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作 者:苏卫[1] 陈鹰[1,2] 董少华[3] 胡晓[3] 胡静波[1]
机构地区:[1]南方医科大学,广州510515 [2]广州军区武汉总医院 [3]湖北中医药大学
出 处:《中国药师》2013年第4期516-520,共5页China Pharmacist
摘 要:目的:研制尼莫地平(nimodipine,NM)自微乳化释药系统(SMEDDS)。方法:以溶解度,相容性试验、自乳化效率及伪三元相图法筛选最佳油相、表面活性剂及助表面活性剂;以星点设计-效应面法优化处方;对NM-SMEDDS分散后粒径、体外溶出度及初步稳定性进行考察。结果:经处方筛选和星点效应面法优化得出最佳处方为:Captex200P,Cremophor EL,Labrosol分别为油相,乳化剂和助乳化剂,比例为30∶47∶23;NM-SMEDDS的粒径分别为33.8±3.42 nm,1 h累积溶出百分率为98.83%,约为市售片剂的3.84倍;经高温(60℃)、低温(4℃)、强光(4 500±500)Lx考察10 d,除强光可引起NM含量降低外,其他各项指标均无明显变化。结论:该处方及工艺筛选、优化法简便可行,容易控制,制备得到的NM-SMEDDS体外溶出度显著增加,稳定性较好,为进一步研发尼莫地平新制剂提供了理论和试验基础。Objective: To prepare nimodipine self-microemulsifying drug delivery system (NM-SMEDDS). Method: The optimal oil phase, surfactant and cosurfactant of NM-SMEDDS were screened using solubility, compatibility, self-microemulsifying efficiency and pseudo-ternary phase diagram as the evaluation indices and method. The formula was optimized by central composite design-re- sponse surface methodology. The microemulsion particle size after dispersion, dissolution and preliminary stability of NM-SMEDDS were determined. Result: The optimal formula consisted of Captex200P, Cremophor EL and Labrasol as the oil phase, surfactant and cosurfactant, respectively with the ratio of 30: 47: 23. The particle diameter of NM-SMEDDS was(33.8 ± 3.42) nm. The accumulative dissolution of NM-SMEDDS was 98.83% , which was about 3.84 times as much as that of the marketed tablets. There was no obvious change under the conditions of high temperature (60℃), low temperature (4℃) and strong light (4 500 ± 500 Lx) in 10 days except the content decrease in strong light. Conclusion: The optimal preparation method is simple, feasible and easy to control. The dissolu-tion of NM is significantly imoroved by NM-SMEDDS with better stability. It can orovide the foundation for the new dosaze form of NM.
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