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微管相关蛋白1B参与外周神经系统培养神经元轴突发生的初始阶段。

Microtubule-associated protein 1B is involved in the initial stages of axonogenesis in peripheral nervous system cultured neurons.

作者信息

Gonzalez-Billault Christian, Owen Rebecca, Gordon-Weeks Phillip R, Avila Jesus

机构信息

Centro de Biologia Molecular Severo Ochoa, UAM-CSIC, Campus Cantoblanco, 28049 Madrid, Spain.

出版信息

Brain Res. 2002 Jul 5;943(1):56-67. doi: 10.1016/s0006-8993(02)02534-9.

Abstract

Neuronal process extension is dependent on the reorganisation of the cytoskeleton, in particular microtubules and microfilaments, and one of the ways in which microtubules are regulated is by a group of microtubule-associated proteins called MAPs. MAP1B, the first MAP to be expressed in developing neurons, has been shown to play an important role during axonogenesis. Previously, we have shown that a phosphorylated isoform of MAP1B is involved in maintaining growth cone microtubules in a dynamically unstable state. In order to further investigate the role of MAP1B during axonogenesis we have cultured dorsal root ganglion (DRG) neurons from a MAP1B deficient mutant mouse. These mice express only trace amounts of MAP1B, have defects in the development of their nervous system and die perinatally. Cultured DRG neurons from MAP1B deficient mice show a reduction in axon elongation and an increase in growth cone area. The reduction in axon elongation is most likely to occur due to an inhibition in the early stages of axonogenesis. Using time-lapse video we have verified that during the first 2 h after plating, MAP1B deficient neurones extend their axons with an average speed that is half the speed of control neurones. These results support the participation of MAP1B during the initial stages of axonogenesis.

摘要

神经元突起的延伸依赖于细胞骨架的重组,尤其是微管和微丝,而微管调节的一种方式是通过一组称为微管相关蛋白(MAPs)来实现的。MAP1B是在发育中的神经元中最早表达的MAP,已被证明在轴突形成过程中起重要作用。此前,我们已经表明,MAP1B的一种磷酸化异构体参与将生长锥微管维持在动态不稳定状态。为了进一步研究MAP1B在轴突形成过程中的作用,我们从MAP1B缺陷突变小鼠中培养了背根神经节(DRG)神经元。这些小鼠仅表达微量的MAP1B,其神经系统发育存在缺陷,并在围产期死亡。来自MAP1B缺陷小鼠的培养DRG神经元显示轴突伸长减少,生长锥面积增加。轴突伸长的减少很可能是由于轴突形成早期的抑制作用。使用延时视频,我们已经证实,在接种后的最初2小时内,MAP1B缺陷神经元延伸其轴突的平均速度是对照神经元速度的一半。这些结果支持MAP1B在轴突形成初始阶段的参与。

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