The timing of compaction: control of a major developmental transition in mouse early embryogenesis.

J B Levy, M H Johnson, H Goodall, B Maro
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Abstract

The effect of protein synthesis inhibitors on compaction of the 8-cell mouse embryo has been investigated. The effects observed depended upon the duration and time of drug application and on the features of compaction scored. Continuous application from the late 2-cell or early 4-cell stages allowed cell flattening and surface polarization to occur in most embryos and advanced development of these features in many of them. Cell coupling developed only when drug addition was delayed until the mid 4-cell stage, and cytoplasmic polarization developed only when drug addition was delayed until the late 4-cell stage. We suggest that control over the timing of compaction is achieved at a post-translational level via a global permissive change within the blastomeres of the embryo.

压实的时间:小鼠早期胚胎发生中一个主要发育转变的控制。
研究了蛋白质合成抑制剂对8细胞小鼠胚胎压实的影响。观察到的效果取决于药物应用的持续时间和时间以及压实评分的特征。从2细胞晚期或4细胞早期开始的持续应用使得大多数胚胎的细胞变平和表面极化发生,并且在许多胚胎中这些特征的高级发育。只有当药物添加延迟到4细胞中期时,才会出现细胞偶联;只有当药物添加延迟到4细胞晚期时,才会出现细胞质极化。我们认为对压实时间的控制是通过胚胎卵裂球内的全局允许变化在翻译后水平上实现的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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