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星状蛋白差异调节苯丁胺类化合物的门控动力学和药理学。

Stargazin differentially modulates ampakine gating kinetics and pharmacology.

机构信息

RespireRx Pharmaceuticals Inc., 126 Valley Road, Glen Rock, NJ 07452, United States.

RespireRx Pharmaceuticals Inc., 126 Valley Road, Glen Rock, NJ 07452, United States.

出版信息

Biochem Pharmacol. 2018 Feb;148:308-314. doi: 10.1016/j.bcp.2018.01.019. Epub 2018 Jan 9.

DOI:10.1016/j.bcp.2018.01.019
PMID:29330065
Abstract

It was previously reported that Stargazin (STG) enhances the surface expression of AMPA receptors, controls receptor gating and slows channel desensitization as an auxiliary subunit of the receptors. Ampakines are a class of AMPA receptor positive allosteric modulators that modify rates of transmitter binding, channel activity and desensitization parameters. As such, they have shown efficacy in animal models of neurodegenerative diseases, where excitatory synaptic transmission is compromised. Given the functional similarities between STG and ampakines, the current study sought to probe interactions between STG and ampakine gating properties. The effects of the high impact ampakines, CX614 and cyclothiazide (CTZ), were compared with homomeric GluR1-flip (Glur1i) and GluR2-flop (Glur2o) receptors expressed in HEK293 cells by transient transfection with or without STG gene. STG dramatically enhanced the surface expression of AMPA receptors and increased glutamate-induced steady-state currents during desensitization. STG also increased ratios of 500 μM kainate and 500 μM glutamate activated steady-state currents. STG reduced association rates of ampakines and differentially affected the dissociation rates for both CX614 and CTZ on desensitized receptors. The estimated Kd value for CX614 was lowered from 340 μM to 70 μM, whereas that for CTZ was lowered from 170 μM to 6 μM by STG. The data suggest that Stargazin can dramatically alter the conformation of the receptor dimer interface where CX614 and CTZ are known to bind. This work also demonstrates the importance of considering STG interactions when developing ampakines to treat neurodegenerative diseases in which AMPAergic signaling is compromised.

摘要

先前有报道称,星状蛋白(STG)作为受体的辅助亚基,可增强 AMPA 受体的表面表达、控制受体门控并减缓通道脱敏。ampakines 是一类 AMPA 受体正变构调节剂,可改变递质结合、通道活性和脱敏参数的速率。因此,它们在兴奋性突触传递受损的神经退行性疾病动物模型中显示出疗效。鉴于 STG 和 ampakines 之间存在功能相似性,本研究旨在探究 STG 与 ampakines 门控特性之间的相互作用。通过瞬时转染,比较了高影响的ampakines(CX614 和 cyclothiazide,CTZ)与在 HEK293 细胞中表达的同型谷氨酸 1-翻转(Glur1i)和谷氨酸 2-翻转(Glur2o)受体之间的相互作用。STG 显著增强了 AMPA 受体的表面表达,并在脱敏过程中增加了谷氨酸诱导的稳态电流。STG 还增加了 500μM kainate 和 500μM 谷氨酸激活的稳态电流的比率。STG 降低了 ampakines 的结合速率,并对脱敏受体上 CX614 和 CTZ 的解离速率产生不同影响。STG 将 CX614 的估计 Kd 值从 340μM 降低到 70μM,而 CTZ 的 Kd 值从 170μM 降低到 6μM。数据表明,星状蛋白可以极大地改变受体二聚体界面的构象,已知 CX614 和 CTZ 在此处结合。这项工作还表明,在开发用于治疗 AMPA 能信号受损的神经退行性疾病的 ampakines 时,考虑 STG 相互作用非常重要。

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