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微管稳定作用决定了神经元最初的极化。

Microtubule stabilization specifies initial neuronal polarization.

作者信息

Witte Harald, Neukirchen Dorothee, Bradke Frank

机构信息

Axonal Growth and Regeneration, Max Planck Institute of Neurobiology, 82152 Martinsried, Germany.

出版信息

J Cell Biol. 2008 Feb 11;180(3):619-32. doi: 10.1083/jcb.200707042.

Abstract

Axon formation is the initial step in establishing neuronal polarity. We examine here the role of microtubule dynamics in neuronal polarization using hippocampal neurons in culture. We see increased microtubule stability along the shaft in a single neurite before axon formation and in the axon of morphologically polarized cells. Loss of polarity or formation of multiple axons after manipulation of neuronal polarity regulators, synapses of amphids defective (SAD) kinases, and glycogen synthase kinase-3beta correlates with characteristic changes in microtubule turnover. Consistently, changing the microtubule dynamics is sufficient to alter neuronal polarization. Application of low doses of the microtubule-destabilizing drug nocodazole selectively reduces the formation of future dendrites. Conversely, low doses of the microtubule-stabilizing drug taxol shift polymerizing microtubules from neurite shafts to process tips and lead to the formation of multiple axons. Finally, local stabilization of microtubules using a photoactivatable analogue of taxol induces axon formation from the activated area. Thus, local microtubule stabilization in one neurite is a physiological signal specifying neuronal polarization.

摘要

轴突形成是建立神经元极性的起始步骤。我们在此利用培养的海马神经元研究微管动力学在神经元极化中的作用。我们观察到,在轴突形成前单个神经突的轴干以及形态极化细胞的轴突中,微管稳定性增强。在操纵神经元极性调节因子、两性缺陷突触(SAD)激酶和糖原合酶激酶-3β后,极性丧失或多轴突形成与微管周转的特征性变化相关。一致地,改变微管动力学足以改变神经元极化。应用低剂量的微管去稳定药物诺考达唑可选择性减少未来树突的形成。相反,低剂量的微管稳定药物紫杉醇会使聚合的微管从神经突轴干转移到突起尖端,并导致多轴突形成。最后,使用紫杉醇的光激活类似物对微管进行局部稳定可诱导从激活区域形成轴突。因此,一个神经突中的局部微管稳定是指定神经元极化的生理信号。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c149/2234250/99f3ce4e830d/jcb1800619f01.jpg

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