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胆汁酸甾体核上的生物转化。

Biotransformations on steroid nucleus of bile acids.

作者信息

Bortolini O, Medici A, Poli S

机构信息

Dipartimento di Chimica, Universitá di Ferrara, Ferrara, Italy.

出版信息

Steroids. 1997 Aug-Sep;62(8-9):564-77. doi: 10.1016/s0039-128x(97)00043-3.

Abstract

The bile acids in mammals are all derivatives of 5 beta-cholan-26-oic acid. They represent the major quantitative pathway by which cholesterol is metabolized in the body. This article covers the microbial and enzymatic transformations of free, saturated bile acids, that kept unaltered the C-24 cyclopentane-perhydrophenantrene nucleus. The bile acids that have been considered include the primary cholic and chenodeoxycholic acids, the secondary deoxycholic and lithocholic acids as well as the relevant dehydrocholic, ursocholic and ursodeoxycholic acids. Among the bile acid biotransformations, attention is paid to reactions that lead to pharmaceutically significant compounds. This is the case of 7 alpha-hydroxy epimerization of chenodeoxycholic acid to ursodeoxycholic acid, currently used for cholesterol galistone dissolution therapy and in the treatment of cholestatic liver diseases. Emphasis has placed on reporting reactions that may be of general interest and on the practical aspects of work in the field of biotransformations.

摘要

哺乳动物体内的胆汁酸均为5β-胆烷-26-酸的衍生物。它们是胆固醇在体内代谢的主要定量途径。本文涵盖了游离饱和胆汁酸的微生物和酶促转化过程,这些转化过程未改变C-24环戊烷并全氢化菲核。所涉及的胆汁酸包括初级胆酸和鹅去氧胆酸、次级脱氧胆酸和石胆酸以及相关的脱氢胆酸、熊去氧胆酸和熊脱氧胆酸。在胆汁酸生物转化过程中,重点关注那些能生成具有药学意义化合物的反应。例如,鹅去氧胆酸的7α-羟基差向异构化生成熊去氧胆酸,目前该反应已用于胆固醇结石溶解治疗以及胆汁淤积性肝病的治疗。本文重点报道了可能具有普遍意义的反应以及生物转化领域工作的实际情况。

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