受精的功能加工:蛋白质水解在精子成熟和激活中的关键作用的证据。

C P Blobel
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引用次数: 67

摘要

受精蛋白是精子表面的一种蛋白,在受精过程中起着重要作用。它是精子通过输卵管迁移、与透明带结合以及与卵质膜有效结合所必需的。肥料蛋白由α和β两个亚基组成,它们都属于金属蛋白酶分解蛋白家族(ADAMs)。在睾丸和附睾的精子成熟的不同阶段,α和β是作为较大的前体产生的。受精素α首先被处理,最有可能是由睾丸细胞分泌途径中的前蛋白转化酶处理。当精子在通过附睾的途中时,β -受精在稍后处理。附睾中受精β的加工与精子受精能力的获得相关,暴露了一个在精子-卵子相互作用中起作用的表位,并触发了精子从整个头到后头的再定位。这些发现表明,在附睾精子成熟和激活过程中,受精蛋白和其他精子蛋白的蛋白水解过程起着重要作用。进一步评估蛋白质水解对精子成熟的功能意义,将为精子成熟的机制带来新的和令人兴奋的见解,也可能揭示某些类型的男性不育的原因。对相关蛋白酶的鉴定可为避孕药物的开发提供新的靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Functional processing of fertilin: evidence for a critical role of proteolysis in sperm maturation and activation.

Fertilin is a sperm surface protein with an essential role in fertilization. It is required for the migration of spermatozoa through the oviduct, for binding to the zona pellucida, and for efficient binding to the egg plasma membrane. Fertilin consists of two subunits, fertilin alpha and beta, both of which belong to the metalloprotease-disintegrin protein family (ADAMs). Fertilin alpha and beta are made as larger precursors that are processed proteolytically at different stages of sperm maturation in the testis and epididymis. Fertilin alpha is processed first, most likely by a pro-protein convertase in the secretory pathway of testicular cells. Fertilin beta is processed later, while spermatozoa are in transit through the epididymis. The processing of fertilin beta in the epididymis correlates with the acquisition of fertilization competence in spermatozoa, exposes an epitope that has a role in sperm-egg interactions, and triggers the relocalization of fertilin from the whole sperm head to the posterior head. These findings indicate that the proteolytic processing of fertilin and perhaps also other sperm proteins plays an important role in sperm maturation and activation in the epididymis. Further evaluation of the functional significance of proteolysis for sperm maturation should lead to new and exciting insights into the mechanism of sperm maturation, and may also uncover the cause of certain types of male infertility. The identification of the responsible proteases could provide novel targets for contraceptive drugs.

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