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一种新型的基于苯丙氨酸的靶向信号将脑蛋白导向神经元树突。

A novel phenylalanine-based targeting signal directs telencephalin to neuronal dendrites.

作者信息

Mitsui Sachiko, Saito Michiko, Hayashi Ken, Mori Kensaku, Yoshihara Yoshihiro

机构信息

Laboratory for Neurobiology of Synapse, RIKEN Brain Science Institute, Wako, Saitama 351-0198, Japan.

出版信息

J Neurosci. 2005 Feb 2;25(5):1122-31. doi: 10.1523/JNEUROSCI.3853-04.2005.

Abstract

Neurons sort out a variety of functional molecules to appropriate subcellular destinations. Telencephalin (TLCN; intercellular adhesion molecule-5) is a cell adhesion molecule specifically localized to somatodendritic membranes in the telencephalic neurons. Here, we established a new in vivo strategy to analyze neuronal sorting mechanisms by ectopic expression of molecules of interest in the cerebellar Purkinje cells of transgenic mice. By using this system, we identified a novel dendritic targeting determinant in the cytoplasmic tail region of TLCN. A full-length TLCN ectopically expressed in the Purkinje cells was localized exclusively to dendrites but not to axons. In contrast, a deletion of cytoplasmic C-terminal 12 amino acids (residues 901-912) or a point mutation of Phe905 to Ala abrogated the dendrite-specific targeting with appearance of the truncated and point-mutated TLCN in both axons and dendrites. Furthermore, an addition of the C-terminal 17 amino acids (residues 896-912) of TLCN to an unrelated molecule (CD8) was sufficient for its specific targeting to dendrites in several types of neurons. Because the C-terminal region of TLCN does not contain any canonical dendritic targeting sequences such as the tyrosine-based motif or the dileucine motif, this study suggests a novel mechanism of protein trafficking to the dendritic compartment of neurons.

摘要

神经元将多种功能分子分选到合适的亚细胞位置。端脑啡肽(TLCN;细胞间粘附分子-5)是一种细胞粘附分子,特异性定位于端脑神经元的胞体树突膜。在此,我们建立了一种新的体内策略,通过在转基因小鼠的小脑浦肯野细胞中异位表达感兴趣的分子来分析神经元分选机制。利用该系统,我们在TLCN的胞质尾部区域鉴定出一种新的树突靶向决定因素。在浦肯野细胞中异位表达的全长TLCN仅定位于树突,而非轴突。相反,胞质C末端12个氨基酸(第901-912位残基)的缺失或Phe905突变为Ala的点突变消除了树突特异性靶向,截短和点突变的TLCN同时出现在轴突和树突中。此外,将TLCN的C末端17个氨基酸(第896-912位残基)添加到一个不相关的分子(CD8)上,足以使其在几种类型的神经元中特异性靶向树突。由于TLCN的C末端区域不包含任何典型的树突靶向序列,如基于酪氨酸的基序或双亮氨酸基序,本研究提示了一种蛋白质转运至神经元树突区室的新机制。

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