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HYDROXYLATED POLYBROMINATED DIPHENYL ETHERS INTERRACT WITH THYROID HORMONE AND ESTROGEN RECEPTORS

机译:羟基化多溴二苯醚与甲状腺激素和雌激素受体相互作用

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摘要

The affinity for thyroid hormone receptor (TR) and estrogen receptor α (ER) of polybromodiphenyl ethers (PBDEs) and hydroxylated PBDEs was examined. 4-Hydroxy-2,2',3,4',5-pentabromodiphenyl ether and 3-hydroxy-2,2',4,4'-tetrabromodiphenyl ether markedly inhibited the binding of triiodothyronine (1×10-10 M) to TR in the concentration range of 1×10-6 - 1×10-4 M. 2,3,4,5,6-Pentabromophenol also showed an inhibitory effect at 1×10-5 - 1×10-4 M. However, 2,2',3,4,4',5'-hexabromodiphenyl ether, decabromodiphenyl ether, 4-methoxy-2,2',3,4',5-pentabromodiphenyl ether, 4-hydroxy-2,2',4',5 -tetrabromodiphenyl ether, 4-hydroxy-2,2',3,4'-tetrabromodiphenyl ether, 4'-hydroxy-2,2',4-tribromodiphenyl ether, 3'-hydroxy-2,4-dibromodiphenyl ether, 2,4,6-tribromophenol and tetrabromohydroquinone did not show affinity for TR. In contrast, 4'-hydroxy-2,2',4-tribromodiphenyl ether and 3'-hydroxy-2,4-dibromodiphenyl ether exhibited estrogenic activity in estrogen-responsive reporter assay using MCF-7 cells at the concentration of 1×10-5 M. However, adjacent bromo substitution of 3- or 4-hydroxylated PBDEs markedly decreased the estrogenic activity. These results suggest that hydroxylated PBDEs act as thyroid hormone-like agents, as well as estrogens.
机译:研究了聚溴二苯醚(PBDEs)和羟基化PBDEs对甲状腺激素受体(TR)和雌激素受体α(ER)的亲和力。 4-羟基-2,2',3,4',5-五溴二苯醚和3-羟基-2,2',4,4'-四溴二苯醚显着抑制三碘甲状腺素(1×10-10 M)与TR在1×10-6-1×10-4 M的浓度范围内。2,3,4,5,6-五溴酚在1×10-5-1×10-4 M处也显示出抑制作用。 ,2,2',3,4,4',5'-六溴二苯醚,十溴二苯醚,4-甲氧基-2,2',3,4',5-五溴二苯醚,4-羟基-2,2', 4',5-四溴二苯醚,4-羟基-2,2',3,4'-四溴二苯醚,4'-羟基-2,2',4-三溴二苯醚,3'-羟基-2,4-二溴二苯醚醚,2,4,6-三溴苯酚和四溴对苯二酚对TR没有亲和力。相比之下,在使用MCF-7细胞以1×10的浓度进行雌激素反应性报告基因分析中,4'-羟基-2,2',4-三溴二苯醚和3'-羟基-2,4-二溴二苯醚表现出雌激素活性。 -5M。但是,相邻的3-或4-羟基化PBDE溴取代明显降低了雌激素活性。这些结果表明,羟基化的多溴二苯醚可作为甲状腺激素样药物以及雌激素。

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  • 会议地点 Beijing(CN)
  • 作者单位

    Graduate School of Biomedical Sciences,Hiroshima University,Kasumi 1-2-3,Minami-ku,Hiroshima 734-8553,Japan Nihon Pharmaceutical University,Komuro 10281,Ina-machi,Saitama 362-0806,Japan;

    Graduate School of Biomedical Sciences,Hiroshima University,Kasumi 1-2-3,Minami-ku,Hiroshima 734-8553,Japan Faculty of Pharmaceutical Sciences,Hiroshima International University,Kure,Hiroshima 737-0112,Japan;

    Graduate School of Biomedical Sciences,Hiroshima University,Kasumi 1-2-3,Minami-ku,Hiroshima 734-8553,Japan;

    Graduate School of Biomedical Sciences,Hiroshima University,Kasumi 1-2-3,Minami-ku,Hiroshima 734-8553,Japan;

    Graduate School of Biomedical Sciences,Hiroshima University,Kasumi 1-2-3,Minami-ku,Hiroshima 734-8553,Japan Nihon Pharmaceutical University,Komuro 10281,Ina-machi,Saitama 362-0806,Japan;

    Niho;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 环境分析化学;
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