首页> 外文期刊>Nature neuroscience >An NGF-responsive element targets myo-inositol monophosphatase-1 mRNA to sympathetic neuron axons.
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An NGF-responsive element targets myo-inositol monophosphatase-1 mRNA to sympathetic neuron axons.

机译:NGF响应​​元件将肌醇单磷酸酶1 mRNA靶向交感神经元轴突。

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摘要

mRNA localization is an evolutionary conserved mechanism that underlies the establishment of cellular polarity and specialized cell functions. To identify mRNAs localized in subcellular compartments of developing neurons, we took an original approach that combines compartmentalized cultures of rat sympathetic neurons and sequential analysis of gene expression (SAGE). Unexpectedly, the most abundant transcript in axons was mRNA for myo-inositol monophosphatase-1 (Impa1), a key enzyme that regulates the inositol cycle and the main target of lithium in neurons. A novel localization element within the 3' untranslated region of Impa1 mRNA specifically targeted Impa1 transcript to sympathetic neuron axons and regulated local IMPA1 translation in response to nerve growth factor (NGF). Selective silencing of IMPA1 synthesis in axons decreased nuclear CREB activation and induced axonal degeneration. These results provide insights into mRNA transport in axons and reveal a new NGF-responsive localization element that directs the targeting and local translation of an axonal transcript.
机译:mRNA定位是进化保守的机制,是建立细胞极性和专门细胞功能的基础。为了鉴定位于发育中的神经元的亚细胞区室中的mRNA,我们采用了一种原始方法,该方法将大鼠交感神经元的区室化培养与基因表达的顺序分析(SAGE)相结合。出乎意料的是,轴突中最丰富的转录物是肌醇单磷酸酶-1(Impa1)的mRNA,肌醇单磷酸酶-1(Impa1)是调节肌醇周期和神经元中锂的主要靶标的关键酶。 Impa1 mRNA 3'非翻译区内的新型定位元件将Impa1转录物特异性地靶向交感神经元轴突,并响应神经生长因子(NGF)调节局部IMPA1翻译。轴突中IMPA1合成的选择性沉默降低了核CREB活化并诱导了轴突变性。这些结果提供了对轴突中mRNA转运的见解,并揭示了一种新的NGF响应​​性定位元件,该元件可指导轴突转录物的靶向和局部翻译。

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