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Staufen1对海马锥体细胞中蛋白质合成依赖性长时程增强和突触功能的调控

Staufen1 regulation of protein synthesis-dependent long-term potentiation and synaptic function in hippocampal pyramidal cells.

作者信息

Lebeau Geneviève, Maher-Laporte Marjolaine, Topolnik Lisa, Laurent Charles E, Sossin Wayne, Desgroseillers Luc, Lacaille Jean-Claude

机构信息

Département de physiologie, Université de Montréal, C.P. 6128 Succ. Centre-ville, Montréal, Québec, Canada.

出版信息

Mol Cell Biol. 2008 May;28(9):2896-907. doi: 10.1128/MCB.01844-07. Epub 2008 Mar 3.

DOI:10.1128/MCB.01844-07
PMID:18316402
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2293094/
Abstract

Staufen1 (Stau1) is an RNA-binding protein involved in transport, localization, decay, and translational control of mRNA. In neurons, it is present in cell bodies and also in RNA granules which are transported along dendrites. Dendritic mRNA localization might be involved in long-term synaptic plasticity and memory. To determine the role of Stau1 in synaptic function, we examined the effects of Stau1 down-regulation in hippocampal slice cultures using small interfering RNA (siRNA). Biolistic transfection of Stau1 siRNA resulted in selective down-regulation of Stau1 in slice cultures. Consistent with a role of Stau1 in transporting mRNAs required for synaptic plasticity, Stau1 down-regulation impaired the late form of chemically induced long-term potentiation (L-LTP) without affecting early-LTP, mGluR1/5-mediated long-term depression, or basal evoked synaptic transmission. Stau1 down-regulation decreased the amplitude and frequency of miniature excitatory postsynaptic currents, suggesting a role in maintaining efficacy at hippocampal synapses. At the cellular level, Stau1 down-regulation shifted spine shape from regular to elongated spines, without changes in spine density. The change in spine shape could be rescued by an RNA interference-resistant Stau1 isoform. Therefore, Stau1 is important for processing and/or transporting in dendrites mRNAs that are critical in regulation of synaptic strength and maintenance of functional connectivity changes underlying hippocampus-dependent learning and memory.

摘要

Staufen1(Stau1)是一种RNA结合蛋白,参与mRNA的运输、定位、降解及翻译控制。在神经元中,它存在于细胞体以及沿树突运输的RNA颗粒中。树突mRNA定位可能参与长期突触可塑性和记忆。为了确定Stau1在突触功能中的作用,我们使用小干扰RNA(siRNA)检测了其在海马脑片培养物中下调的影响。对Stau1 siRNA进行生物弹道转染导致脑片培养物中Stau1的选择性下调。与Stau1在运输突触可塑性所需mRNA中的作用一致,Stau1下调损害了化学诱导的晚期长时程增强(L-LTP),而不影响早期LTP、mGluR1/5介导的长时程抑制或基础诱发的突触传递。Stau1下调降低了微小兴奋性突触后电流的幅度和频率,表明其在维持海马突触效能中发挥作用。在细胞水平上,Stau1下调使棘突形状从规则变为细长,而棘突密度没有变化。棘突形状的改变可以通过一种抗RNA干扰的Stau1同种型来挽救。因此,Stau1对于在树突中加工和/或运输对调节突触强度以及维持海马依赖性学习和记忆所依赖的功能连接变化至关重要的mRNA很重要。

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The zinc-finger protein ZFR is critical for Staufen 2 isoform specific nucleocytoplasmic shuttling in neurons.锌指蛋白ZFR对神经元中Staufen 2亚型特异性核质穿梭至关重要。
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