丹皮酚-羟丙基-β-环糊精包合物的制备及处方工艺优化 点击下载
| 论文标题: | 丹皮酚-羟丙基-β-环糊精包合物的制备及处方工艺优化 |
| 英文标题: | |
| 中文摘要: | 目的:制备丹皮酚-羟丙基-β-环糊精(PAE-HP-β-CD)包合物,优化其处方工艺。方法:采用冷冻干燥法制备PAE- HP-β-CD包合物并进行验证。以包合率为指标,主药-辅料投料比、包合时间、包合温度与搅拌速度为因素,采用星点设计-响应面法优化其处方工艺。结果:制备的PAE-HP-β-CD包合物发生了物相转变。最优处方工艺为主药-辅料投料比3.39 ∶ 1、包合温度50 ℃、包合时间3.2 h、搅拌速度350 r/min;所制得包合物的包合率测得值(87.46%)与预测值(89.12%)的相对误差为1.86%(n=6)。结论:成功制得PAE-HP-β-CD包合物,且其处方工艺稳定可行。 |
| 英文摘要: | OBJECTIVE: To prepare paeonol-HP-β-cyclodextrin (PAE-HP-β-CD) inclusion compound and to optimize its prescription technology. METHODS: PAE-HP-β-CD was prepared by freeze drying method and validated. Using inclusion rate as index, main drug-accessory ratio, inclusion time, inclusion temperature and stirring speed as factors, the preparation technology was optimized by central composite design-response surface methodology. RESULTS: Prepared PAE-HP-β-CD underwent phase transformation. The optimal inclusion technology was as follows as main drug-accessory ratio of 3.39 ∶ 1, inclusion temperature of 50 ℃, inclusion time of 3.2 h, stirring speed of 350 r/min. Relative error between measured value (87.46%) and predicted value (89.12%) of inclusion rate was 1.86% (n=6). CONCLUSIONS: PAE-HP-β-CD inclusion compound is prepared successfully, and its prescription technology is stable and feasible. |
| 期刊: | 2017年第28卷第4期 |
| 作者: | 郑欣,杨培洪,何霖,陈希,程模,游必波 |
| 英文作者: | ZHENG Xin,YANG Peihong,HE Lin,CHEN Xi,CHENG Mo,YOU Bibo |
| 关键字: | 丹皮酚;羟丙基-β-环糊精;包合物;星点设计-响应面法;制备工艺;优化 |
| KEYWORDS: | Paeonol; HP-β-CD; Inclusion compound; Central composite design-response surface methodology; Prescription technology; Optimization |
| 总下载数: | 81次 |
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| 文件大小: | 619.60Kb |
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