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由水性胶体聚合物分散体制备的微孔膜包衣片中氯化钾的持续释放。

Constant potassium chloride release from microporous membrane-coated tablets prepared with aqueous colloidal polymer dispersions.

作者信息

Bodmeier R, Paeratakul O

机构信息

College of Pharmacy, University of Texas, Austin 78712.

出版信息

Pharm Res. 1991 Mar;8(3):355-9. doi: 10.1023/a:1015897616351.

Abstract

To achieve constant drug release and to avoid the use of organic solvents, potassium chloride tablets were coated with aqueous latexes containing dispersed pore-formers with pH-dependent solubility characteristics. The pore-forming agent, dibasic calcium phosphate, was insoluble in the latex but soluble at low pH. Upon contact with simulated gastric fluids, it leached out rapidly to form a rate-controlling, microporous membrane. The release of potassium chloride was linear with time up to 75-80% drug released. It increased with increasing level of pore-former and decreasing membrane thickness but was independent of the degree of agitation and the pH of the dissolution medium after leaching of the pigments. Upon storage at different relative humidities, moisture uptake of the film coat and variations in the release profiles over time were minimal.

摘要

为实现药物的持续释放并避免使用有机溶剂,氯化钾片剂用含有具有pH依赖性溶解特性的分散成孔剂的水性乳胶进行包衣。成孔剂磷酸氢钙在乳胶中不溶,但在低pH下可溶。与模拟胃液接触后,它迅速浸出形成限速微孔膜。氯化钾的释放与时间呈线性关系,直至药物释放75-80%。它随着成孔剂水平的增加和膜厚度的减小而增加,但在色素浸出后与搅拌程度和溶解介质的pH无关。在不同相对湿度下储存时,薄膜包衣的吸湿量和释放曲线随时间的变化很小。

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