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乙酰胆碱受体的拓扑重排改变通道动力学。

Topographical rearrangement of acetylcholine receptors alters channel kinetics.

作者信息

Young S H, Poo M M

出版信息

Nature. 1983;304(5922):161-3. doi: 10.1038/304161a0.

Abstract

Plasma membranes are dynamic structures of proteins and lipids. Protein-protein or protein-lipid interactions within the membrane are believed to have important roles in many membrane functions, including ion transport, enzyme activity and signal reception. The acetylcholine (ACh) receptor-channel complex in skeletal muscle membrane is one of the best known integral membrane proteins. Its ion transport function is accessible to direct measurement at the single-channel level by the use of the 'giga-seal' patch recording technique. Here we used an in situ electrophoresis technique to rearrange the topography of pre-existing ACh receptor-channels in the muscle membrane, and measured the single-channel kinetics of ACh-activated channels in two different molecular environments within the membrane: those in the diffusely distributed region and those in the ACh receptor clusters induced by the applied field. We found that the channel kinetics are significantly prolonged in the ACh receptor cluster compared with the non-clustered region of the same cell. This result strongly supports the notion that the function of a membrane ionic channel depends on the local molecular environment.

摘要

质膜是由蛋白质和脂质构成的动态结构。膜内的蛋白质-蛋白质或蛋白质-脂质相互作用被认为在许多膜功能中发挥重要作用,包括离子运输、酶活性和信号接收。骨骼肌膜中的乙酰胆碱(ACh)受体通道复合物是最著名的整合膜蛋白之一。通过使用“千兆封接”膜片钳记录技术,可以在单通道水平直接测量其离子运输功能。在这里,我们使用原位电泳技术重新排列肌肉膜中预先存在的ACh受体通道的拓扑结构,并测量膜内两种不同分子环境中ACh激活通道的单通道动力学:分散分布区域中的通道和外加电场诱导的ACh受体簇中的通道。我们发现,与同一细胞的非簇集区域相比,ACh受体簇中的通道动力学显著延长。这一结果有力地支持了膜离子通道的功能取决于局部分子环境这一观点。

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