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The opioid peptide beta-endorphin stimulates acrosome reaction in human spermatozoa

机译:阿片肽β-内啡肽刺激人精子顶体反应

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摘要

The acrosome reaction occurs in vivo following sperm capacitation and is essential for the acquisition of sperm fertilization ability. However, little is known about the molecular identity of the physiological acrosome reaction regulators. In addition to progesterone, which is produced by cumulus oophorus cells and known to regulate acrosome reaction by activating the specific calcium channel CatSper, endogenous opioid peptides such as beta-endorphin and met-enkephalin are present at high concentrations in the follicular fluid suggesting that the opioid system may be involved in the mechanisms regulating the acrosome reaction in humans. By using Reverse Transcription-PCR, western blot and immunofluorescence approaches, we described the presence and localization of the beta-endorphin precursor, pro-opiomelanocortinin the middle section and in flagellum of human spermatozoa, and inside the seminiferous tubules of human testis. Flow cytometry and intracellular calcium analyses showed that beta-endorphin causes an inversely dose-dependent increase in the percentage of acrosome-reacted sperm cells by a calcium-independent protein kinase C pathway. These findings are important for future studies of sperm physiology and provide new insight into the function of the opioid system as a target of fertility management.
机译:顶体反应在精子获能后体内发生,对于获得精子受精能力至关重要。但是,关于生理顶体反应调节剂的分子同一性知之甚少。除了由卵丘卵细胞产生的孕酮并已知通过激活特定的钙通道CatSper来调节顶体反应外,卵泡液中还存在高浓度的内源性阿片肽,例如β-内啡肽和甲脑啡肽。阿片样物质系统可能参与调节人类顶体反应的机制。通过使用逆转录PCR,蛋白质印迹和免疫荧光方法,我们描述了β-内啡肽前体,pro-opiomelanocortin在人精子中段和鞭毛中以及人睾丸生精小管中的存在和定位。流式细胞仪和细胞内钙分析表明,β-内啡肽通过钙非依赖性蛋白激酶C途径引起顶体反应的精子细胞百分比成反比剂量依赖性。这些发现对于将来对精子生理的研究很重要,并提供了对阿片样物质系统作为生育管理目标的功能的新见解。

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