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在微囊化过程中,普朗尼克表面活性剂对重组人生长激素抗乳化诱导聚集的稳定作用。

Stabilization of recombinant human growth hormone against emulsification-induced aggregation by Pluronic surfactants during microencapsulation.

作者信息

Wei Gang, Lu Li Fang, Lu Wei Yue

机构信息

Fudan University-PharmCo Targeting Drug Research Center, Department of Pharmaceutics, School of Pharmacy, Fudan University, Shanghai 200032, PR China.

出版信息

Int J Pharm. 2007 Jun 29;338(1-2):125-32. doi: 10.1016/j.ijpharm.2007.01.043. Epub 2007 Feb 2.

DOI:10.1016/j.ijpharm.2007.01.043
PMID:17336005
Abstract

Protein aggregation upon exposing to the water/organic solvent interface is one of the most significant obstacles in developing poly(lactic-co-glycolic acid) (PLGA) microspheres with double emulsion process. The aim of present study is to devise a formulation strategy to prevent recombinant human growth hormone (rhGH) from aggregation during microencapsulation. The excipients used for stabilizing rhGH were selected from sugars, nonionic surfactants, polyol, and protein. Among the candidates, surfactants exhibited potentialities in protecting rhGH against emulsification-induced aggregation. It was also found that Pluronic F127 showed an outstanding as well as concentration-dependent stabilizing effect on rhGH, which was different to Pluronic F68 and Tween 20. After the rhGH solution comprising F127 and sucrose was emulsified with methylene chloride, the recovery of monomeric protein achieved 99.0%, principally attributed to the presence of F127. This solution was subsequently encapsulated as inner aqueous phase in the PLGA microspheres by a conventional double emulsion process, with the encapsulation efficiency higher than 98%. Improvement in the release of rhGH was observed for the microspheres co-encapsulating Pluronic F127 regardless in the presence or absence of sucrose, compared to the microspheres containing rhGH alone. The result further implied that co-encapsulation of Pluronic F127 in the microspheres played an important role in the stabilization of rhGH.

摘要

在双乳液法制备聚乳酸-乙醇酸共聚物(PLGA)微球过程中,蛋白质暴露于水/有机溶剂界面时发生聚集是最显著的障碍之一。本研究的目的是设计一种配方策略,以防止重组人生长激素(rhGH)在微囊化过程中聚集。用于稳定rhGH的辅料从糖类、非离子表面活性剂、多元醇和蛋白质中选择。在这些候选辅料中,表面活性剂在保护rhGH免受乳化诱导聚集方面表现出潜力。还发现泊洛沙姆F127对rhGH表现出优异的且浓度依赖性的稳定作用,这与泊洛沙姆F68和吐温20不同。含F127和蔗糖的rhGH溶液用二氯甲烷乳化后,单体蛋白回收率达到99.0%,这主要归因于F127的存在。随后通过传统双乳液法将该溶液作为内水相包封在PLGA微球中,包封效率高于98%。与单独含有rhGH的微球相比,无论有无蔗糖,共包封泊洛沙姆F127的微球中rhGH的释放均有所改善。结果进一步表明,在微球中共包封泊洛沙姆F127对rhGH的稳定起着重要作用。

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