ZBP1 的有限可用性限制了轴突 mRNA 的定位和神经再生能力。
Limited availability of ZBP1 restricts axonal mRNA localization and nerve regeneration capacity.
机构信息
Department of Biological Sciences, University of Delaware, Newark, USA.
出版信息
EMBO J. 2011 Sep 30;30(22):4665-77. doi: 10.1038/emboj.2011.347.
Abstract
Subcellular localization of mRNAs is regulated by RNA-protein interactions. Here, we show that introduction of a reporter mRNA with the 3'UTR of β-actin mRNA competes with endogenous mRNAs for binding to ZBP1 in adult sensory neurons. ZBP1 is needed for axonal localization of β-actin mRNA, and introducing GFP with the 3'UTR of β-actin mRNA depletes axons of endogenous β-actin and GAP-43 mRNAs and attenuates both in vitro and in vivo regrowth of severed axons. Consistent with limited levels of ZBP1 protein in adult neurons, mice heterozygous for the ZBP1 gene are haploinsufficient for axonal transport of β-actin and GAP-43 mRNAs and for regeneration of peripheral nerve. Exogenous ZBP1 can rescue the RNA transport deficits, but the axonal growth deficit is only rescued if the transported mRNAs are locally translated. These data support a direct role for ZBP1 in transport and translation of mRNA cargos in axonal regeneration in vitro and in vivo.
摘要
mRNA 的亚细胞定位受 RNA-蛋白相互作用的调控。在这里,我们表明,引入带有 β-肌动蛋白 mRNA 3'UTR 的报告 mRNA 会与内源性 mRNAs 竞争与成年感觉神经元中的 ZBP1 结合。ZBP1 是 β-肌动蛋白 mRNA 轴突定位所必需的,引入带有 β-肌动蛋白 mRNA 3'UTR 的 GFP 会耗尽轴突内源性 β-肌动蛋白和 GAP-43 mRNAs,并减弱体外和体内切断轴突的再生长。与成年神经元中 ZBP1 蛋白水平有限一致,ZBP1 基因杂合子的小鼠对 β-肌动蛋白和 GAP-43 mRNAs 的轴突运输以及外周神经的再生都是半不足的。外源性 ZBP1 可以挽救 RNA 运输缺陷,但只有在运输的 mRNAs 局部翻译时,轴突生长缺陷才会得到挽救。这些数据支持 ZBP1 在体外和体内轴突再生中对 mRNA 货物的运输和翻译的直接作用。
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