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TARP γ8 选择性 AMPA 受体治疗剂的调节机制。

Modulatory mechanisms of TARP γ8-selective AMPA receptor therapeutics.

机构信息

Neurobiology Division, MRC Laboratory of Molecular Biology, Cambridge, UK.

IST Austria, Klosterneuburg, Austria.

出版信息

Nat Commun. 2023 Mar 25;14(1):1659. doi: 10.1038/s41467-023-37259-5.

Abstract

AMPA glutamate receptors (AMPARs) mediate excitatory neurotransmission throughout the brain. Their signalling is uniquely diversified by brain region-specific auxiliary subunits, providing an opportunity for the development of selective therapeutics. AMPARs associated with TARP γ8 are enriched in the hippocampus, and are targets of emerging anti-epileptic drugs. To understand their therapeutic activity, we determined cryo-EM structures of the GluA1/2-γ8 receptor associated with three potent, chemically diverse ligands. We find that despite sharing a lipid-exposed and water-accessible binding pocket, drug action is differentially affected by binding-site mutants. Together with patch-clamp recordings and MD simulations we also demonstrate that ligand-triggered reorganisation of the AMPAR-TARP interface contributes to modulation. Unexpectedly, one ligand (JNJ-61432059) acts bifunctionally, negatively affecting GluA1 but exerting positive modulatory action on GluA2-containing AMPARs, in a TARP stoichiometry-dependent manner. These results further illuminate the action of TARPs, demonstrate the sensitive balance between positive and negative modulatory action, and provide a mechanistic platform for development of both positive and negative selective AMPAR modulators.

摘要

AMPA 谷氨酸受体 (AMPARs) 在整个大脑中介导兴奋性神经传递。它们的信号通过特定于脑区的辅助亚基进行独特的多样化,为选择性治疗药物的开发提供了机会。与 TARP γ8 相关的 AMPARs 在海马体中丰富,并成为新兴抗癫痫药物的靶点。为了了解它们的治疗活性,我们确定了与三种有效、化学性质不同的配体相关的 GluA1/2-γ8 受体的冷冻电镜结构。我们发现,尽管共享一个暴露于脂质和可及于水的结合口袋,但结合部位突变对药物作用的影响不同。结合膜片钳记录和 MD 模拟,我们还证明了配体触发的 AMPAR-TARP 界面的重排有助于调节。出乎意料的是,一种配体(JNJ-61432059)以双功能方式起作用,以 TARP 计量依赖性的方式对 GluA1 产生负向影响,但对包含 GluA2 的 AMPAR 产生正向调节作用。这些结果进一步阐明了 TARPs 的作用,展示了正向和负向调节作用之间敏感的平衡,并为正向和负向选择性 AMPAR 调节剂的开发提供了一个机制平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2701/10039940/525366bbcd21/41467_2023_37259_Fig1_HTML.jpg

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