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Rapid reversal of translational silencing: Emerging role of microRNA degradation pathways in neuronal plasticity

机译:翻译沉默的快速逆转:microRNA降解途径在神经元可塑性中的新兴作用

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摘要

As microRNAs silence translation, rapid reversal of this process has emerged as an attractive mechanism for driving de novo protein synthesis mediating neuronal plasticity. Herein, we summarize recent studies identifying neuronal stimuli that trigger rapid decreases in microRNA levels and reverse translational silencing of plasticity transcripts. Although these findings indicate that neuronal stimulation elicits rapid degradation of selected microRNAs, we are only beginning to decipher the molecular pathways involved. Accordingly, we present an overview of several molecular pathways implicated in mediating microRNA degradation: Lin-28, translin/trax, and MCPIP1. As these degradation pathways target distinct subsets of microRNAs, they enable neurons to reverse silencing rapidly, yet selectively. (C) 2016 Elsevier Inc. All rights reserved.
机译:随着microRNA沉默翻译的出现,该过程的快速逆转已成为驱动介导神经元可塑性的从头蛋白合成的有吸引力的机制。在这里,我们总结了最近的研究,这些研究确定了可触发microRNA水平快速降低和可塑性转录本反向翻译沉默的神经元刺激。尽管这些发现表明神经元刺激会引起所选microRNA的快速降解,但我们才刚刚开始破译涉及的分子途径。因此,我们提出了介导microRNA降解的几种分子途径的概述:Lin-28,translin / trax和MCPIP1。由于这些降解途径靶向microRNA的不同子集,因此它们使神经元能够快速而选择性地逆转沉默。 (C)2016 Elsevier Inc.保留所有权利。

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