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首页> 外文期刊>The Journal of Chemical Physics >Polarization-dependent fluorescence of proteins bound to nanopore-confined lipid bilayers
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Polarization-dependent fluorescence of proteins bound to nanopore-confined lipid bilayers

机译:与纳米孔受限的脂质双层结合的蛋白质的偏振依赖性荧光

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摘要

Lipid bilayers are essential structural component of biological membranes of all the living species: from viruses and bacteria to plants and humans. Biophysical and biochemical properties of such membranes are important for understanding physical mechanisms responsible for drug targeting. Binding events between proteins and the membrane may be ascertained by introducing fluorescence markers (chromophores) to the proteins. Here we describe a novel biosensing platform designed to enhance signals of these fluorescence markers. Nanoporous aluminum oxide membranes with and without gold (Au) surface coating have been employed for optical detection of bound conjugated streptavidin to biotinylated lipid bilayers - a model system that mimics protein docking to the membrane surface. Unexpectedly, it was found that fluorescence signals from such structures vary when pumped with E-polarized and H-polarized incident optical beams. The origin of the observed polarization-dependent effects and the implications for enhanced fluorescence detection in a biochip format are being discussed. (C) 2008 American Institute of Physics.
机译:脂质双层是所有生物物种生物膜必不可少的结构组成部分:从病毒和细菌到植物和人类。这种膜的生物物理和生化特性对于理解负责药物靶向的物理机制很重要。蛋白质和膜之间的结合事件可以通过向蛋白质中引入荧光标记(发色团)来确定。在这里,我们描述了一种新颖的生物传感平台,旨在增强这些荧光标记的信号。具有和不具有金(Au)表面涂层的纳米多孔氧化铝膜已用于光学检测结合的共轭链霉亲和素与生物素化脂质双层的结合-一种模拟蛋白质对接至膜表面的模型系统。出乎意料的是,发现当用E偏振和H偏振入射光束泵浦时,来自这种结构的荧光信号会变化。讨论了观察到的偏振依赖性效应的起源以及以生物芯片形式增强荧光检测的意义。 (C)2008美国物理研究所。

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