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谷氨酸转运体同源蛋白外门在结合共转运的钠离子时相对于底物发生相反的运动。

Opposite movement of the external gate of a glutamate transporter homolog upon binding cotransported sodium compared with substrate.

机构信息

Neuroscience Graduate Program, School of Medicine, Oregon Health and Science University, Beaverton, Oregon 97006-8921, USA.

出版信息

J Neurosci. 2011 Apr 20;31(16):6255-62. doi: 10.1523/JNEUROSCI.6096-10.2011.

DOI:10.1523/JNEUROSCI.6096-10.2011
PMID:21508248
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3096012/
Abstract

Recently, a new model for glutamate uptake by glutamate transporters was proposed based on crystal structures of the bacterial glutamate transporter homolog Glt(Ph). It was proposed that hairpin two (HP2) functions as the extracellular gate and that Na(+) and glutamate binding closes HP2, thereby allowing for the translocation of the glutamate binding pocket across the membrane. However, the conformation of HP2 in the apo state and the Na(+) bound state is unknown. We here use double site-directed spin-labeling electron paramagnetic resonance spectroscopy on the bacterial transporter Glt(Ph) from Pyrococcus horikoshi to examine conformational changes in HP2. Surprisingly, the cotransported substrates Na(+) and aspartate induce opposite movements of HP2. We find that in the apo state, HP2 is in a similar conformation as in the aspartate-bound closed state. Na(+) binding to the apo state opens HP2, whereas the subsequent binding of aspartate closes HP2. Our findings show that Na(+) binding opens and stabilizes the extracellular gate, thereby allowing for amino acid substrate binding. In contrast, in the absence of Na(+) and aspartate, HP2 closes, suggesting a potential mechanism for the translocation of the empty binding pocket necessary to complete the transport cycle. The finding that physiological Na(+) concentrations stabilize the open HP2 state would ensure that the outward-facing conformation of the transporter is maintained in physiological solutions and that glutamate transporters are ready to quickly bind glutamate released from glutamatergic synapses.

摘要

最近,基于细菌谷氨酸转运蛋白同源物 Glt(Ph) 的晶体结构,提出了一种谷氨酸转运体摄取谷氨酸的新模型。该模型提出发夹结构 2 (HP2) 作为细胞外门,Na(+) 和谷氨酸结合关闭 HP2,从而允许谷氨酸结合口袋跨膜转运。然而,HP2 在apo 状态和 Na(+) 结合状态下的构象尚不清楚。我们使用来自 Pyrococcus horikoshi 的细菌转运蛋白 Glt(Ph) 的双定点定向自旋标记电子顺磁共振波谱法来检查 HP2 的构象变化。令人惊讶的是,共转运的底物 Na(+) 和天冬氨酸诱导 HP2 的相反运动。我们发现,在 apo 状态下,HP2 处于与天冬氨酸结合的关闭状态相似的构象。Na(+) 结合到 apo 状态会打开 HP2,而随后结合天冬氨酸会关闭 HP2。我们的研究结果表明,Na(+) 结合打开并稳定细胞外门,从而允许氨基酸底物结合。相比之下,在没有 Na(+) 和天冬氨酸的情况下,HP2 关闭,这表明了转运蛋白完成转运循环所需的空结合口袋转运的潜在机制。发现生理 Na(+) 浓度稳定打开的 HP2 状态将确保转运蛋白的外向构象在生理溶液中得以维持,并且谷氨酸转运蛋白随时准备快速结合从谷氨酸能突触释放的谷氨酸。

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本文引用的文献

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Evidence for a third sodium-binding site in glutamate transporters suggests an ion/substrate coupling model.谷氨酸转运体中第三个钠离子结合位点的证据表明存在离子/底物偶联模型。
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