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When a sperm meets an egg: block to polyspermy.

机译:当精子遇到卵子时:阻止多精子。

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摘要

Embryonic development is initiated after the fertilizing spermatozoon enters the egg and triggers a series of events known as egg activation. Activation results in an increase in intracellular calcium concentration, cortical granule exocytosis (CGE), cell cycle resumption and recruitment of maternal mRNA. CGE is an evolutionary developed mechanism that causes modification of the zona pellucida to prevent penetration of additional spermatozoa, ensuring successful egg activation and embryo development. The egg CGE is a unique and convenient mammalian model for studying the different proteins participating at the membrane fusion cascade, which, unlike other secretory cells, occurs only once in the egg's lifespan. This article highlights a number of proteins, ascribed to participate in CGE and thus the block to polyspermy. CGE can be triggered either by a calcium dependent pathway, or via protein kinase C (PKC) activation that requires a very low calcium concentration. In a recent study, we suggested that the filamentous actin (F-actin) at the egg's cortex is a dynamic network. It can be maneuvered towards allowing CGE by activated actin associated proteins and/or by activated PKC and its down stream proteins, such as myristoylated alanine-rich C kinase substrate (MARCKS). MARCKS, a protein known to cross-link F-actin in other cell types, was found to be expressed and colocalized with actin in non-activated MII eggs. We further demonstrated MARCKS dissociation from actin after activation by ionomycin, a process that can lead to the breakdown of the actin network, thus allowing CGE. The more we know of the intricate process of CGE and of the proteins participating in it, the more the assisted reproductive procedures might benefit from that knowledge.
机译:受精精子进入卵子并引发一系列称为卵子激活的事件后,胚胎发育便开始了。激活导致细胞内钙浓度,皮质颗粒胞吐作用(CGE),细胞周期恢复和母体mRNA募集增加。 CGE是一种进化发展的机制,可引起透明带的修饰,以防止其他精子穿透,从而确保成功的卵子活化和胚胎发育。鸡蛋CGE是一种独特而便捷的哺乳动物模型,用于研究参与膜融合级联反应的不同蛋白质,与其他分泌细胞不同,该蛋白质在鸡蛋的寿命中仅发生一次。本文重点介绍了参与CGE并因此阻止多精子的多种蛋白质。 CGE可以通过钙依赖性途径触发,也可以通过需要非常低钙浓度的蛋白激酶C(PKC)激活来触发。在最近的研究中,我们认为卵皮层的丝状肌动蛋白(F-actin)是一个动态网络。可以通过激活的肌动蛋白相关蛋白和/或激活的PKC及其下游蛋白(例如肉豆蔻酰化的富含丙氨酸的C激酶底物(MARCKS))来操纵CGE。发现MARCKS是一种已知可在其他细胞类型中交联F-肌动蛋白的蛋白质,在未激活的MII卵中与肌动蛋白一起表达并共定位。我们进一步证明了离子霉素激活后,肌动蛋白从肌动蛋白上解离,该过程可能导致肌动蛋白网络崩溃,从而导致CGE。我们对CGE的复杂过程和参与其中的蛋白质了解得越多,辅助生殖程序就可能从该知识中受益。

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