首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >The slow axonal transport of the microtubule-associated protein tau and the transport rates of different isoforms and mutants in cultured neurons.
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The slow axonal transport of the microtubule-associated protein tau and the transport rates of different isoforms and mutants in cultured neurons.

机译:微管相关蛋白tau的轴突运输缓慢,以及培养的神经元中不同亚型和突变体的运输速率。

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摘要

We demonstrate that the microtubule-associated protein tau, in the form of enhanced green fluorescent protein (EGFP) tau, is transported along axons of neurons in culture in the slow component of axonal transport with a speed comparable with that previously measured in vivo. It was demonstrated that the EGFP tag has no effect on transport characteristics, and the methodology enables slow transport rates of individual tau isoforms and tau mutants to be measured. We also expressed EGFP-tagged tau isoforms containing either three or four C-terminal repeats and zero or two N-terminal inserts in cultured neurons. No significant differences were found in the average rate of slow transport of the wild-type tau isoforms, suggesting that the exon 10 C-terminal repeat or the N-terminal inserts do not contain regions that play a significant regulatory role in axonal transport. Similarly, we found that missense mutations in tau have no noticeable effect on the rate of transport; hence their ability to cause neurodegeneration is by another mechanism other than that affecting the overall slow axonal transport of tau.
机译:我们证明微管相关蛋白tau,以增强的绿色荧光蛋白(EGFP)tau的形式,沿着轴突运输的缓慢组成部分沿着培养中的神经元轴突运输,其速度与先前在体内测得的速度相当。事实证明,EGFP标签对转运特性没有影响,该方法能够测定单个tau同工型和tau突变体的缓慢转运速率。我们还表达了EGFP标记的tau亚型,在培养的神经元中包含三个或四个C末端重复和0或两个N末端插入。在野生型tau异构体的平均慢速传输速率上没有发现显着差异,这表明外显子10 C末端重复序列或N末端插入片段不包含在轴突运输中起重要调控作用的区域。同样,我们发现tau中的错义突变对转运速率没有明显影响。因此,它们引起神经变性的能力是由另一种机制引起的,而不是影响总体缓慢的tau轴突运输。

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