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基于表面等离子体激元的电生理学用于转运体研究。

SSM-Based Electrophysiology for Transporter Research.

作者信息

Bazzone Andre, Barthmes Maria, Fendler Klaus

机构信息

Max Planck Institute of Biophysics, Frankfurt/Main, Germany; Nanion Technologies GmbH, Munich, Germany.

Nanion Technologies GmbH, Munich, Germany.

出版信息

Methods Enzymol. 2017;594:31-83. doi: 10.1016/bs.mie.2017.05.008. Epub 2017 Jul 26.

Abstract

Functional characterization of transport proteins using conventional electrophysiology can be challenging, especially for low turnover transporters or transporters from bacteria and intracellular compartments. Solid-supported membrane (SSM)-based electrophysiology is a sensitive and cell-free assay technique for the characterization of electrogenic membrane proteins. Purified proteins reconstituted into proteoliposomes or membrane vesicles from cell culture or native tissues are adsorbed to the sensor holding an SSM. A substrate or a ligand is applied via rapid solution exchange. The electrogenic transporter activity charges the sensor, which is recorded as a transient current. The high stability of the SSM allows cumulative measurements on the same sensor using different experimental conditions. This allows the determination of kinetic properties including EC, IC, K, K, and rate constants of electrogenic reactions. About 100 different transporters have been measured so far using this technique, among them symporters, exchangers, uniporters, ATP-, redox-, and light-driven ion pumps, as well as receptors and ion channels. Different instruments apply this technique: the laboratory setups use a closed flow-through arrangement, while the commercially available SURFER N1 resembles a pipetting robot. For drug screening purposes high-throughput systems, such as the SURFER 96SE enable the simultaneous measurement of up to 96 sensors.

摘要

使用传统电生理学方法对转运蛋白进行功能表征可能具有挑战性,尤其是对于低周转率的转运蛋白或来自细菌和细胞内区室的转运蛋白。基于固体支持膜(SSM)的电生理学是一种用于表征生电膜蛋白的灵敏且无细胞的检测技术。从细胞培养物或天然组织中重组成蛋白脂质体或膜囊泡的纯化蛋白被吸附到装有SSM的传感器上。通过快速溶液交换施加底物或配体。生电转运蛋白活性使传感器带电,该电荷被记录为瞬态电流。SSM的高稳定性允许在相同传感器上使用不同实验条件进行累积测量。这使得能够确定包括电化学反应的EC、IC、K、K和速率常数在内的动力学性质。到目前为止,使用该技术已测量了约100种不同的转运蛋白,其中包括同向转运体、交换体、单向转运体、ATP驱动、氧化还原驱动和光驱动离子泵,以及受体和离子通道。不同的仪器应用该技术:实验室装置使用封闭的流通装置,而市售的SURFER N1类似于移液机器人。出于药物筛选目的,高通量系统,如SURFER 96SE能够同时测量多达96个传感器。

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