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BINARY COMPLEXES OF GLIMEPIRIDE WITH p-CYCLODEXTRIN FOR IMPROVED SOLUBILITY AND DRUG DELIVERY

机译:具有p-Cyperodextrin的胶质脂体的二元络合物,提高溶解度和药物递送

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摘要

Cyclodextrin complexation is a one of the most investigated techniques of solubility and dissolution enhancement of drugs. In the present study, a poorly water soluble drug glimepiride, was complexed with p-cyclodextrin (PCD) with the aim of improving water solubility and drug dissolution. The complexes were prepared using two different methods (solvent evaporation and kneading) and then characterized by Fourier-transform infrared spectroscopy (FT-IR), powder x-ray diffractometry (X-RD), thermal analysis (DSC), scanning electron microscopy and in-vitro dissolution study. The phase solubility study revealed the most suitable ratio of drug to p CD (1:4 molar ratio). Analysis of various physical and pharmacoki-netic parameters for the complex prepared by solvent evaporation method showed better drug content, solubility and drug release profile in comparison to the complex prepared by the kneading method. The complex prepared with solvent evaporation method showed better drug release as compared with that of kneading method and the pure drug. The FT-IR, DSC and X-RD data also confirmed the results. It was concluded that complex prepared with (1:4 drug:pCD molar ratio) using solvent evaporation method showed the better improvement in solubility and drug dissolution.
机译:环糊精络合是药物的最溶解和溶解的最多的药物溶解技术之一。在本研究中,一种较差的水溶性药物胶质化素,与P-环糊精(PCD)络合,目的是改善水溶性和药物溶解。使用两种不同的方法(溶剂蒸发和捏合)制备配合物,然后通过傅里叶变换红外光谱(FT-IR),粉末X射线衍射法(X-RD),热分析(DSC),扫描电子显微镜和体外溶解研究。相溶解度研究显示出最合适的药物与P CD(1:4摩尔比)的比例。通过溶剂蒸发方法制备的复合物的各种物理和药物 - 近核参数的分析显示出更好的药物含量,溶解度和药物释放曲线与通过捏合方法制备的配合物相比。用溶剂蒸发方法制备的络合物显示出更好的药物释放,与捏合方法和纯药物相比。 FT-IR,DSC和X-RD数据也证实了结果。结论是使用溶剂蒸发方法的(1:4药物:PCD摩尔比)制备的复合物,表明溶解度和药物溶解的更好改善。

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