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Release Mechanisms Behind Polysaccharides-Based Famotidine Controlled Release Matrix Tablets

机译:多糖基法莫替丁控释基质片背后的释放机理

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摘要

Polysaccharides, which have been explored to possess gelling properties and a wide margin of safety, were used to formulate single-unit floating matrix tablets by a direct compression technique. This work has the aim to allow continuous slow release of famotidine above its site of absorption. The floating approach was achieved by the use of the low density polypropylene foam powder. Polysaccharides (κ-carrageenan, gellan gum, xyloglucan, and pectin) and blends of polysaccharides (κ-carrageenan and gellan gum) and cellulose ethers (hydroxypropylmethyl cellulose, hydroxypropylcellulose, sodium carboxymethyl cellulose) were tried to modulate the release characteristics. The prepared floating tablets were evaluated for their floating behavior, matrix integrity, swelling studies, in vitro drug release studies, and kinetic analysis of the release data. The differential scanning calorimetry and Fourier transform infrared spectroscopy studies revealed that changing the polymer matrix system by formulation of polymers blends resulted in formation of molecular interactions which may have implications on drug release characteristics. This was obvious from the retardation in drug release and change in its mechanistics.
机译:已开发出具有胶凝特性和宽泛的安全性的多糖,已通过直接压片技术用于配制单单位漂浮基质片剂。这项工作的目的是使法莫替丁在其吸收部位上方连续缓慢释放。浮法是通过使用低密度聚丙烯泡沫粉实现的。尝试了多糖(κ-角叉菜胶,结冷胶,木葡聚糖和果胶)以及多糖(κ-角叉菜胶和结冷胶)和纤维素醚(羟丙基甲基纤维素,羟丙基纤维素,羧甲基纤维素钠)的混合物来调节释放特性。评估所制备的漂浮片剂的漂浮行为,基质完整性,溶胀研究,体外药物释放研究以及释放数据的动力学分析。差示扫描量热法和傅里叶变换红外光谱研究表明,通过调配聚合物共混物来改变聚合物基质系统会导致分子相互作用的形成,这可能对药物释放特性产生影响。从药物释放的延迟和其机理的变化可以明显看出这一点。

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