Modulators of the structural dynamics of the retinoid X receptor to reveal receptor function

Nahoum, Virginie; Pérez, Efrèn; Germain, Pierre; Rodrı́guez-Barrios, Fátima; Manzo, Fabio; Kammerer, Sabrina; Lemaire, G.; Hirsch, Oliver; Royer, Catherine A.; Gronemeyer, Hinrich; Lera, Ángel R. de; Bourguet, William

doi:10.1073/pnas.0705356104

Cited by 135 publications

(180 citation statements)

References 37 publications

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“…The conclusion from this study, namely that activation of PPARG is not solely determined by helix 12 positioning and dynamics, led the authors to conclude that the 'understanding of allosteric signaling must be extended beyond the idea of a dynamic helix 12 acting as a molecular switch' (Bruning et al 2007). Similar observations were noted for the LBD of RXRA (Yan et al 2004, 2006, Nahoum et al 2007) and, more recently, ERa (Dai et al 2008). In the case of ERa, different groups of hydrogen exchange signatures are observed for ER agonists and SERMs, suggesting that hydrogen exchange signatures can provide a method for predicting tissue-specific ligand response.…”

Section: J Kojetin Et Al: Implications Of a Second Er Ligand-bindisupporting

confidence: 63%

Implications of the binding of tamoxifen to the coactivator recognition site of the estrogen receptor

Kojetin¹,

Burris²,

Jensen³

et al. 2008

Endocrine Related Cancer

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A number of studies have reported on the unusual pharmacological behavior of type I antiestrogens, such as tamoxifen. These agents display mixed agonist/antagonist activity in a dose-, cell-, and tissue-specific manner. Consequently, many efforts have been made to develop so-called 'pure' antiestrogens that lack mixed agonist/antagonist activity. The recent report of the structure of estrogen receptor (ER) b with a second molecule of 4-hydroxytamoxifen (HT) bound in the coactivator-binding surface of the ligand-binding domain (LBD) represents the first direct example of a second ER ligand-binding site and provides insight into the possible origin of mixed agonist/antagonist activity of type I antiestrogens. In this review, we summarize the biological reports leading up to the structural conformation of a second ER ligand-binding site, compare the ERb LBD structure bound with two HT molecules to other ER structures, and discuss the potential for small molecular inhibitors designed to directly inhibit ER-coactivator and, more generally, nuclear receptor (NR)-coactivator interactions. The studies support a departure from the traditional paradigm of drug targeting to the ligand-binding site, to that of a rational approach targeting a functionally important surface, namely the NR coactivator-binding (activation function-2) surface. Furthermore, we provide evidence supporting a reevaluation of the strict interpretation of the agonist/antagonist state with respect to the position of helix 12 in the NR LBD.

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Section: J Kojetin Et Al: Implications Of a Second Er Ligand-bindisupporting

confidence: 63%

Implications of the binding of tamoxifen to the coactivator recognition site of the estrogen receptor

Kojetin¹,

Burris²,

Jensen³

et al. 2008

Endocrine Related Cancer

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“…Role of RXR in Bexarotene-enhanced Myoblast Differentiation-To assess whether bexarotene-enhanced myoblast differentiation is mediated through RXR activation, we first employed a potent RXR antagonist UVI3003 (34). C2C12 myoblasts were differentiated with bexarotene in the presence of high concentrations of UVI3003, about 30-and 150-fold of K d values.…”

Section: Resultsmentioning

confidence: 99%

Retinoid X Receptor-selective Signaling in the Regulation of Akt/Protein Kinase B Isoform-specific Expression

AlSudais

Aabed

Nicola

et al. 2016

Journal of Biological Chemistry

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The differentiation and fusion of myoblasts into mature myotubes are complex processes responding to multiple signaling pathways. The function of Akt/PKB is critical for myogenesis, but less is clear as to the regulation of its isoform-specific expression. Bexarotene is a drug already used clinically to treat cancer, and it has the ability to enhance the commitment of embryonic stem cells into skeletal muscle lineage. Whereas bexarotene regulates fundamental biological processes through retinoid X receptor (RXR)-mediated gene expression, molecular pathways underlying its positive effects on myogenesis remain unclear. In this study, we have examined the signaling pathways that transmit bexarotene action in the context of myoblast differentiation. We show that bexarotene promotes myoblast differentiation and fusion through the activation of RXR and the regulation of Akt/PKB isoform-specific expression. Interestingly, bexarotene signaling appears to correlate with residuespecific histone acetylation and is able to counteract the detrimental effects of cachectic factors on myogenic differentiation. We also signify an isoform-specific role for Akt/PKB in RXRselective signaling to promote and to retain myoblast differentiation. Taken together, our findings establish the viability of applying bexarotene in the prevention and treatment of musclewasting disorders, particularly given the lack of drugs that promote myogenic differentiation available for potential clinical applications. Furthermore, the model of bexarotene-enhanced myogenic differentiation will provide an important avenue to identify additional genetic targets and specific molecular interactions that we can study and apply for the development of potential therapeutics in muscle regeneration and repair.

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“…DNA oligos and sequencing were provided by the Keck Biotechnology Center at Yale University. UVI3001 and UVI3003 are gifts from Prof. Angel R. de Lera (Universidade de Vigo, Spain) ( 41 ).…”

Section: Methodsmentioning

confidence: 99%

Retinoic acid represses CYP7A1 expression in human hepatocytes and HepG2 cells by FXR/RXR-dependent and independent mechanisms

Cai

Nguyen

et al. 2010

Journal of Lipid Research

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Modulators of the structural dynamics of the retinoid X receptor to reveal receptor function

Cited by 135 publications

References 37 publications

Implications of the binding of tamoxifen to the coactivator recognition site of the estrogen receptor

Implications of the binding of tamoxifen to the coactivator recognition site of the estrogen receptor

Retinoid X Receptor-selective Signaling in the Regulation of Akt/Protein Kinase B Isoform-specific Expression

Retinoic acid represses CYP7A1 expression in human hepatocytes and HepG2 cells by FXR/RXR-dependent and independent mechanisms

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