首页> 外文OA文献 >A quantitative study of the biospecific desorption of rat liver (M4) lactate dehydrogenase from 10-carboxydecylamino-Sepharose. Determination of the number of ligand-binding sites blocked on adsorption.
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A quantitative study of the biospecific desorption of rat liver (M4) lactate dehydrogenase from 10-carboxydecylamino-Sepharose. Determination of the number of ligand-binding sites blocked on adsorption.

机译:定量研究大鼠肝脏(M4)乳酸脱氢酶从10-羧基癸基氨基-琼脂糖中解吸的生物特异性。测定吸附时阻断的配体结合位点的数目。

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摘要

1. The theory of Nichol, Ogston, Winzor & Sawyer [(1974) Biochem. J. 143, 435-443] for quantitative affinity chromatography, when adapted for use with a non-specific column from which a multi-site protein can be specifically desorbed by its free ligand, permits determination of the concentration of adsorption sites on the column, their adsorptive affinity (as an association constant) and either the intrinsic (site) constant for ligand-binding to the protein or an 'occlusion coefficient' (defined as the number of ligand-binding sites blocked on adsorption), one of which must be known. 2. The theory has been applied to the NADH-specific desorption of rat liver M4 lactate dehydrogenase from 10-carboxydecylamino-Sepharose. It suggests that most of the enzyme molecules are adsorbed with at least two NADH-binding sites blocked, indicating an extensive adsorption interface in relation to the protein surface. Other chromatographic parameters were also determined for the system. 3. Among topics discussed are (a) factors affecting the experimentally determined value for the number of blocked sites, (b) the nature of the adsorption sites on the column and (c) the similarity of the analysis to that for determining Hill coefficients, and other possible applications.
机译:1. Nichol,Ogston,Winzor&Sawyer的理论[(1974)Biochem。 J. 143,435-443]用于定量亲和色谱法,当适合与非特异性色谱柱配合使用时,可以通过其游离配体将多位点蛋白特异性解吸,从而可以确定色谱柱上吸附位点的浓度,它们的吸附亲和力(作为缔合常数)以及配体与蛋白质结合的固有(位点)常数或“闭塞系数”(定义为吸附时被阻断的配体结合位点的数目),其中之一必须被知道。 2.该理论已应用于大鼠肝脏M4乳酸脱氢酶从10-羧基癸基氨基-琼脂糖中的NADH特异性解吸。这表明大多数酶分子被至少两个被限制的NADH结合位点吸附,表明相对于蛋白质表面而言广泛的吸附界面。还为系统确定了其他色谱参数。 3.讨论的议题包括(a)影响实验确定的封端位点值的因素,(b)色谱柱上吸附位点的性质,以及(c)分析与确定Hill系数的相似性,和其他可能的应用程序。

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    Kyprianou, P; Yon, R J;

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  • 年度 1982
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  • 正文语种 en
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