海藻酸钠-壳聚糖P-VP8~*IgY微胶囊的制备及其释放性能  被引量：6

作　　者：谭文芳 郭伦爱 段文韬 戴迎春[2] 张绪富[1] TAN Wenfang;GUO Lunai;DUAN Wentao;DAI Yingchun;ZHANG Xufu(School of Traditional Chinese Medicine,Guangzhou 510515,China;Department of Epidemiology,School of Public ealth,Southern Medical University,Guangzhou 510515,China)

机构地区：[1]南方医科大学中医药学院,广东广州510515 [2]南方医科大学公共卫生学院流行病学系,广东广州510515

出　　处：《沈阳药科大学学报》2018年第10期825-830,共6页Journal of Shenyang Pharmaceutical University

基　　金：广州市科技计划项目产学研协同创新重大专项民生科技研究专题资助项目(201604020111);南方医科大学大学生创业训练计划资助项目(201712121210)

摘　　要：目的在前期试验成功制备纯化出抗诺如和轮状病毒的双价特异性P-VP8~*IgY基础上,本研究作者制备海藻酸钠-壳聚糖P-VP8~*IgY微胶囊并优化最佳制备工艺。方法以海藻酸钠-壳聚糖为微胶囊囊材,采用复凝聚技术"一步法"制备P-VP8~*IgY微胶囊。以微胶囊的成囊效果和包封率为评价指标,通过单因素分析和L9(34)正交试验优化微胶囊的最佳制备工艺。并运用SDS-PAGE和ELISA法评价海藻酸钠-壳聚糖P-VP8~*IgY微胶囊的释放性能和生物学活性。结果海藻酸钠-壳聚糖P-VP8~*IgY微胶囊的最佳制备工艺条件为:海藻酸钠浓度为3. 0%、壳聚糖浓度为0. 4%、氯化钙浓度为2%(均为质量分数)、壳聚糖与氯化钙溶液(成囊液)的p H值为5. 5,IgY投药量为10 g·L-1。制备的海藻酸钠-壳聚糖P-VP8~*IgY微胶囊大部分呈规则球形,表面较为光滑圆整,包封率可达到85%。制备的微胶囊在胃液2 h后的释放率为7%,肠液6 h后的释放率高达86%,且生物活性良好。结论本工艺制备的海藻酸钠-壳聚糖P-VP8~*IgY微胶囊能够保护特异性P-VP8~*IgY不被胃酸环境破坏,具有较好的缓释作用。Objective On the basis of successful preparation of purified P-VP8-＊dual IgY specific to norovirus and rotavirus,this study aimed to establish the optimal preparation process of microcapsules and evaluate its sustained release performance. Methods P-VP8-＊IgY microcapsules were prepared by one-step method using chitosan and sodium alginate as wall materials. Preparation of the microcapsules was evaluated by cystoid shape together withencapsulation rate and optimized using single factor analysis and L9（ 34）orthogonal design. The release rate and bio-activity of IgY were also evaluated using SDS-PAGE and ELISA. Results The concentration optimal conditions were showed as follows： 3. 0% sodium alginate,0. 3%chitosan,2. 0% calcium chloride（ mass fraction）,the pH value of chitosan and calcium chloride solution5. 5,and IgY loading rate 10 g·L^-1. M ostof microcapsules shaped round and smooth,the encapsulationratec could reach to 85%. The release rate was only 7. 1% after 2 h simulated gastric fluid digestion,while it could reach more than 86% after 6 h simulated intestinal fluid digestion. Conclusion The chitosan-alginate P-VP8-＊IgY microcapsules had a good sustained release effect,which can protect P-VP8-＊IgY from destruction in gastric acid,and achieve the sustained release in intestinal tract.

关 键 词：P-VP8^＊IgY 微胶囊 制备工艺 释放性能 

分 类 号：R94[医药卫生—药剂学]