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冷冻电镜解析 GluK3- 型谷氨酸受体神经递质结合域的结构动力学。

Structural dynamics of the GluK3-kainate receptor neurotransmitter binding domains revealed by cryo-EM.

机构信息

Laboratory of Membrane Protein Biology, National Centre for Cell Science, NCCS Complex, S. P. Pune University, Pune, Maharashtra 411007, India.

Bioinformatics Centre, S. P. Pune University, Pune, Maharashtra 411007, India.

出版信息

Int J Biol Macromol. 2020 Apr 15;149:1051-1058. doi: 10.1016/j.ijbiomac.2020.01.282. Epub 2020 Jan 30.

DOI:10.1016/j.ijbiomac.2020.01.282
PMID:32006583
Abstract

Kainate receptors belong to the ionotropic glutamate receptor family and play critical roles in the regulation of synaptic networks. The kainate receptor subunit GluK3 has unique functional properties and contributes to presynaptic facilitation at the hippocampal mossy fiber synapses along with roles at the post-synapses. To gain structural insights into the unique functional properties and dynamics of GluK3 receptor, we imaged them via electron microscopy in the apo-state and in complex with either agonist kainate or antagonist UBP301. Our analysis of all the GluK3 full-length structures not only provides insights into the receptor transitions between desensitized and closed states but also reveals a "non-classical" conformation of neurotransmitter binding domain in the closed-state distinct from that observed in AMPA and other kainate receptor structures. We show by molecular dynamics simulations that Asp759 influences the stability of the LBD dimers and hence could be responsible for the observed conformational variability and dynamics of the GluK3 via electron microscopy. Lower dimer stability could explain faster desensitization and low agonist sensitivity of GluK3. In overview, our work helps to associate biochemistry and physiology of GluK3 receptors with their structural biology and offers structural insights into the unique functional properties of these atypical receptors.

摘要

kainate 受体属于离子型谷氨酸受体家族,在调节突触网络方面发挥着关键作用。kainate 受体亚基 GluK3 具有独特的功能特性,除了在后突触中发挥作用外,还参与海马苔藓纤维突触的突触前易化。为了深入了解 GluK3 受体的独特功能特性和动力学,我们通过电子显微镜在apo 状态和与激动剂 kainate 或拮抗剂 UBP301 复合物中对其进行成像。我们对所有 GluK3 全长结构的分析不仅提供了对受体在脱敏和关闭状态之间的转变的深入了解,还揭示了在关闭状态下与 AMPA 和其他 kainate 受体结构中观察到的不同的“非经典”神经递质结合域构象。我们通过分子动力学模拟表明,Asp759 影响 LBD 二聚体的稳定性,因此可能是通过电子显微镜观察到的 GluK3 构象变异性和动力学的原因。较低的二聚体稳定性可以解释 GluK3 的脱敏更快和激动剂敏感性低。总的来说,我们的工作有助于将 GluK3 受体的生物化学和生理学与结构生物学联系起来,并为这些非典型受体的独特功能特性提供结构见解。

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