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小规模分子运动实现了人类谷氨酸转运体对谷氨酸的摄取。

Small-scale molecular motions accomplish glutamate uptake in human glutamate transporters.

作者信息

Koch Hans P, Larsson H Peter

机构信息

Neurological Sciences Institute, Oregon Health and Science University, Beaverton, Oregon 97006, USA.

出版信息

J Neurosci. 2005 Feb 16;25(7):1730-6. doi: 10.1523/JNEUROSCI.4138-04.2005.

Abstract

Glutamate transporters remove glutamate from the synaptic cleft to maintain efficient synaptic communication between neurons and to prevent glutamate concentrations from reaching neurotoxic levels. Glutamate transporters play an important role in ischemic neuronal death during stroke and have been implicated in epilepsy and amytropic lateral sclerosis. However, the molecular structure and the glutamate-uptake mechanism of these transporters are not well understood. The most recent models of glutamate transporters have three or five subunits, each with eight transmembrane domains, and one or two membrane-inserted loops. Here, using fluorescence resonance energy transfer (FRET) analysis, we have determined the relative position of the extracellular regions of these domains. Our results are consistent with a trimeric glutamate transporter with a large (>45 A) extracellular vestibule. In contrast to other transport proteins, our FRET measurements indicate that there are no large-scale motions in glutamate transporters and that glutamate uptake is accompanied by relatively small motions around the glutamate-binding sites. The large extracellular vestibule and the small-scale conformational changes could contribute to the fast kinetics predicted for glutamate transporters. Furthermore, we show that, despite the multimeric nature of glutamate transporters, the subunits function independently.

摘要

谷氨酸转运体从突触间隙清除谷氨酸,以维持神经元之间高效的突触通讯,并防止谷氨酸浓度达到神经毒性水平。谷氨酸转运体在中风期间的缺血性神经元死亡中起重要作用,并且与癫痫和肌萎缩侧索硬化症有关。然而,这些转运体的分子结构和谷氨酸摄取机制尚未完全了解。最新的谷氨酸转运体模型有三个或五个亚基,每个亚基有八个跨膜结构域,以及一个或两个插入膜内的环。在这里,我们使用荧光共振能量转移(FRET)分析,确定了这些结构域细胞外区域的相对位置。我们的结果与具有大的(>45 Å)细胞外前庭的三聚体谷氨酸转运体一致。与其他转运蛋白不同,我们的FRET测量表明谷氨酸转运体中没有大规模运动,并且谷氨酸摄取伴随着谷氨酸结合位点周围相对较小的运动。大的细胞外前庭和小规模的构象变化可能有助于谷氨酸转运体预测的快速动力学。此外,我们表明,尽管谷氨酸转运体具有多聚体性质,但亚基独立发挥功能。

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