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哺乳动物精子的“激活”:参与顶体反应促进和调控的分子事件。

The "switching on" of mammalian spermatozoa: molecular events involved in promotion and regulation of capacitation.

机构信息

Division of Reproduction and Endocrinology, School of Biomedical and Health Sciences, King's College London, London SE1 1UL, UK.

出版信息

Mol Reprod Dev. 2010 Mar;77(3):197-208. doi: 10.1002/mrd.21124.

DOI:10.1002/mrd.21124
PMID:19908247
Abstract

Following the discovery of mammalian sperm capacitation and its fundamental importance for the acquisition of fertilizing potential, it has gradually become possible to identify some specific molecules and molecular events that play pivotal roles in the "switching on" of spermatozoa. These are discussed in the context of the promotion and regulation of capacitation, emphasizing differences between commonly used conditions in vitro and the environment in vivo where spermatozoa normally undergo capacitation. Although typical culture media used in vitro do support capacitation, they do not prevent capacitated cells from undergoing spontaneous acrosome reactions and so losing fertilizing potential. This is not a problem in vitro, but could be in vivo where few spermatozoa reach the site of fertilization. Several small molecules, known to be present in vivo, have been shown in vitro to bind to spermatozoa and to regulate capacitation, first accelerating capacitation and then inhibiting spontaneous acrosome reactions, by regulating cAMP production. Since spermatozoa would contact these molecules during and after ejaculation, it is plausible that they serve a similar function in vivo. The mechanisms whereby the presence or absence of decapacitation factors might alter plasma membrane architecture and so alter functionality of a number of membrane-associated enzymes involved in capacitation are also considered. Finally, several unresolved issues relating to events during capacitation are discussed.

摘要

哺乳动物精子获能的发现及其对获得受精能力的重要性逐渐得到认识,这使得人们有可能识别出一些在精子“启动”过程中起关键作用的特定分子和分子事件。本文讨论了获能的促进和调节,强调了常用的体外条件与精子正常获能的体内环境之间的差异。尽管体外常用的典型培养基确实支持获能,但它们并不能防止获能的细胞自发发生顶体反应,从而失去受精能力。这在体外不是问题,但在体内可能是个问题,因为很少有精子到达受精部位。已经在体外证明,一些已知存在于体内的小分子可以与精子结合,并通过调节 cAMP 产生来调节获能,首先加速获能,然后抑制自发的顶体反应。由于精子在射精过程中和射精后会接触到这些分子,因此它们在体内可能具有类似的功能。还考虑了去获能因子的存在或缺失如何改变质膜结构,从而改变参与获能的许多膜相关酶的功能的机制。最后,还讨论了与获能过程中相关的一些未解决的问题。

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