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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Selective localization of Arc mRNA in dendrites involves activity- and translation-dependent mRNA degradation
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Selective localization of Arc mRNA in dendrites involves activity- and translation-dependent mRNA degradation

机译:树突状细胞中Arc mRNA的选择性定位涉及依赖于活性和翻译的mRNA降解

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摘要

Arc is an immediate early gene that is unique among neuronal mRNAs because its transcripts are transported into dendrites and accumulate near activated synapses, presumably to be translated locally. These qualities pose Arc as playing an important, yet not fully understood, role in the activity-dependent modifications of synapses that are thought to underlie memory storage. Here we show in vivo in rats that newly synthesized Arc mRNA accumulates at activated synapses and that synaptic activity simultaneously triggers mRNA decay that eliminates Arc mRNA from inactive dendritic domains. Arc mRNA degradation occurs throughout the dendrite and requires both NMDA receptor activation and active translation. Synaptic activation did not lead to decreases in another dendritic mRNA (αCaMKII), indicating that there is not a general activation of mRNA degradation in dendrites. These data reveal a novel mechanism for controlling mRNA distribution within dendrites and highlight activity-dependent mRNA degradation as a regulatory process involved in synaptic plasticity.
机译:Arc是一种即时的早期基因,在神经元mRNA中是独特的,因为它的转录物被转运到树突中并积聚在活化的突触附近,大概是本地翻译的。这些特质使Arc在依赖于记忆的突触的活动依赖型修饰中起着重要但尚未完全理解的作用。在这里,我们在大鼠体内显示了新合成的Arc mRNA在激活的突触处积累,并且突触活性同时触发了mRNA衰变,从而从非活动的树突结构域消除了Arc mRNA。 Arc mRNA降解发生在整个树突中,需要NMDA受体激活和主动翻译。突触激活未导致另一个树突状mRNA(αCaMKII)减少,表明树突中没有普遍的mRNA降解活化。这些数据揭示了一种控制树突中mRNA分布的新机制,并强调了依赖活性的mRNA降解作为涉及突触可塑性的调控过程。

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