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与不同抗生物素蛋白类似物结合的[3H]生物素的药代动力学。

Pharmacokinetics of [3H]biotin bound to different avidin analogues.

作者信息

Kang Y S, Saito Y, Pardridge W M

机构信息

Department of Medicine, UCLA School of Medicine 90024-1682, USA.

出版信息

J Drug Target. 1995;3(2):159-65. doi: 10.3109/10611869509059215.

DOI:10.3109/10611869509059215
PMID:7496729
Abstract

The use of avidin-biotin technology in drug delivery facilitates the conjugation of biotinylated therapeutics to transport vectors that are enabled to undergo receptor-mediated transcytosis through the brain capillary endothelial wall, which makes up the blood-brain barrier (BBB) in vivo. However, the conjugation of avidin, a cationic glycosylated protein, to transport vectors greatly increases the rate of removal of the vector from the bloodstream, owing to rapid uptake of avidin by peripheral tissues such as liver and kidney. However, modified avidins may retain high affinity biotin binding properties, but may not be rapidly removed from plasma by peripheral tissues, and such avidin analogues would provide preferred plasma pharmacokinetic profiles. Therefore, the present studies investigate the pharmacokinetics of plasma removal of [3H]biotin bound to one of six different avidin analogues: streptavidin, Neutra-lite avidin, avidin, neutral avidin, Lite-avidin, and succinylated avidin. Isoelectric focusing studies show that avidin and Lite-avidin were highly cationic proteins, whereas neutral avidin, Neutra-lite avidin, and streptavidin were neutral proteins, and succinylated avidin had an acidic isoelectric point. The avidin analogues fell into two groups with respect to rate of biotin removal from plasma. The low clearance group included streptavidin and Neutra-lite avidin, which had a mean plasma clearance of 0.41 mL/min/kg. The high clearance group consisted of succinylated avidin, neutral avidin, and Lite-avidin and had a mean plasma clearance of 17 mL/min/kg, or 40-fold faster than the low clearance avidins.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

抗生物素蛋白-生物素技术在药物递送中的应用有助于将生物素化治疗药物与转运载体结合,这些转运载体能够通过构成体内血脑屏障(BBB)的脑毛细血管内皮壁进行受体介导的转胞吞作用。然而,抗生物素蛋白(一种阳离子糖蛋白)与转运载体的结合会大大提高载体从血液中清除的速率,这是因为肝脏和肾脏等外周组织会快速摄取抗生物素蛋白。不过,修饰后的抗生物素蛋白可能保留高亲和力的生物素结合特性,但不会被外周组织迅速从血浆中清除,此类抗生物素蛋白类似物将提供更理想的血浆药代动力学特征。因此,本研究考察了与六种不同抗生物素蛋白类似物之一结合的[3H]生物素在血浆中的清除药代动力学,这六种类似物分别是:链霉抗生物素蛋白、中性抗生物素蛋白、抗生物素蛋白、中性抗生物素蛋白、轻抗生物素蛋白和琥珀酰化抗生物素蛋白。等电聚焦研究表明,抗生物素蛋白和轻抗生物素蛋白是高度阳离子化的蛋白质,而中性抗生物素蛋白、中性抗生物素蛋白和链霉抗生物素蛋白是中性蛋白质,琥珀酰化抗生物素蛋白具有酸性等电点。就生物素从血浆中的清除速率而言,抗生物素蛋白类似物分为两组。低清除率组包括链霉抗生物素蛋白和中性抗生物素蛋白,其平均血浆清除率为0.41 mL/(min·kg)。高清除率组由琥珀酰化抗生物素蛋白、中性抗生物素蛋白和轻抗生物素蛋白组成,其平均血浆清除率为17 mL/(min·kg),比低清除率抗生物素蛋白快40倍。(摘要截短于250词)

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