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聚乳酸-聚乙二醇共聚物为载体的缓释疫苗微球的制备及特性研究
引用本文:徐希明,沈玉萍,余江南,皋古云,曹建平. 聚乳酸-聚乙二醇共聚物为载体的缓释疫苗微球的制备及特性研究[J]. 中国药学杂志, 2005, 40(14): 1080-1082
作者姓名:徐希明  沈玉萍  余江南  皋古云  曹建平
作者单位:1. 江苏大学药学院,江苏,镇江,212001
2. 中国疾病预防控制中心寄生虫病预防控制所,世界卫生组织疟疾、血吸虫病和丝虫病合作中心,卫生部寄生虫病原和媒介生物学重点实验室,上海,200025
基金项目:国家高技术研究发展计划(863计划)
摘    要: 目的制备缓释疫苗微球。方法以聚乳酸-聚乙二醇共聚物(PELA)为载体,醋酸乙酯为有机溶剂,采用W/O/W溶剂扩散法制备PELA疫苗微球。扫描电子显微镜观察微球的形态,激光散射技术测定其粒径分布;聚丙烯酰胺凝胶电泳(SDS- PAGE)研究微球包裹前后疫苗蛋白的稳定性;BCA法测定疫苗微球的载药量和包封率,同时考察疫苗微球的体外释药性能。结果所得微球呈类球形,平均粒径为5.38μm,疫苗微球载药量为5.12%,包封率达75.25%;包裹前后疫苗蛋白的结构稳定; 体外释药结果显示,疫苗微球前3 d以Higuchi方程(r=0.997 7)释放,3 d后则以零级恒速释放(r=0.992 2),28 d累积释药量为69.10%。结论以PELA为载体的疫苗微球具有较高的包封率、载药量和明显的缓释效果。

关 键 词:聚乳酸-聚乙二醇共聚物  微球  疫苗  缓释
文章编号:1001-2494(2005)14-1080-03
收稿时间:2004-12-10
修稿时间:2004-12-10

Preparation and characteristics of PELA-microspheres for vaccine sustained release
XU Xi-ming,SHEN Yu-ping,YU Jiang-nan,GAO Gu-yun,CAO Jian-ping. Preparation and characteristics of PELA-microspheres for vaccine sustained release[J]. Chinese Pharmaceutical Journal, 2005, 40(14): 1080-1082
Authors:XU Xi-ming  SHEN Yu-ping  YU Jiang-nan  GAO Gu-yun  CAO Jian-ping
Affiliation:1. School of Pharmacy,Jiangsu University,Zhenjiang 212001,China; 2. Institute of Parasitic Diseases,Chinese Center for Disease Control and Prevention,WHO Collaborating Center for Malaria,Schistosomiasis and Filariasis,Shanghai 200025,China
Abstract:OBJECTIVE To prepare the microspheres for vaccine sustained release.METHODS Microspheres containing vaccine were prepared by a modified W/O/W double emulsion-solvent diffusion method with poly-D,L-lactide-co-poly(ethylene glycol) (PELA) as carrier materials and ethyl acetate as organic solvent. Scanning electron microscopy was used for the observation of microspheres. Size distribution was determined by laser scattering technique. The stability of protein was evaluated by SDS-PAGE. The loading capacity and efficiency of vaccine in the microspheres were determined by BCA kits,which was also performed for the release of vaccine from microspheres in vitro.RESULTS Scanning electron micrographs showed that microspheres were almost spherical and the average diameter was about 5.38 μm. The loading capacity and encapsulation efficiency of vaccine in the microspheres was 5.12% and 75.25% , respectively. SDS-PAGE experiment suggested the protein was stable after being incorporated. In vitro release data were described with the following kinetic models: the release profile followed Higuchi equation in 0-3 day(r=0.997 7),the release profile, followed zero-order kinetic in 4-28 day(r=0.992 2). 69.10% Encapsulated vaccine was released over a period of 28 d. CONCLUSION The vaccine-loaded PELA microspheres were found to own a good loading capacity and efficiency,a remarkably sustained release of vaccine.
Keywords:poly-d  l-lactide-co-poly(ethylene glycol)  microspheres  vaccine  sustained release
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