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当前关于类固醇生成的急性调节的知识。

Current knowledge on the acute regulation of steroidogenesis.

机构信息

Department of Animal Science, College of Agriculture and Life Sciences, Cornell University, Ithaca, New York, USA.

Department of Cell Biology and Biochemistry, Texas Tech University Health Sciences Center, Lubbock, Texas, USA.

出版信息

Biol Reprod. 2018 Jul 1;99(1):13-26. doi: 10.1093/biolre/ioy102.

Abstract

How rapid induction of steroid hormone biosynthesis occurs in response to trophic hormone stimulation of steroidogenic cells has been a subject of intensive investigation for approximately six decades. A key observation made very early was that acute regulation of steroid biosynthesis required swift and timely synthesis of a new protein whose role appeared to be involved in the delivery of the substrate for all steroid hormones, cholesterol, from the outer to the inner mitochondrial membrane where the process of steroidogenesis begins. It was quickly learned that this transfer of cholesterol to the inner mitochondrial membrane was the regulated and rate-limiting step in steroidogenesis. Following this observation, the quest for this putative regulator protein(s) began in earnest in the late 1950s. This review provides a history of this quest, the candidate proteins that arose over the years and facts surrounding their rise or decline. Only two have persisted-translocator protein (TSPO) and the steroidogenic acute regulatory protein (StAR). We present a detailed summary of the work that has been published for each of these two proteins, the specific data that has appeared in support of their role in cholesterol transport and steroidogenesis, and the ensuing observations that have arisen in recent years that have refuted the role of TSPO in this process. We believe that the only viable candidate that has been shown to be indispensable is the StAR protein. Lastly, we provide our view on what may be the most important questions concerning the acute regulation of steroidogenesis that need to be asked in future.

摘要

在过去的大约六十年里,人们对促性腺激素刺激甾体生成细胞时甾体激素生物合成的快速诱导机制进行了深入研究。一个早期的关键观察结果是,甾体生物合成的急性调节需要迅速及时地合成一种新的蛋白质,其作用似乎涉及将所有甾体激素(胆固醇)的底物从细胞外膜快速转运到开始甾体生成的线粒体内膜。很快就发现,胆固醇向线粒体内膜的这种转运是甾体生成的调节限速步骤。在此观察之后,人们在 20 世纪 50 年代末开始认真寻找这种假定的调节蛋白。本文回顾了这一探索历程,以及多年来出现的候选蛋白及其兴衰的相关事实。只有两种蛋白一直存在——转位蛋白(TSPO)和甾体生成急性调节蛋白(StAR)。我们详细总结了这两种蛋白的所有已发表的工作,以及支持它们在胆固醇转运和甾体生成中作用的具体数据,以及近年来出现的反驳 TSPO 在这一过程中作用的观察结果。我们认为,唯一被证明是不可或缺的可行候选蛋白是 StAR 蛋白。最后,我们就急性调节甾体生成过程中需要在未来提出的最重要的问题提出了我们的看法。

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