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小鼠卵子发生过程中基因表达的转录后调控

Post-transcriptional control of gene expression during mouse oogenesis.

作者信息

Clarke Hugh J

机构信息

Department of Obstetrics and Gynecology, McGill University Health Centre, Montréal, QC, Canada.

出版信息

Results Probl Cell Differ. 2012;55:1-21. doi: 10.1007/978-3-642-30406-4_1.

Abstract

Post-transcriptional mechanisms play a central role in regulating gene expression during oogenesis and early embryogenesis. Growing oocytes accumulate an enormous quantity of messenger RNAs (mRNAs), but transcription decreases dramatically near the end of growth and is undetectable during meiotic maturation. Following fertilization, the embryo is initially transcriptionally inactive and then becomes active at a species-specific stage of early cleavage. Meanwhile, beginning during maturation and continuing after fertilization, the oocyte mRNAs are eliminated, allowing the embryonic genome to assume control of development. How the mammalian oocyte manages the storage, translation, and degradation of the huge quantity and diversity of mRNAs that it harbours has been the focus of enormous research effort and is the subject of this review. We discuss the roles of sequences within the 3'-untranslated region of certain mRNAs and the proteins that bind to them, sequence-non-specific RNA-binding proteins, and recent studies implicating ribonucleoprotein processing (P-) bodies and cytoplasmic lattices. We also discuss mechanisms that may control the temporally regulated translational activation of different mRNAs during meiotic maturation, as well as the signals that trigger silencing and degradation of the oocyte mRNAs. We close by highlighting areas for future research including the potential key role of small RNAs in regulating gene expression in oocytes.

摘要

转录后机制在卵子发生和早期胚胎发育过程中基因表达调控方面发挥着核心作用。正在生长的卵母细胞积累了大量的信使核糖核酸(mRNA),但在生长接近尾声时转录急剧减少,在减数分裂成熟过程中则检测不到转录。受精后,胚胎最初转录不活跃,然后在早期卵裂的特定物种阶段变得活跃。与此同时,从成熟阶段开始并在受精后持续,卵母细胞的mRNA被清除,从而使胚胎基因组能够掌控发育过程。哺乳动物卵母细胞如何管理其所携带的大量且多样的mRNA的储存、翻译和降解,一直是大量研究工作的重点,也是本综述的主题。我们讨论了某些mRNA的3'非翻译区内的序列及其结合蛋白、序列非特异性RNA结合蛋白的作用,以及最近涉及核糖核蛋白加工(P)小体和细胞质晶格的研究。我们还讨论了在减数分裂成熟过程中可能控制不同mRNA的时间调控翻译激活的机制,以及触发卵母细胞mRNA沉默和降解的信号。最后,我们着重指出了未来研究的领域,包括小RNA在调控卵母细胞基因表达方面的潜在关键作用。

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