聚乳酸微胶囊胰岛素的微胶囊化与控释。

S Y Lin, L T Ho, H L Chiou
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引用次数: 36

摘要

采用乳化-溶剂蒸发工艺将胰岛素包被可生物降解的聚乳酸微胶囊和不可生物降解的乙基纤维素微胶囊。明胶和聚乙烯醇作为保护胶体。研究了保护胶体的浓度和种类对胰岛素微胶囊微粒化特性和释放行为的影响。保护胶体浓度越高,微胶囊的粒径越小。微胶囊的中位直径随着保护胶体粘度的增加而减小。扫描电镜观察表明,与明胶溶液制备的多孔微胶囊相比,高浓度聚乙烯醇溶液制备的微胶囊表面无孔且致密。微胶囊的残留晶体和多孔结构影响微胶囊的释放速度。在初始爆发效应后,胰岛素微胶囊的释放速率是恒定的,因此可以获得长时间的释放。3%的聚乙烯醇是制备聚乳酸微胶囊的最佳选择。
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Microencapsulation and controlled release of insulin from polylactic acid microcapsules.

Insulin has been encapsulated in biodegradable polylactic acid microcapsules and non-biodegradable ethylcellulose microcapsules by using an emulsification-solvent evaporation process. Gelatin and polyvinylalcohol were used as protective colloids. The concentrations and types of protective colloids affecting the micromeritic properties and release behavior of insulin microcapsules were studied. The higher the concentration of protective colloids the smaller the particle size of microcapsules. The median diameter of microcapsules decreased with the increase of the viscosity of protective colloids. Scanning electron microscopic observations suggested that microcapsules prepared from higher concentrations of polyvinylalcohol solution resulted in a nonporous and compact surface on the microcapsules, compared to the porous microcapsules prepared from gelatin solution. The residual crystals and porous structure of microcapsules affected the release rate of microcapsules. After the initial burst effect the release rate of insulin from microcapsules was found to be constant, so that prolonged release was obtainable. Three percent of polyvinylalcohol was the best choice for the preparation of polylactic acid microcapsules.

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