Novel Metabolic Pathways of p-n-Nonylphenol Catalyzed by Cytochrome P450 and Estrogen Receptor Binding Activity of New Metabolites
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概要
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Nonylphenol, which is used industrially as a surfactant, is an endocrine-disrupting chemical (EDC) which has estrogenic activity. The novel biotransformation of nonylphenol was investigated, based on our previously reported ipso-metabolism of para-substituted phenols by cytochrome P450 (P450). Three novel metabolites of nonylphenol, i.e., nonylquinol, 4'-hydroxynonanophenone (CO-NP) as benzyl-oxidized nonylphenol, and hydroquinone, were detected in a rat liver microsome reaction mixture. On the other hand, production of 1-(4'-hydroxyphenyl)nonan-1-ol (OH-NP), namely benzyl-hydroxylated nonylphenol, was detected in a human liver microsome reaction mixture. The formation of all these metabolites was suppressed by the addition of P450 inhibitor. This showed that all nonylphenol metabolism was catalyzed by P450. To identify which P450 isoenzyme is involved in each reaction, fourteen human P450 (CYP) isozymes, CYP1A1, 1A2, 2A6, 2B6, 2C8, 2C9, 2C18, 2C19, 2D6, 2E1, 3A4, 3A5, 3A7, and CYP4A11, were examined. CYP1A1, 1A2, and CYP2B6 effectively catalyzed the production of nonylquinol. CYP2B6 also catalyzed the benzyl-hydroxylation to give OH-NP. Hydroquinone was formed mainly from OH-NP, not via CO-NP. We examined the estrogenic activity of these new metabolites by estrogen receptor (ER)-binding reporter gene assay. Nonylquinol, OH-NP and hydroquinone have no ER-binding activity. However, CO-NP showed the same level of estrogen receptor binding activity as nonylphenol. Moreover, the amount of CO-NP formed was small. Therefore, the novel metabolic pathways led overall to metabolic inactivation, as concerns the estrogenic activity of nonylphenol through the ER.
- 公益社団法人日本薬学会の論文
- 2007-10-01
著者
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OHTA Shigeru
Graduate School of Biomedical Sciences, Hiroshima University
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Shigeyuki Kitamura
Nihon Pharmaceutical University
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Kitamura Shigeyuki
広島大学 医学部総合薬学科生体機能分子動態学
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Kitamura Shigeyuki
広島大学 総合薬
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Kitamura Shigeyuki
広島大学原爆放射能医学研究所
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KITAMURA Shigeyuki
Graduate School of Biomedical Science, Hiroshima University
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MASHINO Tadahiko
Kyoritsu University of Pharmacy
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Sugihara K
Graduate School Of Biomedical Sciences Hiroshima University
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Suzuki T
Departments Of Analytical Biochemistry Meiji Pharmaceutical University
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Suzuki T
Department Of Xenobiotic Metabolism And Molecular Toxicology Institute Of Pharmaceutical Sciences Hi
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Suzuki Tomoharu
Graduate School of Biomedical Sciences, Hiroshima University
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Tezuka Yoshito
Kyoritsu University of Pharmacy
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Takahashi Kyoko
Kyoritsu University of Pharmacy
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Nakamura Shigeo
Kyoritsu University of Pharmacy
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Ohta S
Graduate School Of Biomedical Sciences Hiroshima University
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Mashino Tadahiko
Kyoritsu College Of Pharmacy
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Kitamura Shigeyuki
Institute Of Pharmaceutical Science. Hiroshima University School Of Medicine
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Tsujino Seiichi
Department Of Peripheral Nervous System Research National Institute Of Neuroscience Ncnp
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Nakamura Shigeo
Dep. Of Pharmaceutical Sciences Fac. Of Pharmacy Keio Univ.
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Mashino Tadahiko
Dep. Of Pharmaceutical Sciences Fac. Of Pharmacy Keio Univ.
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Ohta Shigeru
Graduate School Of Biomedical Sciences Hiroshima Univ.
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Kitamura Shigeyuki
Graduate School Of Bioagricultural Sciences Nagoya University
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TAKAHASHI KYOKO
Kyoritsu College of Pharmacy
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