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莫里斯肝癌中的微粒体单加氧酶系统:来自经3-甲基胆蒽处理大鼠的莫里斯肝癌5123D细胞色素P-450的纯化与特性分析

Microsomal monooxygenase system in Morris hepatoma: purification and characterization of cytochromes P-450 from Morris hepatoma 5123D of 3-methylcholanthrene-treated rats.

作者信息

Ohmachi T, Sagami I, Fujii H, Watanabe M

出版信息

Arch Biochem Biophys. 1985 Jan;236(1):176-84. doi: 10.1016/0003-9861(85)90617-4.

Abstract

Two forms of cytochrome P-450 (hepatoma P-450MCI and P-450MCII) were purified from hepatoma 5123D microsomes of tumor-bearing rats treated with 3-methylcholanthrene. Hepatoma P-450MCI had a specific content of 18.4 nmol/mg protein and showed a main protein band with a minimum molecular weight of 56,000 on sodium dodecyl sulfate-polyacrylamide gel. Hepatoma P-450MCII had a specific content of 7.38 nmol/mg protein and a minimum molecular weight of 50,000. The carbon monoxide-reduced difference spectral peak of hepatoma P-450MCI was at 446.5 nm, whereas the peak of hepatoma P-450MCII was at 451 nm. In the reconstituted system, hepatoma P-450MCI catalyzed 3-hydroxylation of benzo[a]pyrene and O-deethylation of 7-ethoxycoumarin, but showed low activities for N-demethylation of benzphetamine and aminopyrine, O-demethylation of p-nitroanisole, and p-hydroxylation of aniline. On the other hand, hepatoma P-450MCII did not catalyze hydroxylation of any of the substrates tested. By Ouchterlony double-diffusion analysis, hepatoma P-450MCI was immunologically indistinguishable from rat liver cytochrome P-450c, but hepatoma P-450MCII was distinct from hepatoma P-450MCI and rat liver cytochrome P-450c. Peptide maps of hepatoma P-450MCI and rat liver cytochrome P-450c after proteolysis with Staphylococcus aureus V8 protease demonstrated the similarity of the two cytochromes P-450.

摘要

从经3-甲基胆蒽处理的荷瘤大鼠的肝癌5123D微粒体中纯化出两种形式的细胞色素P-450(肝癌P-450MCI和P-450MCII)。肝癌P-450MCI的比含量为18.4 nmol/mg蛋白质,在十二烷基硫酸钠-聚丙烯酰胺凝胶上显示出一条最小分子量为56,000的主要蛋白带。肝癌P-450MCII的比含量为7.38 nmol/mg蛋白质,最小分子量为50,000。肝癌P-450MCI的一氧化碳还原差光谱峰位于446.5 nm,而肝癌P-450MCII的峰位于451 nm。在重组系统中,肝癌P-450MCI催化苯并[a]芘的3-羟基化和7-乙氧基香豆素的O-脱乙基化,但对苄非他明和氨基比林的N-脱甲基化、对硝基苯甲醚的O-脱甲基化以及苯胺的p-羟基化活性较低。另一方面,肝癌P-450MCII不催化所测试的任何底物的羟基化。通过奥克特洛尼双向扩散分析,肝癌P-450MCI与大鼠肝细胞色素P-450c在免疫上无法区分,但肝癌P-450MCII与肝癌P-450MCI和大鼠肝细胞色素P-450c不同。用金黄色葡萄球菌V8蛋白酶进行蛋白水解后,肝癌P-450MCI和大鼠肝细胞色素P-450c的肽图显示了这两种细胞色素P-450的相似性。

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