三维有序大孔壳聚糖/尼莫地平固体分散体的研究

李传筠; 黄敏霞; 闫占宽; 张帆; 姜同英<sup>*</sup>

引用本文:	李传筠,黄敏霞,闫占宽,张帆,姜同英.三维有序大孔壳聚糖/尼莫地平固体分散体的研究[J].中国现代应用药学,2014,31(8):957-961.
	LI Chuanjun,HUANG Minxia,YAN Zhankuan,ZHANG Fan,JIANG Tongying.Dissolution, Stability and Pharmacokinetics of Solid Dispersions Made from Three Dimensionally Ordered Macroporous Chitosan Matrix and Nimodipine[J].Chin J Mod Appl Pharm(中国现代应用药学),2014,31(8):957-961.

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三维有序大孔壳聚糖/尼莫地平固体分散体的研究
李传筠^1,2, 黄敏霞³, 闫占宽¹, 张帆¹, 姜同英²
1.江苏恒瑞医药股份有限公司，江苏连云港 222047;2.沈阳药科大学，沈阳 110016;3.浙江海正药业股份有限公司，浙江台州 318000

摘要:

目的制备孔径为470 nm的三维有序大孔壳聚糖/尼莫地平的固体分散体，研究其释药特点、稳定性和药动学。方法利用溶剂蒸发法制备固体分散体，通过药物释放试验考察固体分散体在模拟胃肠液介质中的释放行为；通过含量测定、X-射线衍射和溶出试验检查固体分散体的稳定性；大鼠分别给予自制固体分散体和市售片粉末，测定血药浓度。结果固体分散体在pH 6.8的介质中的溶出度明显比pH 1.2和pH 4.5介质中高，在梯度pH介质中的释药曲线类似阶梯型；结晶度和溶出度在考察时间内基本无变化；自制固体分散体的AUC_{0~12 h}是市售制剂的1.91倍，具有长效作用。结论自制固体分散体稳定性良好，能够提高尼莫地平的大鼠口服生物利用度。

关键词: 三维有序大孔壳聚糖固体分散体溶出稳定性尼莫地平

DOI：

分类号:TQ423.4

基金项目:国家重点基础研究发展计划项目(2009CB930300)；辽宁省教育厅重点实验室项目(LS2010161)

Dissolution, Stability and Pharmacokinetics of Solid Dispersions Made from Three Dimensionally Ordered Macroporous Chitosan Matrix and Nimodipine

LI Chuanjun^1,2, HUANG Minxia³, YAN Zhankuan¹, ZHANG Fan¹, JIANG Tongying²

1.Jiangsu Hengrui Medicine Co., Ltd., Lianyungang 222047, China;2.Shenyang Pharmaceutical University, Shenyang 110016, China;3.Zhejiang Hisun Pharmaceutical Co., Ltd., Taizhou 318000, China

Abstract:

OBJECTIVE To prepare solid dispersions containing chitosan matrix with three dimensionally ordered 470 nm macroporous and nimodipine (3D-CS/NMDP), investigate the drug release, stability and pharmacokinetics. METHODS The solid dispersions were prepared by solvent evaporating method. The drug release behaviors of the 3D-CS/NMDP solid dispersions in artificial gastrointestinal fluid were examined by dissolution experiments. The chemical, crystal and dissolution stability was determined by X-ray diffraction method and dissolution method respectively. After orally administrating the 3D-CS/NMDP solid dispersions and commercial preparations, the plasma drug concentration of rat was measured. RESULTS The dissolution of the solid dispersion in pH 6.8 medium was largely higher than that in pH 1.2 and pH 4.5 medium. Drug release curve in gradient pH media expressed Ladder type. The crystallinity and dissolution of the solid dispersion hardly changed in test period. The 3D-CS/NMDP solid dispersions had 1.91 times AUC_{0-12 h} of commercial preparations, and possessed prolonged action. CONCLUSION The self-made 3D-CS/NMDP solid dispersions have good stability, can markedly improve the bioavailability in rat after oral administration.

Key words: three dimensionally ordered macroporous chitosan solid dispersion dissolution stability nimodipine