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Modulators of the structural dynamics of the retinoid X receptor to reveal receptor function
Authors:Nahoum Virginie  Pérez Efrén  Germain Pierre  Rodríguez-Barrios Fátima  Manzo Fabio  Kammerer Sabrina  Lemaire Geraldine  Hirsch Oliver  Royer Catherine A  Gronemeyer Hinrich  de Lera Angel R  Bourguet William
Affiliation:Institut National de la Santé et de la Recherche Médicale, U554, 34090 Montpellier, France.
Abstract:Retinoid X receptors (RXRalpha, -beta, and -gamma) occupy a central position in the nuclear receptor superfamily, because they form heterodimers with many other family members and hence are involved in the control of a variety of (patho)physiologic processes. Selective RXR ligands, referred to as rexinoids, are already used or are being developed for cancer therapy and have promise for the treatment of metabolic diseases. However, important side effects remain associated with existing rexinoids. Here we describe the rational design and functional characterization of a spectrum of RXR modulators ranging from partial to pure antagonists and demonstrate their utility as tools to probe the implication of RXRs in cell biological phenomena. One of these ligands renders RXR activity particularly sensitive to coactivator levels and has the potential to act as a cell-specific RXR modulator. A combination of crystallographic and fluorescence anisotropy studies reveals the molecular details accounting for the agonist-to-antagonist transition and provides direct experimental evidence for a correlation between the pharmacological activity of a ligand and its impact on the structural dynamics of the activation helix H12. Using RXR and its cognate ligands as a model system, our correlative analysis of 3D structures and dynamic data provides an original view on ligand actions and enables the establishment of mechanistic concepts, which will aid in the development of selective nuclear receptor modulators.
Keywords:crystal structure   ligand design   nuclear receptor   agonist   antagonist
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