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采用统计实验设计优化的氯沙坦与 Duolite AP143 复合物壳聚糖珠的体外和体内研究。

In vitro and in vivo studies on chitosan beads of losartan Duolite AP143 complex, optimized by using statistical experimental design.

机构信息

AISSMS College of Pharmacy, Shivajinagar, Pune 411001, India.

出版信息

AAPS PharmSciTech. 2009;10(3):743-51. doi: 10.1208/s12249-009-9254-x. Epub 2009 Jun 3.

Abstract

The aim of the present research work was to develop release modulated beads of losartan potassium complexed with anion exchange resin, Duolite AP143 (cholestyramine). Chitosan was selected as a hydrophilic polymer for the formation of beads which could sustain the release of the drug up to 12 h, along with drug resin complex (DRC). Chitosan beads were prepared using an in-liquid curing method by ionotropic cross-linking or interpolymer linkage with sodium tripolyphosphate (TPP). The formulation of the beads was optimized for entrapment efficiency and drug release using 3(2) full factorial design. The independent variables selected were DRC/chitosan and percent of TPP. The optimization model was validated for its performance characteristics. Studies revealed that as the concentration of chitosan and TPP was increased, entrapment efficiency and the drug release were found to increase and decrease, respectively. The swelling capacity of chitosan-TPP beads decreased with increasing concentration of TPP. The effect of chitosan concentration and percentage of TPP solution used for cross-linking on entrapment efficiency and drug release rate was extensively investigated. Optimized beads were subjected to in vivo studies in Wistar albino rats to determine the mean arterial blood pressure and compared with marketed formulation. The pharmacodynamic study demonstrates steady blood pressure control for optimized formulation as compared to fluctuated blood pressure for the marketed formulation.

摘要

本研究工作的目的是开发氯沙坦钾与阴离子交换树脂(考来烯胺)复合物的释放调节珠。壳聚糖被选择为亲水聚合物,用于形成珠体,可以将药物的释放持续 12 小时,同时还有药物树脂复合物(DRC)。壳聚糖珠通过离子交联或与三聚磷酸钠(TPP)的共聚内聚形成在液相中固化方法制备。使用 3(2)完全因子设计优化珠的包封效率和药物释放。选择的自变量是 DRC/壳聚糖和 TPP 的百分比。验证了优化模型的性能特征。研究表明,随着壳聚糖和 TPP 浓度的增加,包封效率和药物释放分别增加和减少。壳聚糖-TPP 珠的溶胀能力随 TPP 浓度的增加而降低。研究了壳聚糖浓度和用于交联的 TPP 溶液的百分比对包封效率和药物释放速率的影响。优化后的珠体进行了 Wistar 白化大鼠的体内研究,以确定平均动脉血压,并与市售制剂进行比较。药效学研究表明,与市售制剂的波动血压相比,优化制剂能稳定控制血压。

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