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高效亲和色谱法分析与高密度脂蛋白的药物相互作用。

Analysis of drug interactions with high-density lipoprotein by high-performance affinity chromatography.

机构信息

Department of Chemistry, University of Nebraska, Lincoln, NE 68588-0304, USA.

出版信息

Anal Biochem. 2010 Feb 1;397(1):107-14. doi: 10.1016/j.ab.2009.10.017. Epub 2009 Oct 13.

Abstract

Columns containing immobilized lipoproteins were prepared for the analysis of drug interactions with these particles by high-performance affinity chromatography (HPAC). This approach was evaluated by using it to examine the binding of high-density lipoprotein (HDL) to the drugs propranolol and verapamil. HDL was immobilized by the Schiff base method onto silica and gave HPAC columns with reproducible binding to propranolol over 4-5days of continuous operation at pH 7.4. Frontal analysis experiments indicated that two types of interaction were occurring between R- or S-propranolol and HDL at 37 degrees C: saturable binding with an association equilibrium constant (K(a)) of 1.1-1.9x10(5)M(-1) and nonsaturable binding with an overall affinity constant (n K(a)) of 3.7-4.1x10(4)M(-1). Similar results were found at 4 and 27 degrees C. Verapamil also gave similar behavior, with a K(a) of 6.0x10(4) M(-1) at 37 degrees C for the saturable sites and an n K(a) for the nonsaturable sites of 2.5x10(4)M(-1). These measured affinities gave good agreement with solution phase values. The results indicated that HPAC can be used to study drug interactions with HDL, providing information that should be valuable in obtaining a better description of how drugs are transported within the body.

摘要

通过高效亲和色谱(HPAC),制备了含有固定化脂蛋白的柱子,用于分析这些粒子与药物的相互作用。通过使用该方法来研究高密度脂蛋白(HDL)与药物普萘洛尔和维拉帕米的结合,评估了这种方法。通过席夫碱法将 HDL 固定在硅胶上,得到了 HPAC 柱,在 pH 7.4 下连续运行 4-5 天,对普萘洛尔具有可重复的结合。前沿分析实验表明,R-或 S-普萘洛尔与 HDL 之间在 37 摄氏度下发生了两种类型的相互作用:饱和结合,其缔合平衡常数(K(a))为 1.1-1.9x10(5)M(-1),和非饱和结合,整体亲和常数(n K(a))为 3.7-4.1x10(4)M(-1)。在 4 和 27 摄氏度下也得到了类似的结果。维拉帕米也表现出类似的行为,在 37 摄氏度下,饱和部位的 K(a)为 6.0x10(4) M(-1),非饱和部位的 n K(a)为 2.5x10(4)M(-1)。这些测量的亲和力与溶液相值吻合较好。结果表明,HPAC 可用于研究与 HDL 的药物相互作用,提供的信息对于更好地描述药物在体内的运输方式应该是有价值的。

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