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首页> 外文期刊>The Journal of Physiology >Structural determinants of interaction, trafficking and function in the ClC-2/MLC1 subunit GlialCAM involved in leukodystrophy
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Structural determinants of interaction, trafficking and function in the ClC-2/MLC1 subunit GlialCAM involved in leukodystrophy

机译:参与白细胞营养障碍的ClC-2 / MLC1亚基GlialCAM中相互作用,运输和功能的结构决定因素

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摘要

Mutations in the genes encoding the astrocytic protein MLC1, the cell adhesion molecule GlialCAM or the Cl- channel ClC-2 underlie human leukodystrophies. GlialCAM binds to itself, to MLC1 and to ClC-2, and directs these proteins to cell-cell contacts. In addition, GlialCAM dramatically activates ClC-2 mediated currents. In the present study, we used mutagenesis studies combined with functional and biochemical analyses to determine which parts of GlialCAM are required to perform these cellular functions. We found that the extracellular domain of GlialCAM is necessary for cell junction targeting and for mediating interactions with itself or with MLC1 and ClC-2. The C-terminus is also necessary for proper targeting to cell-cell junctions but is not required for the biochemical interaction. Finally, we identified the first three amino acids of the transmembrane segment of GlialCAM as being essential for the activation of ClC-2 currents but not for targeting or biochemical interaction. Our results provide new mechanistic insights concerning the regulation of the cell biology and function of MLC1 and ClC-2 by GlialCAM.
机译:编码星形细胞蛋白MLC1,细胞粘附分子GlialCAM或Cl通道ClC-2的基因突变是人类白细胞营养不良的基础。 GlialCAM与其自身,MLC1和ClC-2结合,并将这些蛋白质引导至细胞与细胞之间的接触。此外,GlialCAM还可以显着激活ClC-2介导的电流。在本研究中,我们将诱变研究与功能和生化分析相结合,以确定执行这些细胞功能所需的GlialCAM的哪些部分。我们发现,GlialCAM的胞外域对于细胞连接靶向以及介导与其自身或与MLC1和ClC-2的相互作用是必需的。 C末端对于正确靶向细胞-细胞连接也是必需的,但生化相互作用不是必需的。最后,我们确定了GlialCAM跨膜区段的前三个氨基酸对于激活ClC-2电流是必需的,但对于靶向或生化相互作用却不是必需的。我们的结果提供了有关GlialCAM调控MLC1和ClC-2的细胞生物学和功能的新机制的见解。

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