led to the discovery of a new class of hybrid orthosteric/ allosteric (bitopic) molecules. The potential for endogenous allosteric modulators to play a role in physiology and disease remains to be fully appreciated but will likely represent an important area for future studies. Finally, breakthroughs in structural and computational biology are beginning to unravel the mechanistic basis of GPCR allosteric modulation at the molecular level.

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“…For example, the androgen receptor possesses a unique binding surface, termed BF-3, that recognizes small molecules such as 3,3,5-triiodothyroacetic acid to allosterically modulate the binding of coactivators to the adjacent AF-2 region (Estebanez-Perpina et al, 2007b). Most recently, a novel allosteric ligand binding site was identified on PPARg that, when bound by small molecules, engendered a unique pharmacological profile of regulation of the receptor (Hughes et al, 2014). This suggests that the design of allosteric ligands for NHRs may be primed to develop as a field, akin to other classes of receptor modulators over the past decade.…”

Section: Nuclear Hormone Receptorsmentioning

confidence: 99%