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新型胶体给药系统ABCD与传统制剂在大鼠体内给药后两性霉素B的比较药代动力学。

Comparative pharmacokinetics of amphotericin B after administration of a novel colloidal delivery system, ABCD, and a conventional formulation to rats.

作者信息

Fielding R M, Smith P C, Wang L H, Porter J, Guo L S

机构信息

Liposome Technology, Inc., Menlo Park, California 94025.

出版信息

Antimicrob Agents Chemother. 1991 Jun;35(6):1208-13. doi: 10.1128/AAC.35.6.1208.

Abstract

The pharmacokinetics and tissue distribution of two amphotericin B dosage forms were compared in rats. A novel lipid-based colloidal delivery system for amphotericin B (Amphotericin B Colloidal Dispersion [ABCD]) which reduces the toxicity of amphotericin B in animals was compared with a conventional micellar formulation. Male Sprague-Dawley rats received a single intravenous injection of 1.0 mg of ABCD, 5.0 mg of ABCD, or 1.0 mg of micellar amphotericin B per kg. Plasma and tissue samples were obtained at 0.5 to 96 h after dosing and analyzed for amphotericin B by high-pressure liquid chromatography. Animals receiving ABCD demonstrated reduced peak levels in plasma, a three- to sevenfold reduction in amphotericin B delivery to the kidneys (the major target organ for toxicity), and prolonged residence time compared with those receiving the micellar formulation. In contrast, amphotericin B concentrations in the liver were two- to threefold higher with ABCD than with the micellar formulation: nearly 100% of the amphotericin B administered as ABCD was recovered from the liver 30 min after dosing. These results suggest that the colloidal particles of ABCD are taken up by the liver, which then acts as a reservoir of amphotericin B.

摘要

在大鼠中比较了两种两性霉素B剂型的药代动力学和组织分布。将一种新型的两性霉素B脂质胶体递送系统(两性霉素B胶体分散体[ABCD])与传统的胶束制剂进行了比较,该系统可降低两性霉素B在动物体内的毒性。雄性Sprague-Dawley大鼠每千克体重单次静脉注射1.0毫克ABCD、5.0毫克ABCD或1.0毫克胶束两性霉素B。给药后0.5至96小时采集血浆和组织样本,并用高压液相色谱法分析两性霉素B。与接受胶束制剂的动物相比,接受ABCD的动物血浆中的峰值水平降低,两性霉素B向肾脏(毒性的主要靶器官)的递送减少了三至七倍,并且停留时间延长。相比之下,ABCD组肝脏中的两性霉素B浓度比胶束制剂组高两至三倍:给药30分钟后,作为ABCD给药的两性霉素B几乎100%从肝脏中回收。这些结果表明,ABCD的胶体颗粒被肝脏摄取,然后肝脏充当两性霉素B的储存库。

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