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四跨膜蛋白CD9是一种调节 paranodal 连接形成的新型 paranodal 成分。

Tetraspanin protein CD9 is a novel paranodal component regulating paranodal junctional formation.

作者信息

Ishibashi Tomoko, Ding Lei, Ikenaka Kazuhiro, Inoue Yoshiro, Miyado Kenji, Mekada Eisuke, Baba Hiroko

机构信息

Department of Molecular Neurobiology, School of Pharmacy, Tokyo University of Pharmacy and Life Science, Hachioji 192-0392, Japan.

出版信息

J Neurosci. 2004 Jan 7;24(1):96-102. doi: 10.1523/JNEUROSCI.1484-03.2004.

Abstract

The axoglial paranodal junction is essential for the proper localization of ion channels around the node of Ranvier. The integrity of this junction is important for nerve conduction. Although recent studies have made significant progress in understanding the molecular composition of the paranodal junction, it is not known how these membrane components are distributed to the appropriate sites and interact with each other. Here we show that CD9, a member of the tetraspanin family, is present at the paranode. CD9 is concentrated in the paranode as myelination proceeds, but CD9 clusters become diffuse, associated with disruption of the paranode, in cerebroside sulfotransferase-deficient mice. Immunohistochemical and Western blot analysis showed that CD9 is distributed predominantly in the PNS. Ablation of CD9 in mutant mice disrupts junctional attachment at the paranode and alters the paranodal components contactin-associated protein (also known as Paranodin) and neurofascin 155, although the frequency of such abnormalities varies among individuals and individual axons even in the same mouse. Electron micrographs demonstrated that compact myelin sheaths were also affected in the PNS. Therefore, CD9 is a myelin protein important for the formation of paranodal junctions. CD9 also plays a role in the formation of compact myelin in the PNS.

摘要

轴突胶质旁结对于离子通道在郎飞结周围的正确定位至关重要。该结的完整性对神经传导很重要。尽管最近的研究在理解旁结的分子组成方面取得了重大进展,但尚不清楚这些膜成分是如何分布到合适的位点并相互作用的。在这里,我们表明四跨膜蛋白家族成员CD9存在于旁结处。随着髓鞘形成过程的推进,CD9在旁结处聚集,但在脑苷脂硫酸转移酶缺陷小鼠中,CD9簇变得弥散,与旁结的破坏相关。免疫组织化学和蛋白质印迹分析表明,CD9主要分布在周围神经系统。在突变小鼠中敲除CD9会破坏旁结处的连接附着,并改变旁结成分接触蛋白相关蛋白(也称为旁结蛋白)和神经束蛋白155,尽管即使在同一只小鼠中,这种异常的频率在个体和单个轴突之间也有所不同。电子显微镜照片显示,周围神经系统中的紧密髓鞘也受到影响。因此,CD9是一种对旁结形成很重要的髓鞘蛋白。CD9在周围神经系统紧密髓鞘的形成中也发挥作用。

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