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抗甲状腺药物与碘的相互作用:两种源自硒代甲巯咪唑的特殊离子化合物的分离。

Interaction of anti-thyroid drugs with iodine: the isolation of two unusual ionic compounds derived from Se-methimazole.

作者信息

Roy Gouriprasanna, Nethaji Munirathinam, Mugesh G

机构信息

Department of Inorganic & Physical Chemistry, Indian Institute of Science, Bangalore.

出版信息

Org Biomol Chem. 2006 Aug 7;4(15):2883-7. doi: 10.1039/b604060h. Epub 2006 Jun 30.

Abstract

The inhibition of lactoperoxidase (LPO)-catalyzed iodination of l-tyrosine by the anti-thyroid drug methimazole (MMI) and its selenium analogue (MSeI) is described. MSeI inhibits LPO with an IC(50) value of 12.4 microM, and this inhibition could be completely reversed by increasing the peroxide concentration. In addition to the inhibition, MSeI reacts with molecular iodine to produce novel ionic diselenides, and the nature of the species formed in this reaction appear to be solvent-dependent. The formation of ionic species in the reaction is confirmed by single-crystal X-ray studies, FT-IR and FT-Raman spectroscopic investigations. This study provides the first experimental evidence that MSeI not only effectively inhibits the LPO-catalyzed iodination of tyrosine, but also reacts with I(2) to produce novel ionic diselenides. These results also suggest that MSeI reacts with iodine, even in its oxidized form, to form ionic diselenides containing iodide or polyiodide anions, which might be effective intermediates in the inhibition of thyroid hormones.

摘要

本文描述了抗甲状腺药物甲巯咪唑(MMI)及其硒类似物(MSeI)对乳过氧化物酶(LPO)催化的L-酪氨酸碘化反应的抑制作用。MSeI对LPO的抑制中半数抑制浓度(IC50)值为12.4微摩尔,并且通过增加过氧化物浓度可使这种抑制作用完全逆转。除抑制作用外,MSeI还与分子碘反应生成新型离子二硒化物,该反应中形成的物种性质似乎取决于溶剂。通过单晶X射线研究、傅里叶变换红外光谱(FT-IR)和傅里叶变换拉曼光谱(FT-Raman)研究证实了反应中离子物种的形成。本研究提供了首个实验证据,表明MSeI不仅能有效抑制LPO催化的酪氨酸碘化反应,还能与I2反应生成新型离子二硒化物。这些结果还表明,MSeI即使与氧化态的碘反应,也会形成含有碘离子或多碘离子阴离子的离子二硒化物,这可能是抑制甲状腺激素的有效中间体。

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