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双皮质素和双皮质素样激酶在调节生长锥微管中的新作用。

A novel role for doublecortin and doublecortin-like kinase in regulating growth cone microtubules.

机构信息

Department of Neurobiology and Anatomy, Drexel University College of Medicine, Philadelphia, PA 19129, USA.

出版信息

Hum Mol Genet. 2012 Dec 15;21(26):5511-27. doi: 10.1093/hmg/dds395. Epub 2012 Sep 21.

Abstract

Doublecortin (DCX) and doublecortin-like kinase (DCLK), closely related family members, are microtubule-associated proteins with overlapping functions in both neuronal migration and axonal outgrowth. In growing axons, these proteins appear to have their primary functions in the growth cone. Here, we used siRNA to deplete these proteins from cultured rat sympathetic neurons. Normally, microtubules in the growth cone exhibit a gently curved contour as they extend from the base of the cone toward its periphery. However, following depletion of DCX and DCLK, microtubules throughout the growth cone become much more curvy, with many microtubules exhibiting multiple prominent bends over relatively short distances, creating a configuration that we termed wave-like folds. Microtubules with these folds appeared as if they were buckling in response to powerful forces. Indeed, inhibition of myosin-II, which generates forces on the actin cytoskeleton to push microtubules in the growth cone back toward the axonal shaft, significantly decreases the frequency of these wave-like folds. In addition, in the absence of DCX and DCLK, the depth of microtubule invasion into filopodia is reduced compared with controls, and at a functional level, growth cone responses to substrate guidance cues are altered. Conversely, overexpression of DCX results in microtubules that are straighter than usual, suggesting that higher levels of these proteins can enable an even greater resistance to folding. These findings support a role for DCX and DCLK in enabling microtubules to overcome retrograde actin-based forces, thereby facilitating the ability of the growth cone to carry out its crucial path-finding functions.

摘要

双皮质素 (DCX) 和双皮质素样激酶 (DCLK) 是密切相关的家族成员,它们是微管相关蛋白,在神经元迁移和轴突生长中具有重叠的功能。在生长轴突中,这些蛋白似乎主要在生长锥中发挥作用。在这里,我们使用 siRNA 从培养的大鼠交感神经元中耗尽这些蛋白。正常情况下,生长锥中的微管在从锥底延伸到其外围时呈现出轻微弯曲的轮廓。然而,在耗尽 DCX 和 DCLK 后,整个生长锥中的微管变得更加弯曲,许多微管在相对较短的距离内呈现出多个明显的弯曲,形成了我们称之为波浪状褶皱的结构。这些褶皱的微管似乎在响应强大的力而弯曲。事实上,肌球蛋白 II 的抑制作用会在生长锥的肌动蛋白细胞骨架上产生力,将微管推向轴突干,这显著降低了这些波浪状褶皱的频率。此外,在没有 DCX 和 DCLK 的情况下,与对照组相比,微管侵入丝状伪足的深度减小,并且在功能水平上,生长锥对基质导向线索的反应发生改变。相反,DCX 的过表达导致微管比正常情况下更直,这表明这些蛋白的更高水平可以使微管更能抵抗折叠。这些发现支持了 DCX 和 DCLK 在使微管能够克服逆行肌动蛋白基力方面的作用,从而促进生长锥发挥其关键的寻路功能。

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