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非洲爪蟾胚胎中分裂不同步现象及微管依赖染色体周期出现的调控

Regulation of the appearance of division asynchrony and microtubule-dependent chromosome cycles in Xenopus laevis embryos.

作者信息

Clute P, Masui Y

机构信息

Department of Zoology, University of Toronto, Ontario, Canada.

出版信息

Dev Biol. 1995 Oct;171(2):273-85. doi: 10.1006/dbio.1995.1280.

DOI:10.1006/dbio.1995.1280
PMID:7556912
Abstract

Divisions of animal-cap blastomeres dissociated from Xenopus laevis embryos are synchronous mostly up to 12th cleavage or the 13th cell cycle, but become asynchronous afterward, during the midblastula transition (MBT), and at the same time, chromosome cycles become microtubule-dependent and are arrested in mitosis if treated with nocodazole. To investigate causes for these changes in cell-cycle control, we observed division synchrony in animal-cap blastomeres dissociated from embryos whose nucleocytoplasmic ratio (N/C) had been altered by constriction of zygotes or by delaying nucleation into zygote halves and compared their mitotic indices in the presence and absence of nocodazole. Thus, we found that asynchronous divisions always commenced when N/C reached the value of 128 to 256 times that of an animal blastomere of the 32-cell embryo, corresponding to the 12th and 13th cycles of a normal embryo, while the number of synchronous cycles became variable, ranging from 9 to 14, depending on the initial N/C. Treatment with alpha-amanitin or cycloheximide did not alter the number of synchronous cycles. However, the time at which the mitotic index of nocodazole-treated blastomeres first exceeded that of control remained constant, at 3 to 5 hr after 5th cleavage, regardless of the initial N/C. Thus, chromosome cycles of blastomeres first became sensitive to nocodazole at a variable N/C, ranging from 8 to 1024 times that of an animal blastomere of the 32-cell embryo. The timing of the appearance of nocodazole sensitivity was unaffected by alpha-amanitin treatment, whereas it was markedly delayed following cycloheximide treatment. These results suggest that the commencement of division asynchrony is N/C-dependent, whereas the development of microtubule-dependent cell cycles is age-dependent, most likely being programmed by the translation of stored mRNAs.

摘要

从非洲爪蟾胚胎分离出的动物帽卵裂球,在第12次卵裂或第13个细胞周期之前,其分裂大多是同步的,但在中囊胚转换(MBT)期间随后会变得不同步。同时,如果用诺考达唑处理,染色体周期会变得依赖微管,并在有丝分裂中停滞。为了研究细胞周期调控中这些变化的原因,我们观察了从合子收缩或延迟核化到合子两半而改变了核质比(N/C)的胚胎中分离出的动物帽卵裂球的分裂同步性,并比较了在有和没有诺考达唑情况下它们的有丝分裂指数。因此,我们发现当N/C达到32细胞期胚胎动物卵裂球的128至256倍时,异步分裂总是开始,这对应于正常胚胎的第12和13个周期,而同步周期的数量变得可变,从9到14个不等,这取决于初始N/C。用α-鹅膏蕈碱或环己酰亚胺处理不会改变同步周期的数量。然而,无论初始N/C如何,诺考达唑处理的卵裂球的有丝分裂指数首次超过对照的时间保持恒定,在第5次卵裂后3至5小时。因此,卵裂球的染色体周期在可变的N/C时首先对诺考达唑敏感,范围是32细胞期胚胎动物卵裂球的8至1024倍。诺考达唑敏感性出现的时间不受α-鹅膏蕈碱处理的影响,而在环己酰亚胺处理后明显延迟。这些结果表明,分裂异步的开始是N/C依赖性的,而依赖微管的细胞周期的发展是年龄依赖性的,很可能是由储存mRNA的翻译编程的。

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