首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >A novel approach for the control of drug release rate through hydrogel membrane: I. Effect of drug immobilization on drug release rate by copolymerization method.
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A novel approach for the control of drug release rate through hydrogel membrane: I. Effect of drug immobilization on drug release rate by copolymerization method.

机译:一种通过水凝胶膜控制药物释放速率的新方法:I.通过共聚方法固定化药物对药物释放速率的影响。

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Precise control of drug release rate in hydrogel drug delivery systems to better mimic physiological condition is a challenging research topic in development of Advanced Drug Delivery Systems. One of the major issues with bioresponsive drug delivery systems is the excessive 'leakage' of drug while the system is in the 'off' state, which leads to shortening of the device life-time and potential overdose problem for the patient. In the present study, a new approach, based on partition effects, termed drug immobilization via copolymerization, is proposed to control the drug release rate of membrane-based drug delivery systems. In this method, a certain level of drug is pre-immobilized in the membrane through copolymerization. The immobilized drug contributes to the overall chemical potential of drug molecules in the membrane but their mobility is restricted, hence will not be released. At equilibrium, the amount of drug from donor that dissolved in the membrane is reduced due to contribution of immobilized drug, resulting in an effective reduction in partition coefficient and hence the release rate. The testing of the method by bovine serum albumin (BSA) as a model drug confirmed the controllability of the method: almost 35% reduction of the drug leakage in the 'off-state' was observed when 20mg BSA was immobilized in the pH-sensitive hydrogel membrane. The mathematical model of the drug partition in the membrane was modified to describe the new partition phenomenon (mobile drug and immobilized drug in the membrane) in this study.
机译:精确控制水凝胶药物输送系统中的药物释放速率以更好地模拟生理状况是高级药物输送系统开发中的一项具有挑战性的研究课题。生物响应性药物输送系统的主要问题之一是系统处于“关闭”状态时药物的过多“泄漏”,这会缩短设备的使用寿命并给患者带来潜在的用药过量问题。在本研究中,提出了一种基于分配效应的新方法,称为通过共聚固定药物,以控制基于膜的药物递送系统的药物释放速率。在这种方法中,一定水平的药物通过共聚预先固定在膜上。固定化的药物有助于膜中药物分子的整体化学势,但它们的活动性受到限制,因此不会被释放。在平衡时,由于固定化药物的贡献,减少了来自供体的溶解在膜中的药物量,导致分配系数和释放速率的有效降低。用牛血清白蛋白(BSA)作为模型药物对该方法进行的测试证实了该方法的可控性:当将20mg BSA固定在pH敏感型溶液中时,在“关闭状态”观察到的药物泄漏减少了近35%。水凝胶膜。修改了膜中药物分配的数学模型,以描述本研究中的新分配现象(膜中的流动药物和固定药物)。

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