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Drug Release Profiles and Disintegration Properties of Pectin Films

机译:果胶薄膜的药物释放曲线和崩解特性

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摘要

We assessed the disintegration profiles of the film dosage forms (FDs) prepared using pectin by measuring the amount of pectin dissolved from the films in a limited amount of aqueous medium. Furthermore, we used miconazole and dexamethasone as standard drugs and investigated the relationship between the disintegration rate of the FDs and the rate of drug release. We used two types of pectin in this study to develop thin films with a thickness of approximately 25–35 μm. The FDs gradually disintegrated in the aqueous medium, and the disintegration profile of the FDs differed depending on the types of pectin. In addition, the rate of disintegration of the film matrix affected the dissolution rate of the drug incorporated into the FD. Thus, our results show that FDs prepared using pectin are beneficial because of their high solubility in a limited amount of medium, and the rate of drug release from the FDs can be regulated by selecting a specific type of pectin or by altering the concentration of the film base.
机译:我们通过测量在有限量的水性介质中从薄膜中溶解的果胶的量,评估了使用果胶制备的薄膜剂型(FDs)的崩解特性。此外,我们使用咪康唑和地塞米松作为标准药物,并研究了FDs崩解率与药物释放率之间的关系。在这项研究中,我们使用了两种类型的果胶来开发厚度约为25-35μm的薄膜。 FD在水性介质中逐渐崩解,并且FD的崩解曲线根据果胶的类型而不同。另外,膜基质的崩解速率影响掺入FD的药物的溶出速率。因此,我们的结果表明,使用果胶制备的FD具有很好的溶解性,因为它们在有限量的培养基中具有很高的溶解度,并且可以通过选择特定类型的果胶或通过改变果胶的浓度来调节从FD释放药物的速率。电影基地。

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