Structural basis for a molecular allosteric control mechanism of cofactor binding to nuclear receptors

Ősz, Judit; Brélivet, Yann; Peluso‐Iltis, Carole; Cura, Vincent; Eiler, Sylvia; Ruff, Marc; Bourguet, William; Rochel, Natacha; Moras, Dino

doi:10.1073/pnas.1118192109

Cited by 78 publications

(86 citation statements)

References 41 publications

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“…3 D and E). The observation that two distinct orientations of BPAF are found in each monomer rather than occurring randomly is intriguing and suggests the existence of a regulatory crosstalk between the two subunits whereby, as recently reported, ligand and/or coregulator binding to one monomer can affect ligand and coregulator binding to the second monomer of a dimer (37). However, such a situation is not observed in the E 2 or BPA complexes, which yet crystallize in the same crystal form as with BPAF and are therefore engaged in similar packing contacts.…”

Section: Resultsmentioning

confidence: 98%

Structural and mechanistic insights into bisphenols action provide guidelines for risk assessment and discovery of bisphenol A substitutes

Delfosse

Grimaldi

Pons

et al. 2012

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

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326

268

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Bisphenol A (BPA) is an industrial compound and a well known endocrine-disrupting chemical with estrogenic activity. The widespread exposure of individuals to BPA is suspected to affect a variety of physiological functions, including reproduction, development, and metabolism. Here we report that the mechanisms by which BPA and two congeners, bisphenol AF and bisphenol C (BPC), bind to and activate estrogen receptors (ER) α and β differ from that used by 17β-estradiol. We show that bisphenols act as partial agonists of ERs by activating the N-terminal activation function 1 regardless of their effect on the C-terminal activation function 2, which ranges from weak agonism (with BPA) to antagonism (with BPC). Crystallographic analysis of the interaction between bisphenols and ERs reveals two discrete binding modes, reflecting the different activities of compounds on ERs. BPA and 17β-estradiol bind to ERs in a similar fashion, whereas, with a phenol ring pointing toward the activation helix H12, the orientation of BPC accounts for the marked antagonist character of this compound. Based on structural data, we developed a protocol for in silico evaluation of the interaction between bisphenols and ERs or other members of the nuclear hormone receptor family, such as estrogen-related receptor γ and androgen receptor, which are two known main targets of bisphenols. Overall, this study provides a wealth of tools and information that could be used for the development of BPA substitutes devoid of nuclear hormone receptor-mediated activity and more generally for environmental risk assessment.crystal structure | endocrine disruptor | nuclear receptor | virtual screening

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Section: Resultsmentioning

confidence: 98%

Structural and mechanistic insights into bisphenols action provide guidelines for risk assessment and discovery of bisphenol A substitutes

Delfosse

Grimaldi

Pons

et al. 2012

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

Self Cite

326

268

View full text Add to dashboard Cite

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“…3B ). According to recent studies ( 87,97 ), only one coactivator molecule is recruited by the heterodimer through the RAR partner, and the architecture of the DNA-bound receptor complexes orients the coactivator on one side of the DNA opposite to the RXR LBD and DBD so that it can reach its targets, the histone tails. This raises the question how the RXR partner participates in the transcriptional activity of the heterodimers in addition to increasing DNA binding effi ciency ( 98 ).…”

Section: The End Of Transcriptionmentioning

confidence: 99%

Vitamin A and retinoid signaling: genomic and nongenomic effects

Tanoury

Piskunov

Rochette‐Egly

2013

Journal of Lipid Research

329

257

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“…Estrogens have been shown to play an important role in human breast cancer development and ~1/3 of breast cancers are stimulated by estradiol (49). Estrogens exert their effects through the action of the estrogen receptors α and β (ERα and ERβ), which belong to the steroid hormone superfamily of nuclear receptors (NRs) (50,51). ERs are members of the large NR family of transcription factors that are typically activated upon binding to small lipophilic molecules (52).…”

Section: Luminal a Subtype Breast Cancer Therapeutic Potentialsmentioning

confidence: 99%

Estrogen receptor-positive breast cancer molecular signatures and therapeutic potentials (Review)

et al. 2013

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Abstract. In this review, the advances in the study of breast cancer molecular classifications and the molecular signatures of the luminal subtypes A and B of breast cancer were summarized. Effective clinical outcomes depend mainly on successful preclinical diagnosis and therapeutic decisions. Over the last few years, the ever-expanding investigations focusing on breast cancer diagnosis and the clinical trials have provided accumulating information on the molecular characteristics of breast cancer. Specifically, among the estrogen receptor (ER)-positive types of breast cancer, the luminal subtype A breast cancer has been shown to exhibit good clinical outcomes with endocrine therapy, whereas the luminal subtype B breast cancer represents the more complicated type, diagnostically as well as therapeutically. Furthermore, even in luminal subtype A breast cancer, the resistance to treatment has become the major limitation for endocrine-based therapy. Accumulating molecular data and further clinical trials may enable more accurate diagnostic and therapeutic decisions. The molecular signatures have emerged as a powerful tool for future diagnosis and therapeutic decisions, although currently available data are limited.

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Structural basis for a molecular allosteric control mechanism of cofactor binding to nuclear receptors

Cited by 78 publications

References 41 publications

Structural and mechanistic insights into bisphenols action provide guidelines for risk assessment and discovery of bisphenol A substitutes

Structural and mechanistic insights into bisphenols action provide guidelines for risk assessment and discovery of bisphenol A substitutes

Vitamin A and retinoid signaling: genomic and nongenomic effects

Estrogen receptor-positive breast cancer molecular signatures and therapeutic potentials (Review)

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