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首页> 外文期刊>Current Nutraceuticals. >Formulation and Evaluation of Isabgol and Liquorice-Based Nutraceuticals Floating Tablets for Management of Gastric Ulcer
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Formulation and Evaluation of Isabgol and Liquorice-Based Nutraceuticals Floating Tablets for Management of Gastric Ulcer

机译:制定和评估Isabgol和Liquorice-Based保健品浮动平板电脑胃溃疡的管理

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摘要

Background: Floating tablets extend drug residence time, enhance bioavailability and promote the delivery of local drugs to the stomach. With this objective, floating tablets were prepared for the treatment of gastric ulcers containing aqueous extract of liquorice and Isabgol. Methods: Tablets containing HPMC K100M (hydrophilic polymer), liquorice extract, sodium bicarbonate (gas generating agent), talc, and magnesium stearate were prepared using direct compression method. Physical parameters of formulations such as diameter, thickness, hardness, friability, weight uniformity, drug content, buoyancy time, dissolution, and the mechanism for drug release, were assessed. The formulations have been optimized based on buoyancy time and in-vitro drug release. Results: The diameter of all formulations was in the range 11.310-11.833 mm; thickness was in the range 4.02-4.071 mm. The hardness ranged from 3.1 to 3.4 kg/cm. All the formulations passed the USP requirements for friability and uniformity of weight. All tablet formulations had a buoyancy period of less than 5 min and throughout the research, the tablet stayed in floating condition. All tablet formulations were accompanied in drug discharge by zero-order kinetics and Korsmeyer-Peppas model. Conclusion: It was discovered that the optimized formulation was F7, which released 98.5 percent of the drug in 8 hr. in-vitro, while the buoyancy time was 3.5 min. For gastroretentive drug delivery systems, formulations containing Isabgol, sodium bicarbonate and HPMC K100 M in combination may be promising.
机译:背景:浮动平板电脑延长药物住所时间,提高生物利用度,促进交付当地药物胃。客观、浮动平板电脑准备的包含水治疗胃溃疡提取甘草和Isabgol。平板电脑包含HPMC K100M(亲水聚合物),甘草提取物、碳酸氢钠(气体生成代理)、滑石和镁硬脂酸是准备使用直接压缩方法。直径、厚度、硬度、易碎性、重量均匀性、药物含量、浮力,解散,药物释放机制,被评估。优化基于浮力时间和体外药物释放。配方范围在11.310 - -11.833毫米;厚度在4.02 - -4.071毫米。硬度范围从3.1到3.4公斤/厘米。配方通过了USP要求易碎性和统一的重量。配方有浮力小于5的时期分钟,整个研究,平板电脑在浮动状态。配方同时在药物排出零级动力学和Korsmeyer-Peppas模型。优化配方F7,发布98.5百分比在8小时的药物。gastroretentive浮力时间是3.5分钟。药物输送系统,配方包含Isabgol、碳酸氢钠和HPMC K100 M组合可能是有前途的。

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