半自动化法制备盐酸二甲双胍不对称膜胶囊的统计优化及体外评价。

ISRN Pharmaceutics Pub Date : 2013-12-08 eCollection Date: 2013-01-01 DOI:10.1155/2013/719196
Venkatesh Teja Banala, Bharath Srinivasan, Deveswaran Rajamanickam, Basavaraj Basappa Veerbadraiah, Madhavan Varadarajan
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引用次数: 7

摘要

不对称膜胶囊(AMCs)是一种新型的渗透输送装置,它能以可控的方式输送多种药物。在本工作中,我们开发并验证了一种半自动工艺,通过制造液压辅助台式模型来制造amc。以乙酸丁酸纤维素(CAB)为包覆聚合物,丙二醇(PG)为增塑剂和成孔剂,采用浸涂相转化法制备了AMCs的囊壁。物理参数的比较检查证实了半自动过程的一致性、效率和可重复性优于手动过程。扫描电镜研究显示,一个薄的密集区域支持较厚的多孔膜的胶囊壳。以盐酸二甲双胍为模型药物,采用2(3)全因子设计,制备复方抗生素。采用Design-Expert 8.0.2(美国)软件研究PG浓度、果糖和氯化钾含量等处方变量对体外释药的影响。体外释放研究发现,孔前浓度和渗透剂水平对药物释放有直接影响。通过对优化处方(OPT)的验证研究发现,药物释放与pH和搅拌强度无关,而与溶解介质的渗透压有关。在13小时内,OPT遵循可控的零级释放动力学。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Statistical optimization and in vitro evaluation of metformin hydrochloride asymmetric membrane capsules prepared by a novel semiautomatic manufacturing approach.

Statistical optimization and in vitro evaluation of metformin hydrochloride asymmetric membrane capsules prepared by a novel semiautomatic manufacturing approach.

Statistical optimization and in vitro evaluation of metformin hydrochloride asymmetric membrane capsules prepared by a novel semiautomatic manufacturing approach.

Statistical optimization and in vitro evaluation of metformin hydrochloride asymmetric membrane capsules prepared by a novel semiautomatic manufacturing approach.

Asymmetric membrane capsules (AMCs) are one of the novel osmotic delivery devices which deliver a wide range of drugs in controlled manner. In the present work, we developed and validated a semiautomatic process by fabricating a hydraulic assisted bench top model for manufacturing AMCs. The capsule walls of AMCs were prepared by dip coating phase inversion process using cellulose acetate butyrate (CAB) as coating polymer and propylene glycol (PG) as plasticizer and pore former. The comparative examination of physical parameters confirmed the consistency, efficiency, and reproducibility of the semiautomatic process over the manual procedure. The SEM studies revealed a thin dense region supported on a thicker porous membrane of the capsule shells. Formulations of AMCs were prepared based on a 2(3) full factorial design using metformin hydrochloride as the model drug. The effect of formulation variables such as concentration of PG and levels of fructose and potassium chloride were studied on the in vitro drug release using Design-Expert 8.0.2 (USA) software. From the in vitro release studies, it was observed that the concentration of pore former and level of osmogents had a direct effect on the drug release. From the validation studies of the optimized formulation (OPT) with the predicted response, it was observed that the drug release was independent of pH and agitation intensity but dependent on osmotic pressure of the dissolution medium. The OPT followed controlled zero-order release kinetics over a period of 13 h.

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