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首页> 外文期刊>Archives of Pharmacal Research >Optimization of promethazine theoclate fast dissolving tablet using pore forming technology by 3-factor, 3-level response surface-full factorial design
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Optimization of promethazine theoclate fast dissolving tablet using pore forming technology by 3-factor, 3-level response surface-full factorial design

机译:通过三因子,三级响应表面全因子设计,利用造孔技术优化异丙嗪茶碱速溶片的制备

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摘要

The present research work was undertaken to optimize and formulate Promethazine Theoclate as a fast dissolving tablet using pore forming technology that disintegrates or dissolves rapidly and offer a suitable approach for the treatment of nausea and vomiting. Fast dissolving tablets of Promethazine Theoclate was prepared by increasing the solubility i.e. using β-cyclodextrin, crospovidone, and menthol. A 33 full factorial design was employed to investigate the combined influence of these three independent variables, i.e., amount of menthol, crospovidone and β-cyclodextrin on disintegration time, percentage friability and percentage drug release after 5 min. In the optimization study, multiple regression analysis has revealed that an optimum amount of menthol, crospovidone and β-cyclodextrin gives a rapidly disintegrating/dissolving tablet. In order to prove the validity of the evolved mathematical model a checkpoint batch was also prepared. Optimized tablets were prepared with an optimum amount of β-cyclodextrin, menthol and crospovidone which disintegrated in the 30 s, having friability 0.599% and released drug 89% after 5 min.
机译:进行了本研究工作,以利用快速分解或溶解并提供合适的方法来治疗恶心和呕吐的成孔技术,来优化和配制异丙甲菊酯Theoclate作为速溶片剂。通过增加溶解度,即使用β-环糊精,交聚维酮和薄荷醇来制备异丙嗪甲磺酸盐的速溶片剂。采用3 3 全因子设计研究了薄荷,薄荷油,交联维酮和β-环糊精的含量这三个独立变量对崩解时间,脆碎度和5分钟后药物释放百分比的综合影响。 。在优化研究中,多元回归分析表明,薄荷醇,交聚维酮和β-环糊精的最适量可制得快速崩解/溶解的片剂。为了证明所发展的数学模型的有效性,还准备了一批检查点。用最适量的β-环糊精,薄荷醇和交聚维酮制备的优化片剂在30 s内崩解,脆性为0.599%,5分钟后释放89%。

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