抗疟药物卤泛群主要与人血清中的低密度脂蛋白和高密度脂蛋白结合。
The antimalarial drug halofantrine is bound mainly to low and high density lipoproteins in human serum.
作者信息
Cenni B, Meyer J, Brandt R, Betschart B
机构信息
Department of Medical Parasitology, Swiss Tropical Institute, Basel.
出版信息
Br J Clin Pharmacol. 1995 May;39(5):519-26. doi: 10.1111/j.1365-2125.1995.tb04489.x.
Abstract
- The major serum proteins which bind halofantrine were identified by size exclusion chromatography. In addition, the binding affinity of halofantrine to human erythrocytes and serum proteins was measured by an erythrocyte partitioning technique. The influence of serum-drug binding on the distribution of halofantrine in whole blood was estimated by simulating several disease-related changes in the levels of the most important binding proteins. 2. The chromatographic resolution of serum preincubated with halofantrine allowed a quantitative analysis of binding to low density lipoproteins, high density lipoproteins, alpha 1-acid glycoprotein and albumin using the erythrocyte partitioning technique. Very low density lipoproteins did not bind halofantrine to a significant extent. 3. In whole blood halofantrine is bound to serum proteins (83%) and to erythrocytes (17%). Low density lipoproteins (affinity constant nKP = 44.4 l g-1) and high density lipoproteins (nKP = 14.4 l g-1) were the most important binding proteins in serum. alpha 1-acid glycoprotein (nKP = 4.39 l g-1) and albumin (nKP = 0.27 l g-1) had relatively low binding affinities. 4. The concentration of serum proteins influences both the fraction of unbound drug and the fraction of drug associated with the erythrocytes. Changes in serum protein concentrations often encountered in malaria are likely to increase both the unbound fraction and the fraction bound to the erythrocytes.
摘要
- 通过尺寸排阻色谱法鉴定了与卤泛群结合的主要血清蛋白。此外,采用红细胞分配技术测定了卤泛群与人红细胞和血清蛋白的结合亲和力。通过模拟几种与疾病相关的最重要结合蛋白水平变化,评估了血清-药物结合对卤泛群在全血中分布的影响。2. 用红细胞分配技术对与卤泛群预孵育的血清进行色谱分离,可定量分析其与低密度脂蛋白、高密度脂蛋白、α1-酸性糖蛋白和白蛋白的结合情况。极低密度脂蛋白与卤泛群的结合程度不显著。3. 在全血中,卤泛群与血清蛋白(83%)和红细胞(17%)结合。低密度脂蛋白(亲和常数nKP = 44.4 l g-1)和高密度脂蛋白(nKP = 14.4 l g-1)是血清中最重要的结合蛋白。α1-酸性糖蛋白(nKP = 4.39 l g-1)和白蛋白(nKP = 0.27 l g-1)的结合亲和力相对较低。4. 血清蛋白浓度会影响游离药物分数和与红细胞结合的药物分数。疟疾中常见的血清蛋白浓度变化可能会增加游离分数和与红细胞结合的分数。
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