首页> 外文期刊>International Journal of Pharmaceutics >Zero-order delivery of a highly soluble, low dose drug alfuzosin hydrochloride via gastro-retentive system.
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Zero-order delivery of a highly soluble, low dose drug alfuzosin hydrochloride via gastro-retentive system.

机译:通过胃滞留系统零级递送高溶解度,低剂量的盐酸阿夫唑嗪药物。

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摘要

A composite gastro-retentive matrix for zero-order delivery of highly soluble drug alfuzosin hydrochloride (10mg) has been designed and characterized. Two systems containing polyethylene oxide (PEO), hydroxypropylmethylcellulose (HPMC), sodium bicarbonate, citric acid and polyvinyl pyrrolidone were dry blended and compressed into triple layer and bi-layer composite matrices. Dissolution studies using the USP 27 paddle method at 100 and 50rpm in pH 2.0 and 6.8 were performed using UV spectroscopy at 244nm, with automatic sampling over a 24h period using a marketed product as a reference to calculate the "f(2)" factor. Textural characteristics of each layer, the composite matrix as a whole, and floatation potential were determined under conditions similar to dissolution. Percent matrix swelling and erosion along with digital images were also obtained. Both systems proved to be effective in providing prolonged floatation, zero-order release, and complete disentanglement and erosion based on the analysis of data with "f(2)" of 68 and 71 for PEO and HPMC based systems, respectively. The kinetics of drug release, swelling and erosion, and dynamics of textural changes during dissolution for the designed composite systems offer a novel approach for developing gastro-retentive drug delivery system that has potential to enhance bioavailability and site-specific delivery to the proximal small intestine.
机译:设计并表征了一种用于零级递送高溶解度药物阿夫唑嗪盐酸盐(10mg)的复合胃滞留基质。将包含聚环氧乙烷(PEO),羟丙基甲基纤维素(HPMC),碳酸氢钠,柠檬酸和聚乙烯吡咯烷酮的两种体系干混,并压制成三层和双层复合基质。使用USP 27桨法在pH 2.0和6.8下以100和50rpm在244nm处进行溶出度研究,并使用市售产品作为参考在24小时内自动取样以计算“ f(2)”因子。在类似于溶解的条件下测定每一层的纹理特征,整个复合基质和漂浮势。还获得了百分比的基质膨胀和侵蚀以及数字图像。分别基于基于PEO和HPMC的系统的“ f(2)”分别为68和71的数据分析,两种系统均被证明可有效延长浮力,零级释放以及完全解缠和腐蚀。设计的复合系统的药物释放,溶胀和侵蚀动力学以及溶出过程中质地变化的动力学特性为开发胃滞留性药物输送系统提供了一种新颖的方法,该系统具有增强生物利用度和向近端小肠特定部位输送的潜力。 。

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