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The structure and function of glutamate receptor ion channels.

机译:谷氨酸受体离子通道的结构和功能。

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As in the case of many ligand-gated ion channels, the biochemical and electrophysiological properties of the ionotropic glutamate receptors have been studied extensively. Nevertheless, we still do not understand the molecular mechanisms that harness the free energy of agonist binding, first to drive channel opening, and then to allow the channel to close (desensitize) even though agonist remains bound. Recent crystallographic analyses of the ligand-binding domains of these receptors have identified conformational changes associated with agonist binding, yielding a working hypothesis of channel function. This opens the way to determining how the domains and subunits are assembled into an oligomeric channel, how the domains are connected, how the channel is formed, and where it is located relative to the ligand-binding domains, all of which govern the processes of channel activation and desensitization.
机译:与许多配体门控离子通道一样,离子型谷氨酸受体的生化和电生理特性已得到广泛研究。然而,我们仍然不了解利用激动剂结合的自由能的分子机制,首先驱动通道开放,然后即使激动剂保持结合,也允许通道关闭(脱敏)。这些受体的配体结合结构域的最新晶体学分析已经鉴定出与激动剂结合相关的构象变化,产生了通道功能的有效假设。这为确定域和亚基如何组装成寡聚通道,域如何连接,通道如何形成以及相对于配体结合域的位置开辟了道路,所有这些因素都决定着通道激活和脱敏。

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