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人胞质硫酸转移酶的差异性异源雌激素硫酸化活性:人SULT2B1a和SULT2B1b硫酸转移酶的分子克隆、表达及纯化

Differential xenoestrogen-sulfating activities of the human cytosolic sulfotransferases: molecular cloning, expression, and purification of human SULT2B1a and SULT2B1b sulfotransferases.

作者信息

Pai T Govind, Sugahara Takuya, Suiko Masahito, Sakakibara Yoichi, Xu Faye, Liu Ming-Cheh

机构信息

Department of Biochemistry, Biomedical Research Center, The University of Texas Health Center at Tyler, 11937 US HWY 271, Tyler, TX 75708, USA.

出版信息

Biochim Biophys Acta. 2002 Nov 14;1573(2):165-70. doi: 10.1016/s0304-4165(02)00416-6.

DOI:10.1016/s0304-4165(02)00416-6
PMID:12399026
Abstract

Environmental xenoestrogens have been implicated in human reproductive disorders and an increased incidence of breast cancer. Sulfation, a Phase II detoxification mechanism involving the cytosolic sulfotransferases (STs), may be an important mechanism in vivo for fending off these compounds. In this study, we report on the molecular cloning, expression, and purification of two human cytosolic STs, SULT2B1a and SULT2b1b. The activities of these two enzymes, as well as the other eight known human cytosolic STs previously prepared, toward representative environmental xenoestrogens were examined. Activity data showed that P-form (SULT1A1) PST displayed the highest activity toward these compounds, while SULT1C ST #2 also showed considerable activity, indicating that these enzymes may play a more important role in detoxification of environmental xenoestrogens. SULT1C ST #1, SULT2B1a ST, SULT2B1b ST and NST showed negligible or undetectable activity toward these compounds. The other four enzymes, M-form (SULT1A3) PST, SULT1B2 ST, SULT2A1 ST and SULT1E ST showed intermediate levels of activity toward some of these compounds. Kinetic studies on the sulfation of xenoestrogens by P-form (SULT1A1) PST were performed. The results are interpreted in the context of the endocrine-disrupting nature of these xenoestrogens.

摘要

环境中的外源性雌激素已被认为与人类生殖紊乱及乳腺癌发病率上升有关。硫酸化作用是一种涉及胞质磺基转移酶(STs)的Ⅱ相解毒机制,可能是体内抵御这些化合物的重要机制。在本研究中,我们报道了两种人类胞质STs,即SULT2B1a和SULT2B1b的分子克隆、表达及纯化。检测了这两种酶以及先前制备的其他八种已知人类胞质STs对代表性环境外源性雌激素的活性。活性数据表明,P型(SULT1A1)PST对这些化合物表现出最高活性,而SULT1C ST #2也显示出相当的活性,这表明这些酶可能在环境外源性雌激素的解毒中发挥更重要的作用。SULT1C ST #1、SULT2B1a ST、SULT2B1b ST和NST对这些化合物的活性可忽略不计或无法检测到。其他四种酶,即M型(SULT1A3)PST、SULT1B2 ST、SULT2A1 ST和SULT1E ST对其中一些化合物表现出中等水平的活性。对P型(SULT1A1)PST催化外源性雌激素硫酸化进行了动力学研究。根据这些外源性雌激素的内分泌干扰特性对结果进行了解释。

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