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大鼠睾丸微粒体由孕酮生成睾酮,且不释放中间产物17α-羟孕酮和雄烯二酮。

Production of testosterone from progesterone by rat testicular microsomes without release of the intermediates 17 alpha-hydroxyprogesterone and androstenedione.

作者信息

Eckstein B, Borut A, Cohen S

出版信息

Eur J Biochem. 1987 Jul 15;166(2):425-9. doi: 10.1111/j.1432-1033.1987.tb13533.x.

Abstract

It has been shown that during the in vitro conversion of progesterone to androstenedione, 17 alpha-hydroxyprogesterone is not an obligatory intermediate which equilibrates with freely diffusible steroids in the incubation medium. Recently a cytochrome P-450 was purified that catalyzed, in addition to hydroxylase/lyase activities, reduction of androstenedione to testosterone. In order to determine whether progesterone could be transformed to testosterone without both intermediates (17 alpha-hydroxyprogesterone and androstenedione) being equilibrated with steroids in the medium, several double-label double-substrate experiments were performed. When rat microsomes were incubated with an equimolar mixture of [14C]progesterone and 17 alpha-hydroxy[3H]progesterone, androstenedione was isolated with a 11-fold higher 14C/3H ratio than 17 alpha-hydroxyprogesterone, indicating that androstenedione could not be produced from free, diffusible 17 alpha-hydroxyprogesterone. Incubation of an equimolar mixture of 17 alpha-hydroxy[3H]progesterone and [14C]androstenedione with testicular microsomes resulted in the incorporation of 3-4-fold more 17 alpha-hydroxyprogesterone into testosterone than of androstenedione, although the latter is the immediate precursor of testosterone. In an experiment in which equimolar concentrations of [3H]progesterone and [14C]androstenedione were incubated with testicular microsomes, the large pool of progesterone inhibited competitively lyase activity, but still the label of progesterone was incorporated into testosterone to the same extent as that of androstenedione. These results indicate that testosterone can be produced by immature rat testicular microsomes from added progesterone on an organized unit without the intermediates equilibrating with the incubation medium.

摘要

已表明,在孕酮体外转化为雄烯二酮的过程中,17α-羟孕酮并非与孵育介质中可自由扩散的类固醇达到平衡的必需中间体。最近纯化了一种细胞色素P - 450,它除了具有羟化酶/裂解酶活性外,还能催化雄烯二酮还原为睾酮。为了确定孕酮是否可以在没有这两种中间体(17α-羟孕酮和雄烯二酮)与介质中的类固醇达到平衡的情况下转化为睾酮,进行了几个双标记双底物实验。当大鼠微粒体与[14C]孕酮和17α-羟基[3H]孕酮的等摩尔混合物一起孵育时,分离出的雄烯二酮的14C/3H比值比17α-羟孕酮高11倍,这表明雄烯二酮不是由游离的、可扩散的17α-羟孕酮产生的。将17α-羟基[3H]孕酮和[14C]雄烯二酮的等摩尔混合物与睾丸微粒体一起孵育,结果显示,尽管雄烯二酮是睾酮的直接前体,但17α-羟孕酮转化为睾酮的量比雄烯二酮多3 - 4倍。在一个实验中,将等摩尔浓度的[3H]孕酮和[14C]雄烯二酮与睾丸微粒体一起孵育,大量的孕酮竞争性抑制裂解酶活性,但孕酮的标记物仍以与雄烯二酮相同的程度掺入睾酮中。这些结果表明,未成熟大鼠睾丸微粒体可以在一个有组织的单元上,将添加的孕酮转化为睾酮,而无需中间体与孵育介质达到平衡。

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