Makoto Nakai scite author profile

Octyl-and nonylphenols in the environment have been proposed to function as estrogens. To gain insight into their structural essentials in binding to the estrogen receptor, a series of phenols with saturated alkyl groups at the para position, HO-C 6 H 4 -C n H 2n+1 (n = 0±12), were examined for their ability to displace [ 3 H]17b-estradiol in the recombinant human estrogen receptor, which was expressed in Sf9 cells using the vaculovirus expression system. All tested para-alkylphenols were found to bind fully to the estrogen receptors in a dose-dependent manner. The interaction of alkylphenols with the receptor became stronger with increase in the number of the alkyl carbons and the activity was maximized with n = 9 of nonylphenol. Phenol (n = 0) exhibited weak but full binding to the receptor, whereas anisole with a protected phenolic hydroxyl group was completely inactive. Also, alkanes such as n-octane, 2,2,4-trimethylpentane corresponding to tert-octane, and n-nonane exhibited no binding. The results indicate that the binding of para-alkylphenols to the estrogen receptor is due to the effect of covalent bonding of two constituents of the phenol and alkyl groups, which correspond to the A-ring and hydrophobic moiety of the steroid structure, respectively. When alkylphenols were examined for their receptor binding conformation by 1 H-NMR measurements and ab initio molecular orbital calculations, it was suggested that nonbranched alkyl groups are in an extended conformation, while branched alkyl groups are in a folded conformation. These results suggest that branched and nonbranched alkyl moieties of alkylphenols interact differently with the lipophilic ligand binding cavity of the estrogen receptor when compared to the binding of 17b-estradiol.

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Screening for androgen receptor activities in 253 industrial chemicals by in vitro reporter gene assays using AR-EcoScreenTM cells

Araki¹,

Ohno²,

Nakai³

et al. 2005

Toxicology in Vitro

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Analysis of clinical variables of donors and recipients with respect to short-term graft outcome in human liver transplantation

Totsuka

Fung

Hakamada

et al. 2004

Transplantation Proceedings

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Relationship between the results of in vitro receptor binding assay to human estrogen receptor α and in vivo uterotrophic assay: Comparative study with 65 selected chemicals

Akahori

Nakai

Yamasaki

et al. 2008

Toxicology in Vitro

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Makoto Nakai

Accelerated evolution in the protein-coding regions is universal in crotalinae snake venom gland phospholipase A2 isozyme genes.

Structural requirements of para‐alkylphenols to bind to estrogen receptor

Screening for androgen receptor activities in 253 industrial chemicals by in vitro reporter gene assays using AR-EcoScreenTM cells

Analysis of clinical variables of donors and recipients with respect to short-term graft outcome in human liver transplantation

Relationship between the results of in vitro receptor binding assay to human estrogen receptor α and in vivo uterotrophic assay: Comparative study with 65 selected chemicals

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