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Development and In Vivo Floating Behavior of Verapamil HCl Intragastric Floating Tablets

机译:维拉帕米HCl胃内漂浮片的研制及体内漂浮行为。

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摘要

A novel gastro retentive controlled release drug delivery system of verapamil HCl was formulated in an effort to increase the gastric retention time of the dosage form and to control drug release. Hydroxypropylmethylcellulose (HPMC), carbopol, and xanthan gum were incorporated for gel-forming properties. Buoyancy was achieved by adding an effervescent mixture of sodium bicarbonate and anhydrous citric acid. In vitro drug release studies were performed, and drug release kinetics was evaluated using the linear regression method. The optimized intragastric floating tablet composed of 3:2 of HPMC K4M to xanthan gum exhibited 95.39% drug release in 24 h in vitro, while the buoyancy lag time was 36.2 s, and the intragastric floating tablet remained buoyant for >24 h. Zero-order and non-Fickian release transport was confirmed as the drug release mechanism from the optimized formulation (F7). X-ray studies showed that total buoyancy time was able to delay the gastric emptying of verapamil HCl intragastric floating tablet in mongrel dogs for more than 4 h. Optimized intragastric floating tablet showed no significant change in physical appearance, drug content, total buoyancy time, or in vitro dissolution pattern after storage at 40°C/75% relative humidity for 3 months.
机译:为了增加剂型在胃中的滞留时间并控制药物的释放,制定了维拉帕米盐酸盐的新型胃滞留控释药物递送系统。为了形成凝胶,并入了羟丙基甲基纤维素(HPMC),卡波姆和黄原胶。通过添加碳酸氢钠和无水柠檬酸的泡腾混合物来实现浮力。进行了体外药物释放研究,并使用线性回归方法评估了药物释放动力学。由HPMC K4M与黄原胶的3:2组成的优化的胃内漂浮片在体外24小时内显示95.39%的药物释放,而浮力滞后时间为36.2 s,并且胃内漂浮片保持浮力> 24小时。零级和非Fickian释放运输被确认为来自优化配方(F7)的药物释放机制。 X射线研究表明,总的浮力时间能够使杂种犬的维拉帕米HCl胃内漂浮片的胃排空延迟超过4小时。优化的胃内漂浮片剂在40°C / 75%相对湿度下存放3个月后,其物理外观,药物含量,总浮力时间或体外溶出度没有明显变化。

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