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Argonautes、miRISC 和 RNA 结合蛋白之间相互作用在神经元和神经胶质细胞中局部翻译调控中的作用。

A Proposed Role for Interactions between Argonautes, miRISC, and RNA Binding Proteins in the Regulation of Local Translation in Neurons and Glia.

机构信息

Department of Genetics.

Department of Psychiatry.

出版信息

J Neurosci. 2022 Apr 20;42(16):3291-3301. doi: 10.1523/JNEUROSCI.2391-21.2022.

Abstract

The first evidence of local translation in the CNS appeared nearly 40 years ago, when electron microscopic studies showed polyribosomes localized to the base of dendritic spines. Since then, local translation has been established as an important regulatory mechanism for gene expression in polarized or functionally compartmentalized cells. While much attention has been placed on characterizing the local transcriptome and regulatory "grammar" directing mRNA localization in neurons and glia, less is understood about how these cells subsequently de-repress mRNA translation in their peripheral processes to produce a rapid translational response to stimuli. MicroRNA-mediated translation regulation offers a possible solution to this question. Not only do miRNAs provide the specificity needed for targeted gene regulation, but association and dynamic interactions between Argonaute (AGO) with sequence-specific RNA-binding proteins may provide a molecular switch to allow for de-repression of target mRNAs. Here, we review the expression and activity of different AGO proteins in miRNA-induced silencing complexes in neurons and glia and discuss known pathways of miRNA-mediated regulation, including activity-dependent pre-miRNA maturation in dendrites. We further detail work on AGO and RNA-binding protein interactions that allow for the reversal of miRNA-mediated translational silencing, and we propose a model for how intercellular communication may play a role in the regulation of local translation.

摘要

CNS 中局部翻译的第一个证据出现在近 40 年前,当时电子显微镜研究表明多核糖体定位于树突棘的基部。从那时起,局部翻译已被确立为极化或功能分隔细胞中基因表达的重要调节机制。虽然人们已经关注了描述神经元和神经胶质细胞中局部转录组和调节“语法”指导 mRNA 定位的特征,但对于这些细胞如何随后解除其外周突中 mRNA 翻译的抑制以产生对刺激的快速翻译反应,人们的了解较少。miRNA 介导的翻译调控为这个问题提供了一个可能的解决方案。miRNAs 不仅提供了靶向基因调控所需的特异性,而且 Argonaute (AGO) 与序列特异性 RNA 结合蛋白之间的关联和动态相互作用可能提供了一个分子开关,允许靶 mRNA 的去抑制。在这里,我们回顾了不同 AGO 蛋白在神经元和神经胶质细胞中 miRNA 诱导的沉默复合物中的表达和活性,并讨论了已知的 miRNA 介导的调节途径,包括树突中依赖于活性的前体 miRNA 成熟。我们进一步详细介绍了允许 miRNA 介导的翻译沉默逆转的 AGO 和 RNA 结合蛋白相互作用的工作,并提出了一个关于细胞间通讯如何在局部翻译调节中发挥作用的模型。

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