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砷化合物的酶促甲基化。VI. 体外仓鼠肝脏亚砷酸盐和甲基胂酸甲基转移酶活性的表征

Enzymatic methylation of arsenic compounds. VI. Characterization of hamster liver arsenite and methylarsonic acid methyltransferase activities in vitro.

作者信息

Wildfang E, Zakharyan R A, Aposhian H V

机构信息

Department of Pharmacology and Toxicology, University of Arizona, Tucson 85721, USA.

出版信息

Toxicol Appl Pharmacol. 1998 Oct;152(2):366-75. doi: 10.1006/taap.1998.8409.

Abstract

Methylation of inorganic arsenic to methylarsonic acid (MMA) and dimethylarsinic acid (DMA) has been considered to be the major pathway of inorganic arsenic biotransformation and detoxification. Comparative studies, in vivo, have demonstrated variation in the abilities of animals to methylate inorganic arsenic. We propose that the rate of inorganic arsenite methylation may be one of the factors responsible for observed species variation. Arsenite and MMA methyltransferases of Golden Syrian hamster liver have been partially purified 40- and 67-fold, respectively. The monothiol L-cysteine promotes greater activities, in vitro, of these enzymes than similar concentrations of either glutathione or dithiothreitol. The pH optima of the partially purified arsenite and MMA methyltransferase activities are 7.6 and 8.0, respectively. Both activities display classic Michaelis-Menten enzyme kinetics. The K(m) and Vmax of hamster liver arsenite methyltransferase are 1.79 x 10(-6) M and 0.022 pmol/mg protein/60 min, respectively. Hamster liver MMA methyltransferase has K(m) and Vmax values of 7.98 x 10(-4) M and 0.007 pmol/mg protein/60 min, respectively. A similar kinetic relationship of these activities is also observed in the liver of the rabbit, which, like the hamster, excretes higher amounts of MMA than most other species studied. The higher K(m) and lower Vmax of MMA methyltransferase, compared to arsenite methyltransferase, measured in these two species suggests that MMA may be produced at a rate higher than it can be subsequently methylated to DMA, thereby allowing MMA to accumulate and be excreted.

摘要

无机砷甲基化生成甲基胂酸(MMA)和二甲基胂酸(DMA)被认为是无机砷生物转化和解毒的主要途径。体内比较研究表明,动物甲基化无机砷的能力存在差异。我们认为无机亚砷酸盐甲基化速率可能是导致观察到的物种差异的因素之一。金黄叙利亚仓鼠肝脏中的亚砷酸盐和MMA甲基转移酶已分别部分纯化了40倍和67倍。在体外,单硫醇L-半胱氨酸比相同浓度的谷胱甘肽或二硫苏糖醇更能促进这些酶的活性。部分纯化的亚砷酸盐和MMA甲基转移酶活性的最适pH分别为7.6和8.0。两种活性均显示出典型的米氏酶动力学。仓鼠肝脏亚砷酸盐甲基转移酶的K(m)和Vmax分别为1.79×10(-6) M和0.022 pmol/mg蛋白质/60分钟。仓鼠肝脏MMA甲基转移酶的K(m)和Vmax值分别为7.98×10(-4) M和0.007 pmol/mg蛋白质/60分钟。在兔子肝脏中也观察到了这些活性的类似动力学关系,兔子与仓鼠一样,排泄的MMA量比大多数其他研究物种都要高。在这两个物种中测得的MMA甲基转移酶与亚砷酸盐甲基转移酶相比,K(m)较高而Vmax较低,这表明MMA的产生速率可能高于其随后甲基化生成DMA的速率,从而使MMA得以积累并排泄。

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