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细胞色素P450活性与克拉拉细胞细胞毒性的关系。II. 小鼠、仓鼠、大鼠和恒河猴肺和鼻黏膜中萘环氧化立体选择性的比较。

Relationship of cytochrome P450 activity to Clara cell cytotoxicity. II. Comparison of stereoselectivity of naphthalene epoxidation in lung and nasal mucosa of mouse, hamster, rat and rhesus monkey.

作者信息

Buckpitt A, Buonarati M, Avey L B, Chang A M, Morin D, Plopper C G

机构信息

Department of Pharmacology, School of Medicine, University of California, Davis.

出版信息

J Pharmacol Exp Ther. 1992 Apr;261(1):364-72.

PMID:1560380
Abstract

Naphthalene, a murine Clara cell cytotoxicant, is metabolized by cytochrome P450 monooxygenases to unstable, chiral epoxide metabolites which can conjugate with glutathione in the presence of glutathione transferases. Analysis of the three diasteriomeric glutathione adducts produced from conjugation of naphthalene oxides was used in these studies to characterize the stereochemistry of naphthalene epoxidation in preparations of nasal mucosa, lung and liver of the mouse, rat, hamster and monkey. The highest rates of naphthalene metabolism were observed in mouse lung and liver microsomal incubations. Rat, hamster and monkey lung microsomal preparations metabolized naphthalene at 12, 37, and 1%, respectively, of the rate observed in mouse lung. The ratio of chiral epoxides produced in microsomal incubations was dependent upon the concentration of naphthalene. At high substrate concentrations (0.25-1.0 mM), the ratio of 1R,2S- to 1S,2R-naphthalene oxide, as assessed by the glutathione adducts generated (adduct 2/adducts 1 + 3), in murine lung microsomal incubations was 10:1 and at low concentrations (0.062 mM and below) varied from 13.8:1 to 30:1. In contrast, the ratio of 1R,2S- to 1S,2R-naphthalene oxide produced in murine liver microsomes varied from 1:1 at high substrate concentrations to 5:1 at low substrate concentrations. The ratio of naphthalene oxides was unaffected by the concentration of glutathione in the incubation. In contrast to the preferential formation of 1R,2S-naphthalene oxide observed in mouse lung microsomal preparations, lung microsomes derived from the rat, hamster and monkey yielded 1R,2S- to 1S,2R-epoxide ratios of 0.48, 0.61 and 0.12, respectively, at 0.5 mM naphthalene.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

萘是一种对小鼠克拉拉细胞具有细胞毒性的物质,它被细胞色素P450单加氧酶代谢为不稳定的手性环氧化物代谢产物,这些代谢产物在谷胱甘肽转移酶存在的情况下可与谷胱甘肽结合。在这些研究中,通过分析萘氧化物结合产生的三种非对映体谷胱甘肽加合物,来表征小鼠、大鼠、仓鼠和猴子的鼻黏膜、肺和肝制剂中萘环氧化的立体化学。在小鼠肺和肝微粒体孵育中观察到萘代谢的最高速率。大鼠、仓鼠和猴子的肺微粒体制剂代谢萘的速率分别为小鼠肺中观察到速率的12%、37%和1%。微粒体孵育中产生的手性环氧化物的比例取决于萘的浓度。在高底物浓度(0.25 - 1.0 mM)下,通过产生的谷胱甘肽加合物评估(加合物2/加合物1 + 3),小鼠肺微粒体孵育中1R,2S - 与1S,2R - 萘氧化物的比例为10:1,在低浓度(0.062 mM及以下)时从13.8:1变化到30:1。相比之下,小鼠肝微粒体中产生的1R,2S - 与1S,2R - 萘氧化物的比例在高底物浓度下为1:1,在低底物浓度下为5:1。萘氧化物的比例不受孵育中谷胱甘肽浓度的影响。与在小鼠肺微粒体制剂中观察到的优先形成1R,2S - 萘氧化物相反,在0.5 mM萘时,来自大鼠、仓鼠和猴子的肺微粒体产生的1R,2S - 与1S,2R - 环氧化物的比例分别为0.48、0.61和0.12。(摘要截断于250字)

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