改变血液中活性雄激素的概念

Pentti K. Siiteri, Niklas H. Simberg
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引用次数: 29

摘要

我们提供了一个简短的历史回顾,在我们的理解的发展,内分泌机制的表达,雄激素的作用在妇女。另一种替代自由激素概念的观点认为,至少在某些靶细胞中,与SHBG结合的雄激素是生物学上相关的分子。几乎在每一个例子中,已经观察到的SHBG血液水平的变化都与这一观点相一致。目前只有少量的直接证据支持所提出的假设机制。如前所述,在细胞摄取水平上控制雄激素的作用将提供明显的优势,以及解释雄激素和雌激素之间拮抗作用的潜在机制,这仍然是一个谜。值得注意的是,所提出的机制不是雄激素或其他类固醇激素作用的强制性机制。合成类固醇不与SHBG或CBG明显结合,可通过简单扩散进入靶细胞并与细胞内受体结合。甲基睾酮和地塞米松等化合物的代谢比它们的天然对应物慢得多,因此从循环中被清除得很慢。众所周知,使用这些化合物选择适当治疗方案的困难可能与它们绕过类固醇激素动作调节进入靶细胞的重要调节步骤有关。有希望的是,最近分子内分泌学强大的新工具的发展将加速这个问题的答案:血液中的活性雄激素是什么?
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3 Changing concepts of active androgens in blood

We have provided a brief historical review of developments in our understanding of the endocrine mechanisms underlying the expression of androgen action in women. An alternative to the free hormone concept is considered which proposes that, at least in some target cells, androgens bound to SHBG are the biologically relevant molecules. In nearly every instance, the changes in blood levels of SHBG that have been observed are consistent with this idea. At present there are only bits of direct evidence to support the hypothetical mechanism proposed. As already mentioned, control of androgen action at the level of cellular uptake would provide obvious advantages as well as a potential mechanism to explain the antagonism between androgens and oestrogens which is still a mystery. It is important to note that the proposed mechanism is not obligatory for androgen or other steroid hormone action. Synthetic steroids which do not bind to SHBG or CBG clearly can gain access to target cells by simple diffusion and bind to intracellular receptors. Compounds such as methyltestosterone and dexamethasone are metabolized much more slowly than their natural counterparts and therefore are cleared slowly from the circulation. It is possible that the well-known difficulties in selecting appropriate therapeutic regimens with such compounds is related to the fact that they bypass an important regulatory step in steroid hormone action—modulated entry into target cells. Hopefully, the recent development of powerful new tools of molecular endocrinology will hasten the answer to the question: What is the active androgen in blood?

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