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后期发育过程中的mRNA定位:过去、现在与未来

mRNA Localization During Later Development: Past, Present, and Future.

作者信息

Hughes Sarah C, Simmonds Andrew J

机构信息

Department of Medical Genetics, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, AB, Canada.

Department of Cell Biology, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, AB, Canada.

出版信息

Front Genet. 2019 Mar 7;10:135. doi: 10.3389/fgene.2019.00135. eCollection 2019.

Abstract

Multiple mechanisms tightly regulate mRNAs during their transcription, translation, and degradation. Of these, the physical localization of mRNAs to specific cytoplasmic regions is relatively easy to detect; however, linking localization to functional regulatory roles has been more difficult to establish. Historically, is a highly effective model to identify localized mRNAs and has helped identify roles for this process by regulating various cell activities. The majority of the well-characterized functional roles for localizing mRNAs to sub-regions of the cytoplasm have come from the oocyte and early syncytial embryo. At present, relatively few functional roles have been established for mRNA localization within the relatively smaller, differentiated somatic cell lineages characteristic of later development, beginning with the cellular blastoderm, and the multiple cell lineages that make up the gastrulating embryo, larva, and adult. This review is divided into three parts-the first outlines past evidence for cytoplasmic mRNA localization affecting aspects of cellular activity post-blastoderm development in . The majority of these known examples come from highly polarized cell lineages such as differentiating neurons. The second part considers the present state of affairs where we now know that many, if not most mRNAs are localized to discrete cytoplasmic regions in one or more somatic cell lineages of cellularized embryos, larvae or adults. Assuming that the phenomenon of cytoplasmic mRNA localization represents an underlying functional activity, and correlation with the encoded proteins suggests that mRNA localization is involved in far more than neuronal differentiation. Thus, it seems highly likely that past-identified examples represent only a small fraction of localization-based mRNA regulation in somatic cells. The last part highlights recent technological advances that now provide an opportunity for probing the role of mRNA localization in , moving beyond cataloging the diversity of localized mRNAs to a similar understanding of how localization affects mRNA activity.

摘要

在mRNA的转录、翻译和降解过程中,多种机制对其进行严格调控。其中,mRNA在细胞质特定区域的物理定位相对易于检测;然而,将定位与功能调控作用联系起来则更难确定。从历史上看,[具体生物名称]是识别定位mRNA的高效模型,并通过调节各种细胞活动帮助确定了这一过程的作用。将mRNA定位到细胞质亚区域的大多数已明确的功能作用来自[具体生物名称]的卵母细胞和早期合胞体胚胎。目前,对于在发育后期相对较小、已分化的体细胞谱系(从细胞胚盘开始)以及构成原肠胚、幼虫和成虫的多个细胞谱系中mRNA定位所起的功能作用,确定得相对较少。本综述分为三个部分——第一部分概述了过去关于细胞质mRNA定位影响[具体生物名称]胚盘后发育阶段细胞活动方面的证据。这些已知例子大多来自高度极化的细胞谱系,如分化中的神经元。第二部分探讨了目前的情况,即我们现在知道,在细胞化胚胎、幼虫或成虫的一个或多个体细胞谱系中,许多(如果不是大多数)mRNA都定位到离散的细胞质区域。假设细胞质mRNA定位现象代表一种潜在的功能活动,并且与编码蛋白的相关性表明mRNA定位所涉及的远不止神经元分化。因此,过去确定的例子很可能仅代表体细胞中基于定位的mRNA调控的一小部分。最后一部分重点介绍了最近的技术进展,这些进展为探究mRNA定位在[具体生物名称]中的作用提供了机会,从编目定位mRNA的多样性转向类似地了解定位如何影响mRNA活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e616/6416162/c653673eb193/fgene-10-00135-g0001.jpg

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