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重组人磺基转移酶(SULT)1A1基因变体和SULT1E1对膳食多酚的可变硫酸化作用。

Variable sulfation of dietary polyphenols by recombinant human sulfotransferase (SULT) 1A1 genetic variants and SULT1E1.

作者信息

Ung Din, Nagar Swati

机构信息

Department of Pharmaceutical Sciences, Temple University School of Pharmacy, 3307 North Broad St., Philadelphia, PA 19140, USA.

出版信息

Drug Metab Dispos. 2007 May;35(5):740-6. doi: 10.1124/dmd.106.013987. Epub 2007 Feb 9.

DOI:10.1124/dmd.106.013987
PMID:17293380
Abstract

Human cytosolic sulfotransferases (SULTs) catalyze the sulfate conjugation of several important endo- and xenobiotics. Among the superfamily of SULT enzymes, SULT1A1 catalyzes the sulfation of small planar phenolic compounds, whereas SULT1E1 has a major role in estrogen conjugation. The human SULT1A1 gene has common single nucleotide polymorphisms that define three allozymes, SULT1A11, 2, and 3. The enzyme kinetics of SULT1A1 allozymes and SULT1E1 were characterized for the polyphenolic substrates apigenin, chrysin, epicatechin, quercetin, and resveratrol. Purified recombinant SULT proteins were generated in a baculoviral-insect cell system, and incubated in vitro with each substrate to determine catalytic activity. The effect of polyphenol sulfation was examined in mammalian cell lines stably expressing SULT1E1. For all polyphenols investigated, "normal-activity" SULT1A11 allozyme had significantly greater Vmax estimates than SULT1E1, and allele-specific differences in SULT1A1-mediated sulfation were observed. The polymorphic SULT1A12 allozyme exhibited low activity toward apigenin, epicatechin, and resveratrol. SULT1A11 and *3 acted as normal-activity allozymes for these substrates. Altered cellular proliferation was observed in MCF-7 cells stably expressing SULT1E1 upon treatment with chrysin, quercetin, or resveratrol, thus suggesting inactivation of these compounds by SULT1E1. These results suggest an important role for SULT isozymes and their pharmacogenetics in polyphenol disposition.

摘要

人胞质磺基转移酶(SULTs)催化多种重要内源性和外源性物质的硫酸化结合反应。在SULT酶超家族中,SULT1A1催化小分子平面酚类化合物的硫酸化,而SULT1E1在雌激素结合反应中起主要作用。人类SULT1A1基因存在常见的单核苷酸多态性,可定义三种同工酶,即SULT1A11、2和3。针对多酚类底物芹菜素、白杨素、表儿茶素、槲皮素和白藜芦醇,对SULT1A1同工酶和SULT1E1的酶动力学进行了表征。在杆状病毒-昆虫细胞系统中产生纯化的重组SULT蛋白,并在体外与每种底物孵育以确定催化活性。在稳定表达SULT1E1的哺乳动物细胞系中检测了多酚硫酸化的作用。对于所有研究的多酚,“正常活性”的SULT1A11同工酶的Vmax估计值显著高于SULT1E1,并且观察到SULT1A1介导的硫酸化存在等位基因特异性差异。多态性的SULT1A12同工酶对芹菜素、表儿茶素和白藜芦醇表现出低活性。SULT1A11和*3对这些底物起正常活性同工酶的作用。在用白杨素、槲皮素或白藜芦醇处理后,在稳定表达SULT1E1的MCF-7细胞中观察到细胞增殖改变,这表明这些化合物被SULT1E1失活。这些结果表明SULT同工酶及其药物遗传学在多酚代谢中起重要作用。

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