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Systematically optimized topical delivery system for Loperamide hydrochloride: Formulation design in vitro and in vivo biopharmaceutical evaluation

机译:盐酸洛哌丁胺的系统优化局部给药系统:制剂设计体内和体外生物药物评估

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摘要

This study aimed to develop a suitable topical delivery system containing diethylene glycol monoethyl ether (DGME) for Loperamide hydrochloride (Lop). Two factors, three levels Central-Composite design were applied by generating a quadratic polynomial equation to form contour plots and response surface for prediction of responses as two selected independent variables with EtOH-DGME ratio and EtOH concentration. The response variables flux and skin retention were determined in hairless mouse skin model. The selected optimum formulation was evaluated for the skin transport characteristics by developing dermatokinetic analysis model and the results demonstrated DGME improved the delivery of Lop into skin deep layers, which was further confirmed by confocal laser scanning microscopy (CLSM) study. skin permeation was found to have triphasic correlation with plasma AUC in the pharmacokinetic study. The correlation enabled the prediction of pharmacokinetic profile of Lop from permeation results. Therefore, the optimum formulation capable of enhancing Lop intracutaneous depot could be a candidate for topical delivery of Lop as analgesics.
机译:这项研究旨在开发一种适用于盐酸洛哌丁胺(Lop)的含有二甘醇单乙醚(DGME)的局部给药系统。通过生成二次多项式方程以形成等高线图和响应面来预测两个作为独立选择的具有EtOH-DGME比和EtOH浓度的独立变量的变量,从而应用了三级中央复合设计这两个因子。在无毛小鼠皮肤模型中确定反应变量通量和皮肤保留率。通过开发的皮肤动力学分析模型评估所选的最佳配方的皮肤运输特性,结果表明DGME改善了Lop向皮肤深层的递送,这已通过共聚焦激光扫描显微镜(CLSM)研究得到了进一步证实。在药代动力学研究中发现皮肤渗透与血浆AUC具有三重相关性。该相关性使得能够根据渗透结果预测Lop的药代动力学特征。因此,能够增强Lop皮内贮库的最佳制剂可以作为Lop的局部镇痛药。

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