不同效应器对胆固醇- 7 -羟化酶的调节作用。

Z R Vlahcevic
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引用次数: 0

摘要

胆固醇降解为胆汁酸,占每天体内胆固醇总量的50%。胆固醇7 α -羟化酶和甾醇27-羟化酶分别催化中性和酸性途径的初始步骤。这两种酶最近都被克隆并测序,因此可以研究它们调控的分子基础。在大鼠体内,胆固醇7 α -羟化酶受三类效应分子调节:a)疏水(但不亲水)胆汁酸,b)胆固醇,c)激素(糖皮质激素加甲状腺素、胰高血糖素和胰岛素)。目前大多数研究表明,胆固醇7 α -羟化酶的调控可能发生在基因转录水平。甾醇27-羟化酶是一种线粒体P-450酶,似乎受到疏水胆汁酸的调节,但其程度低于胆固醇7-羟化酶。这种酸性途径对总胆汁酸合成的贡献尚不清楚,但它似乎比以前认为的更重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Regulation of cholesterol 7 alpha-hydroxylase by different effectors.

Cholesterol degradation to bile acids represents 50% of total elimination of cholesterol from the body each day. Cholesterol 7 alpha-hydroxylase and sterol 27-hydroxylase catalyze initial steps in the neutral and acidic pathways, respectively. Both enzymes were recently cloned and sequenced, and hence the molecular basis of their regulation could be studied. In the rat, cholesterol 7 alpha-hydroxylase is regulated by three classes of effector molecules: a) hydrophobic (but not hydrophilic) bile acids, b) cholesterol, and c) hormones (glucocorticoids plus thyroxine, glucagon and insulin). Most studies presented so far indicate that regulation of cholesterol 7 alpha-hydroxylase probably occurs at the level of gene transcription. Sterol 27-hydroxylase, a mitochondrial P-450 enzyme, appears to be regulated by hydrophobic bile acids, but to a lesser extent than cholesterol 7 alpha-hydroxylase. The contribution of this acidic pathway to total bile acid synthesis is not known but it appears to be more significant than previously thought.

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