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作 者:时明[1,2] 朱来清[2] 孙庆雪[1] 王金萍[1] 黄桂华[1]
机构地区:[1]山东大学药学院,济南250012 [2]济宁市第一人民医院,山东济宁272011
出 处:《中国药房》2013年第45期4280-4283,共4页China Pharmacy
摘 要:目的:制备头孢匹胺钠脂质体并进行质量评价。方法:采用逆相蒸发法制备头孢匹胺钠脂质体,在单因素考察基础上,以药脂比(A)、磷脂与胆固醇质量比(B)、有机相(乙醚)与水相体积比(C)、超声时间(D)为因素,以包封率为考察指标,按L9(34)正交试验设计表优化最佳处方和工艺,并进行处方验证;考察脂质体的形态,测定其粒径、Zeta电位、包封率、载药量和72 h体外累积释放度并进行模型拟合。结果:正交试验设计优化的A为1∶6、B为5∶1、C为4∶1、D为5 min,验证试验证明处方合理;所得的脂质体为封闭的多层囊状或圆球体,大小均匀,平均粒径为(7.146±0.29)μm,Zeta电位为-11.75 mV,包封率为(82.10±4.21)%,载药量为(15.42±0.67)%;72 h体外累积释放度为76.84%,体外释药行为符合Weibull模型(r=0.991 0)。结论:采用逆相蒸发法制备的头孢匹胺钠脂质体,包封率较高,体外释药有明显的缓释效果。OBJECTIVE: To prepare Cefpiramide sodium liposome, and to evaluate its physicochemical property. METHODS: Cefpiramide sodium liposome was prepared by reverse phase evaporation method. Based on single factor test, the formulation and preparation technology were optimized by L^(34) orthogonal experiment with the ratio of drug to lipid (A), the ratio of phospha- tides to cholesterol (B), the ratio of organic phase (ether) to water phase (C) and ultrasound time (D) as factors using entrapment efficiency as index. The morphology of the liposome was investigated, and particle size, Zeta potential, entrapment efficiency, drug-loading amount and 72 h accumulative release rate in vitro were determined. RESULTS: The optimal formulation was as fol- lows : A was 1 : 6, B was 5 : 1, C was 4 : 1 and D was 5 rain. Validation test showed that the formulation was reasonable. Prepared liposome was closed multilayer cystiform or spherical shape, with uniform size. The mean diameter, Zeta potential, entrapment effi- ciency, drug-loading amount and 72 h accumulative release rate in vitro were ( 7.146 ± 0.29) gm, -- 11.75 mV, (82.10 ± 4.21 ) %, (15.42 ± 0.67)% and 76.84%, respectively. The drug release of the liposome was consistent with Weibull' s model (r=0.991 0). CONCLUSIONS: Cefpiramide sodium could be encapsulated liposome with higher encapsulation efficiency using reverse phase evaporation method, and the liposome has a good sustained-release property in vitro.
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