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利用荧光寿命技术在筛选应用中提供高效的防误报保护。

Use of fluorescence lifetime technology to provide efficient protection from false hits in screening applications.

机构信息

Edinburgh Instruments, Kirkton Campus, Livingston, West Lothian EH54 7DQ, UK.

出版信息

Anal Biochem. 2011 Feb 1;409(1):89-97. doi: 10.1016/j.ab.2010.10.017. Epub 2010 Oct 21.

Abstract

This article describes novel data analysis of fluorescence lifetime-based protein kinase assays to identify and correct for compound interference in several practical cases. This ability, together with inherent advantages of fluorescence lifetime technology (FLT) as a homogeneous, antibody-free format independent of sample concentration, volume, excitation intensity, and geometry, makes fluorescence lifetime a practical alternative to the established "gold standards" of radiometric and mobility shift (Caliper) assays. The analysis is based on a photochemical model that sets constraints on the values of fluorescence lifetimes in the time responses of the assay. The addition of an exponential component with free floating lifetime to the constrained model, in which the lifetimes are constants predetermined from control measurements and the preexponential coefficients are "floating" parameters, allows the relative concentration of phosphorylated and nonphosphorylated substrates to be calculated even in the presence of compound fluorescence. The method is exemplified using both simulated data and experimental results measured from mixtures of dye-labeled phosphorylated and nonphosphorylated kinase substrates. A change of the fluorescence lifetime is achieved by the phosphorylated substrate-specific interaction with a bifunctional ligand, where one binding site interacts with the phosphate group and the other interacts with the dye.

摘要

本文描述了一种基于荧光寿命的新型蛋白激酶分析方法,用于在几种实际情况下识别和校正化合物干扰。这种能力,加上荧光寿命技术(FLT)作为一种均相、无需抗体的格式,独立于样品浓度、体积、激发强度和几何形状的固有优势,使得荧光寿命成为放射性和迁移率(Caliper)测定等既定“金标准”的实际替代方案。该分析基于一个光化学反应模型,该模型对测定时间响应中的荧光寿命值施加了约束。在受约束的模型中添加一个具有自由浮动寿命的指数分量,其中寿命是从对照测量中预先确定的常数,而预指数系数是“浮动”参数,即使在存在化合物荧光的情况下,也可以计算出磷酸化和非磷酸化底物的相对浓度。该方法使用模拟数据和从染料标记的磷酸化和非磷酸化激酶底物混合物中测量的实验结果进行了举例说明。荧光寿命的变化是通过磷酸化底物与双功能配体的特异性相互作用实现的,其中一个结合位点与磷酸基团相互作用,另一个与染料相互作用。

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