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首页> 外文期刊>Journal of Immunological Methods >A rigorous multiple independent binding site model for determining cell-based equilibrium dissociation constants.
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A rigorous multiple independent binding site model for determining cell-based equilibrium dissociation constants.

机译:用于确定基于细胞的平衡解离常数的严格的多重独立结合位点模型。

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摘要

A new 4-parameter nonlinear equation based on the standard multiple independent binding site model (MIBS) is presented for fitting cell-based ligand titration data in order to calculate the ligand/cell receptor equilibrium dissociation constant and the number of receptors/cell. The most commonly used linear (Scatchard Plot) or nonlinear 2-parameter model (a single binding site model found in commercial programs like Prism(R)) used for analysis of ligand/receptor binding data assumes only the K(D) influences the shape of the titration curve. We demonstrate using simulated data sets that, depending upon the cell surface receptor expression level, the number of cells titrated, and the magnitude of the K(D) being measured, this assumption of always being under K(D)-controlled conditions can be erroneous and can lead to unreliable estimates for the binding parameters. We also compare and contrast the fitting of simulated data sets to the commonly used cell-based binding equation versus our more rigorous 4-parameter nonlinear MIBS model. It is shown through these simulations that the new 4-parameter MIBS model, when used for cell-based titrations under optimal conditions, yields highly accurate estimates of all binding parameters and hence should be the preferred model to fit cell-based experimental nonlinear titration data.
机译:提出了一个基于标准多独立结合位点模型(MIBS)的新的4参数非线性方程,用于拟合基于细胞的配体滴定数据,以便计算配体/细胞受体平衡解离常数和受体/细胞数。用于分析配体/受体结合数据的最常用的线性(Scatchard图解)或非线性2参数模型(在商业程序中发现的单个结合位点模型,如Prism®)假设只有K(D)影响形状滴定曲线。我们证明了使用模拟的数据集,根据细胞表面受体表达水平,滴定的细胞数和被测K(D)的大小,始终处于K(D)控制条件下的这种假设可以错误,并可能导致对绑定参数的估计不可靠。我们还将比较和对比模拟数据集与常用的基于单元格的绑定方程的拟合与我们更严格的4参数非线性MIBS模型的对比。通过这些模拟表明,新的4参数MIBS模型在最佳条件下用于基于细胞的滴定时,可以对所有结合参数进行高度准确的估计,因此应成为适合基于细胞的实验非线性滴定数据的首选模型。

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