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首页> 外文期刊>Development >Ca(2+) oscillations induced by a cytosolic sperm protein factor are mediated by a maternal machinery that functions only once in mammalian eggs.
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Ca(2+) oscillations induced by a cytosolic sperm protein factor are mediated by a maternal machinery that functions only once in mammalian eggs.

机译:Ca(2+)振荡由胞浆中的精子蛋白因子诱导的母体机制只在哺乳动物卵中起作用一次。

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At fertilization in mammals, the sperm activates the egg by inducing a series of oscillations in the intracellular free Ca(2+) concentration. There is evidence showing that this oscillatory event is triggered by a sperm-derived protein factor which diffuses into egg cytoplasm after gamete membrane fusion. At present the identity of this factor and its precise mechanism of action is unknown. Here, we studied the specificity of action of the sperm factor in triggering Ca(2+) oscillations in mammalian eggs. In doing so, we examined the patterns of Ca(2+) signaling in mouse eggs, zygotes, parthenogenetic eggs and maturing oocytes following the stimulation of bovine sperm extracts which contain the sperm factor. It is observed that the sperm factor could induce Ca(2+) oscillations in metaphase eggs, maturing oocytes and parthenogenetically activated eggs but not in the zygotes. We present evidence that Ca(2+) oscillations induced by the sperm factor require a maternal machinery. This machinery functions only once in mammalian oocytes and eggs, and is inactivated by sperm-derived components but not by parthenogenetic activation. In addition, it is found that neither InsP(3) receptor sensitivity to InsP(3) nor Ca(2+) pool size are the determinants that cause the fertilized egg to lose its ability to generate sperm-factor-induced Ca(2+) oscillations at metaphase. In conclusion, our study suggests that the orderly sequence of Ca(2+) oscillations in mammalian eggs at fertilization is critically dependent upon the presence of a functional maternal machinery that determines whether the sperm-factor-induced Ca(2+) oscillations can persist.
机译:在哺乳动物的受精时,精子通过诱导细胞内游离Ca(2+)浓度的一系列振荡来激活卵。有证据表明,这种振荡事件是由精子衍生的蛋白质因子触发的,该蛋白质因子在配子膜融合后扩散到卵细胞质中。目前,该因素的身份及其确切的作用机理尚不清楚。在这里,我们研究了在哺乳动物卵中触发Ca(2+)振荡的精子因子作用的特异性。在这样做时,我们检查了包含精子因子的牛精子提取物刺激后,小鼠卵,受精卵,孤雌生殖卵和成熟卵母细胞中Ca(2+)信号的模式。观察到,精子因子可以在中期卵,成熟的卵母细胞和单性生殖激活卵中诱导Ca(2+)振荡,但在受精卵中却不能。我们目前的证据,由精子因子诱导的Ca(2+)振荡需要一个母体机制。该机制仅在哺乳动物卵母细胞和卵中起作用一次,并且被精子衍生的成分失活,而不能由孤雌生殖激活。此外,发现InsP(3)受体对InsP(3)的敏感性和Ca(2+)库的大小都不是导致受精卵丧失产生精子因子诱导的Ca(2+)能力的决定因素。 )中期振荡。总之,我们的研究表明,受精时哺乳动物卵中Ca(2+)振荡的有序序列严重取决于功能性母体机制的存在,该机制决定了精子因子诱导的Ca(2+)振荡是否能够持续。

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