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细胞色素P-450的不同形式负责胆汁酸和中性类固醇的6β-羟基化。

Distinct forms of cytochrome P-450 are responsible for 6 beta-hydroxylation of bile acids and of neutral steroids.

作者信息

Zimniak P, Holsztynska E J, Radominska A, Iscan M, Lester R, Waxman D J

机构信息

Department of Internal Medicine, University of Arkansas for Medical Sciences, Little Rock 72205.

出版信息

Biochem J. 1991 Apr 1;275 ( Pt 1)(Pt 1):105-11. doi: 10.1042/bj2750105.

Abstract

Cytochrome P-450-dependent 6 beta-hydroxylation of bile acids in rat liver contributes to the synthesis of the quantitatively important pool of 6-hydroxylated bile acids, as well as to the detoxification of hydrophobic bile acids. The lithocholic acid 6 beta-hydroxylation reaction was investigated and compared with androstenedione 6 beta-hydroxylation. Differential responses of these two activities to inducers and inhibitors of microsomal P-450 enzymes, lack of mutual inhibition by the two substrates and differential inhibition by antibodies raised against several purified hepatic cytochromes P-450 were observed. From these results it was concluded that 6 beta-hydroxylation of lithocholic acid is catalysed by P-450 form(s) different from the subfamily IIIA cytochromes P-450 which are responsible for the bulk of microsomal androstenedione 6 beta-hydroxylation. Similar, but more tentative, results revealed that the 7 alpha-hydroxylation of lithocholic acid and of androstenedione may be also catalysed by distinct P-450 enzymes. The results indicate that cytochromes P-450 hydroxylating bile acids are distinct from analogous enzymes that carry out reactions of the same regio- and stereo-specificity on neutral steroids (steroid hormones). A comparison of pairs of cytochromes P-450 that catalyse the same reaction on closely related steroid molecules will help to define those structural elements in the proteins that determine the recognition of their respective substrates.

摘要

大鼠肝脏中细胞色素P - 450依赖性胆汁酸6β-羟基化作用,不仅有助于合成数量上占重要比例的6-羟基化胆汁酸库,还参与疏水性胆汁酸的解毒过程。研究了石胆酸6β-羟基化反应,并与雄烯二酮6β-羟基化反应进行了比较。观察到这两种活性对微粒体P - 450酶诱导剂和抑制剂的不同反应、两种底物之间不存在相互抑制以及针对几种纯化的肝细胞色素P - 450产生的抗体的不同抑制作用。从这些结果得出结论,石胆酸的6β-羟基化是由不同于细胞色素P - 450亚家族IIIA的P - 450形式催化的,后者负责大部分微粒体雄烯二酮的6β-羟基化。类似但更具试探性的结果表明,石胆酸和雄烯二酮的7α-羟基化也可能由不同的P - 450酶催化。结果表明,使胆汁酸羟基化的细胞色素P -

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Stero-bile sterols. 39. Metabolism of lithocholic acid.甾体胆汁甾醇。39. 石胆酸的代谢。
J Biochem. 1961 Jul;50:20-3. doi: 10.1093/oxfordjournals.jbchem.a127402.
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