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New insights into the molecular mechanisms of biomembrane structural changes and interactions by optical biosensor technology

机译:光学生物传感器技术对生物膜结构变化和相互作用的分子机制的新见解

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Biomolecular-membrane interactions play a critical role in the regulation of many important biological processes such as protein trafficking, cellular signalling and ion channel formation. Peptide/protein-membrane interactions can also destabilise and damage the membrane which can lead to cell death. Characterisation of the molecular details of these binding-mediated membrane destabilisation processes is therefore central to understanding cellular events such as antimicrobial action, membrane-mediated amyloid aggregation, and apoptotic protein induced mitochondrial membrane permeabilisation. Optical biosensors have provided a unique approach to characterising membrane interactions allowing quantitation of binding events and new insight into the kinetic mechanism of these interactions. One of the most commonly used optical biosensor technologies is surface plasmon resonance (SPR) and there have been an increasing number of studies reporting the use of this technique for investigating biophysical analysis of membrane-mediated events. More recently, a number of new optical biosensors based on waveguide techniques have been developed, allowing membrane structure changes to be measured simultaneously with mass binding measurements. These techniques include dual polarisation interferometry (DPI), plasmon waveguide resonance spectroscopy (PWR) and optical waveguide light mode spectroscopy (OWLS). These techniques have expanded the application of optical biosensors to allow the analysis of membrane structure changes during peptide and protein binding. This review provides a theoretical and practical overview of the application of biosensor technology with a specific focus on DPI, PWR and OWLS to study biomembrane-mediated events and the mechanism of biomembrane disruption. (C) 2015 Elsevier B.V. All rights reserved.
机译:生物分子-膜相互作用在许多重要的生物过程(例如蛋白质运输,细胞信号传导和离子通道形成)的调节中起着关键作用。肽/蛋白质-膜相互作用也会破坏膜并破坏膜,从而导致细胞死亡。因此,这些结合介导的膜去稳定过程的分子细节的表征对于理解细胞事件(如抗菌作用,膜介导的淀粉样蛋白聚集和凋亡蛋白诱导的线粒体膜通透性)至关重要。光学生物传感器提供了表征膜相互作用的独特方法,从而可以定量结合事件并深入了解这些相互作用的动力学机制。表面等离子体共振(SPR)是最常用的光学生物传感器技术之一,并且越来越多的研究报告称该技术用于研究膜介导事件的生物物理分析。最近,已经开发了许多基于波导技术的新型光学生物传感器,从而可以在进行质量结合测量的同时测量膜结构的变化。这些技术包括双极化干涉仪(DPI),等离激元波导共振光谱(PWR)和光波导光模光谱(OWLS)。这些技术扩展了光学生物传感器的应用,从而可以分析肽和蛋白质结合过程中的膜结构变化。这篇综述提供了生物传感器技术应用的理论和实践概述,特别侧重于DPI,PWR和OWLS,以研究生物膜介导的事件和生物膜破坏的机理。 (C)2015 Elsevier B.V.保留所有权利。

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