非诺贝特纳米悬液的制备及在Beagle犬体内的生物利用度  被引量:3

Preparation and Bioavailability of Fenofi brate Nanosuspension in Beagle Dogs

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作  者:翁腾飞[1,2] 戚建平[2] 卢懿[2] 尹宗宁[1] 吴伟[2] 

机构地区:[1]四川大学华西药学院,四川成都610041 [2]复旦大学药学院,上海201203

出  处:《中国医药工业杂志》2014年第3期234-239,共6页Chinese Journal of Pharmaceuticals

基  金:上海市教委曙光计划(10SG05);教育部新世纪优秀人才支持计划(NCET-11-0114)

摘  要:采用沉淀法结合高压均质法制备非诺贝特纳米混悬液,利用单因素试验所得优化处方为:选择羟丙甲纤维素E3120 mg和十二烷基硫酸钠30 mg的组合为稳定剂,无水乙醇1 ml为有机溶剂,最高均质压力1 000 bar。所得制品粒径为(439.1±30)nm,多分散指数(PDI)为(0.226±0.015),?电位为(-28.3±0.8)mV。以市售胶囊(Lipanthyl)为参比制剂,考察纳米混悬液的体外溶出与Beagle犬的口服生物利用度。结果表明,制品在2和5 min时溶出度为76%和98%,溶出明显快于参比制剂(5和60 min时溶出度为8%和83%)。Beagle犬口服非诺贝特纳米混悬液后,t max显著缩短,c max和AUC0→t分别是Lipanthyl的8倍和6倍,相对生物利用度为598%。The fenofibrate nanosuspension was prepared by precipitation combined with high-pressure homogenization method. The optimal formulation was obtained by single factor method. The particle size, polydispersion index (PDI) and ξ potential of the optimal nanosuspension prepared with HPMC E3 120 mg and sodium dodecylsulfate (SDS) 30 mg as stabilizers, ethanol 1 ml as the organic solvent and the highest homogenization pressure of 1 000 bar were (439.1±30)nm, (0.226±0.015) and (-28.3±0.8)mV, respectively. The in vitro dissolution and oral bioavailability in Beagle dogs were investigated with the marketed capsule Lipanthyl~ as the reference preparation. The results showed that the release rate of fenofibrate from the nanosuspension was significantly higher than Lipanthyl. The cumulative dissolution at 2 and 5 rain were 76% and 98% for nanosuspension, while only 8% and 83% for Lipanthyl at 5 and 60 min. After oral administration of fenofibrate nanosuspension, the tmax of fenofibric acid was significantly reduced while the Cmax and AUC0-t, were increased by 8- and 6-fold, respectively, compared with Lipanthyl. The relative oral bioavailability of the nanosuspension was 598 %.

关 键 词:纳米混悬液 非诺贝特 难溶性药物 溶出 生物利用度 

分 类 号:R944.9[医药卫生—药剂学]

 

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