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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Not all desensitizations are created equal: physiological evidence that AMPA receptor desensitization differs for kainate and glutamate.
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Not all desensitizations are created equal: physiological evidence that AMPA receptor desensitization differs for kainate and glutamate.

机译:并非所有脱敏作用都相同:生理证据表明,AMPA受体脱敏作用的海藻酸盐和谷氨酸盐有所不同。

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AMPA receptor-mediated responses to the agonist kainate differ from those of glutamate in two important respects. Glutamate is a full agonist that elicits strongly desensitizing responses, whereas kainate is a partial agonist with responses that are often described as weakly desensitizing or non-desensitizing. The efficacy of kainate relative to glutamate has previously been shown to be increased by mutations in the AMPA receptor ligand-binding cleft (Mano et al., 1996) and by coexpression with the auxiliary subunit stargazin (Tomita et al., 2005; Turetsky et al., 2005), but much less is known about factors that affect kainate desensitization. We therefore designed experiments to compare kainate and glutamate desensitization and efficacy in wild-type and mutant AMPA receptors expressed with and without stargazin in HEK293 cells. Desensitization to the two agonists was differentially affected by mutations in the helices participating in bonds between two subunits in the active state of the receptor (Sun et al., 2002), indicating that the protein interactions maintaining the stability of the dimer interface differ depending on which agonist is bound. Kainate efficacy was affected by factors distinct from ligand-binding cleft closure, including mutations in the dimer interface and channel vestibule as well as receptor composition. The increase in kainate responses for AMPA receptors coexpressed with stargazin was the result of both reduced kainate desensitization and increased kainate efficacy. These results provide critical new insights into the agonist dependence of both AMPA receptor activation and desensitization and the mechanism of the effects of stargazin on responses of partial agonists.
机译:AMPA受体介导的对激动剂红藻酸酯的反应在两个重要方面不同于谷氨酸。谷氨酸盐是引起强烈脱敏反应的完全激动剂,而海藻酸盐是具有通常被称为弱脱敏或非脱敏反应的部分激动剂。以前已证明,通过AMPA受体配体结合裂隙的突变(Mano等,1996)和与辅助亚基stargazin的共表达,可提高海藻酸盐相对于谷氨酸的功效(Tomita等,2005; Turetsky等)等人,2005),但是影响红藻氨酸脱敏的因素知之甚少。因此,我们设计了实验,以比较海藻酸盐和谷氨酸脱敏作用以及在HEK293细胞中有和没有stargazin表达的野生型和突变型AMPA受体中的功效。对两种激动剂的脱敏作用受到参与受体活性状态下两个亚基之间键合的螺旋突变的影响(Sun等,2002),表明维持二聚体界面稳定性的蛋白质相互作用因哪个激动剂被绑定。海藻酸盐的功效受不同于配体结合裂隙闭合的因素影响,包括二聚体界面和通道前庭的突变以及受体组成。与stargazin共表达的AMPA受体的海藻酸盐应答增加是海藻酸盐脱敏作用降低和海藻酸盐功效增加的结果。这些结果为AMPA受体激活和脱敏的激动剂依赖性以及stargazin对部分激动剂反应的作用机理提供了重要的新见解。

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