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电泳数据的定量分析:新型曲线拟合方法及其在蛋白质 - DNA 结合常数测定中的应用

Quantitative analysis of electrophoresis data: novel curve fitting methodology and its application to the determination of a protein-DNA binding constant.

作者信息

Shadle S E, Allen D F, Guo H, Pogozelski W K, Bashkin J S, Tullius T D

机构信息

Department of Chemistry, The Johns Hopkins University, Baltimore, MD 21218, USA.

出版信息

Nucleic Acids Res. 1997 Feb 15;25(4):850-60. doi: 10.1093/nar/25.4.850.

Abstract

A computer program, GelExplorer, which uses a new methodology for obtaining quantitative information about electrophoresis has been developed. It provides a straightforward, easy-to-use graphical interface, and includes a number of features which offer significant advantages over existing methods for quantitative gel analysis. The method uses curve fitting with a nonlinear least-squares optimization to deconvolute overlapping bands. Unlike most curve fitting approaches, the data is treated in two dimensions, fitting all the data across the entire width of the lane. This allows for accurate determination of the intensities of individual, overlapping bands, and in particular allows imperfectly shaped bands to be accurately modeled. Experiments described in this paper demonstrate empirically that the Lorentzian lineshape reproduces the contours of an individual gel band and provides a better model than the Gaussian function for curve fitting of electrophoresis bands. Results from several fitting applications are presented and a discussion of the sources and magnitudes of uncertainties in the results is included. Finally, the method is applied to the quantitative analysis of a hydroxyl radical footprint titration experiment to obtain the free energy of binding of the lambda repressor protein to the OR1 operator DNA sequence.

摘要

已开发出一种名为GelExplorer的计算机程序,它采用了一种获取电泳定量信息的新方法。该程序提供了一个直接、易用的图形界面,并具备许多功能,与现有的定量凝胶分析方法相比具有显著优势。该方法使用非线性最小二乘法优化的曲线拟合来解卷积重叠条带。与大多数曲线拟合方法不同,数据在二维空间中处理,对泳道整个宽度上的所有数据进行拟合。这使得能够准确确定单个重叠条带的强度,特别是能够对形状不规则的条带进行精确建模。本文所述的实验通过经验证明,洛伦兹线形能够重现单个凝胶条带的轮廓,并且在电泳条带的曲线拟合方面比高斯函数提供了更好的模型。给出了几个拟合应用的结果,并对结果中不确定性的来源和大小进行了讨论。最后,该方法应用于羟基自由基足迹滴定实验的定量分析,以获得λ阻遏蛋白与OR1操纵子DNA序列结合的自由能。

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