Literature DB >> 17937915

Partial agonists activate PPARgamma using a helix 12 independent mechanism.

John B Bruning1, Michael J Chalmers, Swati Prasad, Scott A Busby, Theodore M Kamenecka, Yuanjun He, Kendall W Nettles, Patrick R Griffin.   

Abstract

Binding to helix 12 of the ligand-binding domain of PPARgamma is required for full agonist activity. Previously, the degree of stabilization of the activation function 2 (AF-2) surface was thought to correlate with the degree of agonism and transactivation. To examine this mechanism, we probed structural dynamics of PPARgamma with agonists that induced graded transcriptional responses. Here we present crystal structures and amide H/D exchange (HDX) kinetics for six of these complexes. Amide HDX revealed each ligand induced unique changes to the dynamics of the ligand-binding domain (LBD). Full agonists stabilized helix 12, whereas intermediate and partial agonists did not at all, and rather differentially stabilized other regions of the binding pocket. The gradient of PPARgamma transactivation cannot be accounted for solely through changes to the dynamics of AF-2. Thus, our understanding of allosteric signaling must be extended beyond the idea of a dynamic helix 12 acting as a molecular switch.

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Year:  2007        PMID: 17937915     DOI: 10.1016/j.str.2007.07.014

Source DB:  PubMed          Journal:  Structure        ISSN: 0969-2126            Impact factor:   5.006


  117 in total

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3.  Time window expansion for HDX analysis of an intrinsically disordered protein.

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Authors:  Jie Zheng; Cesar Corzo; Mi Ra Chang; Jinsai Shang; Vinh Q Lam; Richard Brust; Anne-Laure Blayo; John B Bruning; Theodore M Kamenecka; Douglas J Kojetin; Patrick R Griffin
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Authors:  Laura M van Marrewijk; Steven W Polyak; Marcel Hijnen; Dana Kuruvilla; Mi Ra Chang; Youseung Shin; Theodore M Kamenecka; Patrick R Griffin; John B Bruning
Journal:  ACS Chem Biol       Date:  2015-12-03       Impact factor: 5.100

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