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Formulation and In Vitro Characterization of Xanthan Gum-Based Sustained Release Matrix Tables of Isosorbide-5- Mononitrate

机译:基于黄原胶的异山梨醇-5-一硝酸酯缓释基质表的配制和体外表征

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摘要

In the present investigation an attempt has been made to increase therapeutic efficacy, to reduce frequency of administration and to improve patient compliance by developing a sustained release matrix tablets of isosorbide-5-mononitrate. Sustained release matrix tablets of isosorbide-5-mononitrate were developed by using different drug: polymer ratios, such in F1 (1:0.75), F2 (1:1), F3 (1:1.5), F4 (1:1.75) and F6 (1:2). Xanthan gum was used as matrix former and microcrystalline cellulose as diluent. All the lubricated formulations were compressed, using 8mm flat faced punches. Compressed tablets were evaluated for uniformity of weight, content of active ingredient, friability, hardness, thickness, in vitro dissolution study using basket method and swelling index. Each formulation showed compliance with pharmacopoeial standards. Among all formulations, F5 showed a greater sustained release pattern of drug over a 12 h period with 92.12% of drug being released. The kinetic studies showed that drug release follows the Higuchi model (r2 =0.9851). Korsemeyer and Peppas equation gave an n-value of 0.4566, which was close to 0.5, indicating that drug release follows the Fickian diffusion. Thus, xanthan gum can be used as an effective matrix former to extend the release of isosorbide-5-mononitrate. No significant difference was observed in the dissolution profile of optimized formulation, using basket and paddle apparatus.
机译:在本研究中,已尝试通过开发5-单硝酸异山梨酯的缓释基质片剂来提高治疗功效,减少给药频率并改善患者依从性。通过使用不同的药物:聚合物比例(例如F1(1:0.75),F2(1:1),F3(1:1.5),F4(1:1.75)和F6(1:2)。黄原胶用作基质形成剂,微晶纤维素用作稀释剂。所有润滑配方均使用8mm平面冲头压缩。评估压制片剂的重量均匀性,活性成分含量,易碎性,硬度,厚度,使用篮法的体外溶出度研究和溶胀指数。每种制剂均符合药典标准。在所有制剂中,F5在12小时内显示出更大的药物持续释放模式,其中92.12%的药物被释放。动力学研究表明,药物释放遵循Higuchi模型(r 2 = 0.9851)。 Korsemeyer和Peppas方程的n值为0.4566,接近0.5,表明药物释放遵循Fickian扩散。因此,黄原胶可用作有效的基质形成剂,以延长5-单硝酸异山梨酯的释放。使用篮式和桨式装置在优化配方的溶出曲线中未观察到显着差异。

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