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通过乳液溶剂蒸发法对阿司匹林微胶囊从乙基纤维素、邻苯二甲酸醋酸纤维素及其混合物中的释放动力学研究。

Release kinetic studies of aspirin microcapsules from ethyl cellulose, cellulose acetate phthalate and their mixtures by emulsion solvent evaporation method.

作者信息

Dash Vikas, Mishra Sujeet K, Singh Manoj, Goyal Amit K, Rath Goutam

机构信息

Kanak Manjari Institute of Pharmaceutical Sciences, Chhend Colony, Rourkela, Orissa, India.

出版信息

Sci Pharm. 2010 Jan-Mar;78(1):93-101. doi: 10.3797/scipharm.0908-09. Epub 2009 Dec 19.

Abstract

The present study was oriented towards microencapsulation of aspirin and the study of its release kinetics. The desired encapsulation was achieved by emulsion solvent evaporation method using ethyl cellulose (EC), cellulose acetate phthalate (CAP) and their mixture (1:1) of polymeric constituents. Characterization of the formulations was performed by size, shape, drug loading efficiency and in-vitro drug release analysis. The in-vitro release profiles from different polymeric microcapsules were applied on different kinetic models. The prepared microcapsules were found free flowing and almost spherical in shape with particle sizes ranging from 300â700Îm, having a loading efficiency of 75â85%. The best fit model with the highest correlation coefficient was observed in Higuchi model, indicating diffusion controlled principle. The n value obtained from Korsemeyer-Peppas model varied between 0.5â0.7, confirming that the mechanism of drug release was diffusion controlled. Comparative studies revealed that the release of aspirin from EC microcapsules was slower as compared to that of CAP and their binary mixture.

摘要

本研究旨在对阿司匹林进行微囊化并研究其释放动力学。通过使用乙基纤维素(EC)、邻苯二甲酸醋酸纤维素(CAP)及其聚合物成分的混合物(1:1)的乳液溶剂蒸发法实现了所需的包封。通过尺寸、形状、载药效率和体外药物释放分析对制剂进行了表征。将不同聚合物微胶囊的体外释放曲线应用于不同的动力学模型。所制备的微胶囊呈自由流动状态,形状几乎为球形,粒径范围为300-700μm,载药效率为75-85%。在Higuchi模型中观察到相关性系数最高的最佳拟合模型,表明是扩散控制原理。从Korsemeyer-Peppas模型获得的n值在0.5-0.7之间变化,证实药物释放机制是扩散控制的。比较研究表明,与CAP及其二元混合物相比,阿司匹林从EC微胶囊中的释放较慢。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/917b/3002828/5cba497b8cfc/Scipharm.2010.78.93f1.jpg

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