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Development and optimization of dextromethorphan hydrobromide oral disintegrating tablets: effect of formulation and process variables.

机译:氢溴酸右美沙芬口腔崩解片的开发和优化:配方和工艺变量的影响。

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摘要

Orally disintegrating tablets (ODTs), which disintegrate rapidly (<1?min) in the mouth and do not require water for administration, have become a very popular dosage form. The study aims to develop a simple and inexpensive method of manufacturing ODTs of a sparingly water-soluble drug, Dextromethorphan hydrobromide. Two factors, three levels (3(2)) full factorial design was used to optimize the diluent, microcrystalline cellulose (X(1)) and superdisintegrant, croscarmellose sodium (X(2)) concentrations. Disintegration time, hardness and T(50) values for all the formulations varied from 12.5 to 152.6 s, 3.58 to 4.92 kp and 0.8 to 2.8?min, respectively. The results indicated that the selected variables have a strong influence on disintegration time, hardness and T(50) of the ODTs. The manufactured ODTs formula composed of 30% microcrystalline cellulose in combination with 3% croscarmellose sodium was chosen as optimized formula, as it showed the lowest disintegration time (12.5?±?1.22 s), low T(50) (0.8?min.) and hard tablets (4.92?±?0.28 kp) amongst other tested ODTs formulations. Hardness of DM ODTs was not affected by changing the type of superdisintegrant and lubricant. The disintegration time was significantly (p < 0.05) increased by using sodium starch glycolate instead of croscarmellose sodium.
机译:口腔崩解片(ODTs)在口腔中迅速崩解(<1分钟),不需要水来给药,已成为一种非常受欢迎的剂型。这项研究旨在开发一种简单而廉价的方法来生产微水溶性药物氢溴酸右美沙芬的ODT。两个因素,三个级别(3(2))全因子设计用于优化稀释剂,微晶纤维素(X(1))和超级崩解剂交联羧甲基纤维素钠(X(2))的浓度。所有配方的崩解时间,硬度和T(50)值分别为12.5至152.6 s,3.58至4.92 kp和0.8至2.8?min。结果表明,选择的变量对ODT的崩解时间,硬度和T(50)有很大的影响。选择由30%的微晶纤维素与3%的交联羧甲基纤维素钠组成的ODTs配方作为优化配方,因为它具有最短的崩解时间(12.5?±?1.22 s),低T(50)(0.8?min。)。以及其他经过测试的ODT配方中的硬片(4.92±±0.28 kp)。 DM ODT的硬度不受改变超级崩解剂和润滑剂类型的影响。通过使用淀粉羟乙酸钠代替交联羧甲基纤维素钠,崩解时间显着增加(p <0.05)。

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