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反映两种配体竞争同一受体位点的结合数据的图形分析。

Graphical analysis of binding data reflecting competition between two ligands for the same acceptor sites.

作者信息

Harris S J, Winzor D J

机构信息

Department of Biochemistry, University of Queensland, St. Lucia, Australia.

出版信息

Anal Biochem. 1988 Mar;169(2):319-27. doi: 10.1016/0003-2697(88)90291-6.

Abstract

A theoretical expression is derived for the analysis of results from competitive binding studies in which two multivalent ligands compete for acceptor sites, and a linear transform is suggested for simple graphical representation and assessment of experimental results. The protocol is illustrated by application to competitive binding data, obtained by ultrafiltration, on the interactions of bovine serum albumin with two structurally similar organic anions, methyl orange and methyl red. In a second experimental study the present approach is then used to establish that lactate dehydrogenase and aldolase compete for the same myofibrillar sites of bovine cardiac muscle. Finally, numerically simulated behavior of systems with additional binding sites for either ligand is used to emphasize that the criterion for classical (complete) competition is agreement between an experimentally determined equilibrium constant for ligand binding and the apparent value deduced from competitive binding studies. Nevertheless, the present analysis of competitive binding data should still offer considerable scope for screening quantitatively the cross-reactivities of drug and antigen analogs for their respective specific protein-acceptor sites.

摘要

推导了一个理论表达式,用于分析竞争性结合研究的结果,其中两种多价配体竞争受体位点,并提出了一种线性变换,以便对实验结果进行简单的图形表示和评估。通过将该方法应用于通过超滤获得的竞争性结合数据,说明了牛血清白蛋白与两种结构相似的有机阴离子甲基橙和甲基红相互作用的实验过程。在第二项实验研究中,采用本方法确定乳酸脱氢酶和醛缩酶竞争牛心肌的相同肌原纤维位点。最后,利用对任一配体具有额外结合位点的系统的数值模拟行为,强调经典(完全)竞争的标准是实验测定的配体结合平衡常数与从竞争性结合研究推导的表观值之间的一致性。然而,目前对竞争性结合数据的分析仍应为定量筛选药物和抗原类似物对其各自特异性蛋白质受体位点的交叉反应性提供相当大的空间。

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