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卵母细胞减数分裂的翻译调控:迈向基因组时代。

Translational Control of Oocyte Meiosis: Toward the Genomic Era.

机构信息

Sorbonne Université, CNRS, Laboratoire de Biologie du Développement-Institut de Biologie Paris Seine, LBD-IBPS, F-75005 Paris, France.

出版信息

Cells. 2020 Jun 19;9(6):1502. doi: 10.3390/cells9061502.

Abstract

The study of oocytes has made enormous contributions to the understanding of the G/M transition. The complementarity of investigations carried out on various model organisms has led to the identification of the M-phase promoting factor (MPF) and to unravel the basis of cell cycle regulation. Thanks to the power of biochemical approaches offered by frog oocytes, this model has allowed to identify the core signaling components involved in the regulation of M-phase. A central emerging layer of regulation of cell division regards protein translation. Oocytes are a unique model to tackle this question as they accumulate large quantities of dormant mRNAs to be used during meiosis resumption and progression, as well as the cell divisions during early embryogenesis. Since these events occur in the absence of transcription, they require cascades of successive unmasking, translation, and discarding of these mRNAs, implying a fine regulation of the timing of specific translation. In the last years, the genome has been sequenced and annotated, enabling the development of omics techniques in this model and starting its transition into the genomic era. This review has critically described how the different phases of meiosis are orchestrated by changes in gene expression. The physiological states of the oocyte have been described together with the molecular mechanisms that control the critical transitions during meiosis progression, highlighting the connection between translation control and meiosis dynamics.

摘要

卵母细胞的研究对理解 G/M 转换做出了巨大贡献。在各种模式生物上进行的互补研究导致了 M 期促进因子 (MPF) 的鉴定,并阐明了细胞周期调控的基础。由于蛙卵母细胞提供的生化方法的强大功能,该模型允许鉴定参与 M 期调控的核心信号成分。细胞分裂的一个重要新兴调控层涉及蛋白质翻译。卵母细胞是解决这个问题的独特模型,因为它们积累了大量的休眠 mRNA,这些 mRNA 将在减数分裂恢复和进展以及早期胚胎发生过程中的细胞分裂中使用。由于这些事件发生在没有转录的情况下,它们需要对这些 mRNA 进行连续的揭示、翻译和丢弃的级联,这意味着对特定翻译的时间进行精细调控。在过去的几年中,基因组已经被测序和注释,使这个模型中的组学技术得以发展,并开始进入基因组时代。这篇综述批判性地描述了减数分裂的不同阶段如何通过基因表达的变化来协调。描述了卵母细胞的生理状态以及控制减数分裂进展过程中关键转变的分子机制,突出了翻译控制和减数分裂动力学之间的联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4970/7348711/ec060dbeeb5c/cells-09-01502-g001.jpg

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