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长循环聚乙二醇-共聚聚乳酸-共乙醇酸微胶囊作为静脉给药药物的潜在载体。

Long-circulating poly(ethylene glycol)-coated poly(lactid-co-glycolid) microcapsules as potential carriers for intravenously administered drugs.

机构信息

Institute for Physiological Chemistry, University of Duisburg-Essen, University Hospital Essen , Hufelandstr. 55, 45122 Essen , Germany.

出版信息

J Microencapsul. 2013;30(7):632-42. doi: 10.3109/02652048.2013.770098. Epub 2013 Mar 14.

DOI:10.3109/02652048.2013.770098
PMID:23489015
Abstract

The intrinsic advantages of microcapsules with regard to nanocapsules as intravenous drug carrier systems are still not fully exploited. Especially, in clinical situations where a long-term drug release within the vascular system is desired, if large amounts of drug have to be administered or if capillary leakage occurs, long-circulating microparticles may display a superior alternative to nanoparticles. Here, microcapsules were synthesised and parameters such as in vitro tendency of agglomeration, protein adsorption and in vivo performance were investigated. Biocompatible poly(ethylene glycol) (PEG)-coated poly(DL-lactide-co-glycolide) (PLGA) as wall material, solid and perfluorodecalin (PFD)-filled PEG-PLGA microcapsules (1.5 µm diameter) were manufactured by using a modified solvent evaporation method with either 1% poly(vinyl alcohol) (PVA) or 1.5% cholate as emulsifying agents. Compared to microcapsules manufactured with cholate, the protein adsorption (albumin and IgG) was clearly decreased and agglomeration of capsules was prevented, when PVA was used. The intravenous administration of these microcapsules, both solid and PFD-filled, in rats was successful and exhibited a circulatory half-life of about 1 h. Our data clearly demonstrate that PEG-PLGA microcapsules, manufactured by using PVA, are suitable biocompatible, long-circulating drug carriers, applicable for intravenous administration.

摘要

微胶囊作为静脉药物载体系统相对于纳米胶囊具有内在优势,但尚未得到充分利用。特别是在临床情况下,如果需要在血管系统中长时间释放药物,如果需要给予大量药物或发生毛细血管渗漏,长循环微颗粒可能是纳米颗粒的更好选择。本文合成了微胶囊,并研究了其体外聚集倾向、蛋白质吸附和体内性能等参数。采用改良的溶剂蒸发法,以 1%聚乙烯醇(PVA)或 1.5%胆酸钠作为乳化剂,制备了生物相容性聚(乙二醇)(PEG)-共-聚(DL-乳酸-共-乙醇酸)(PLGA)作为壁材料的固体和全氟癸烷(PFD)填充的 PEG-PLGA 微胶囊(直径 1.5μm)。与使用胆酸钠制备的微胶囊相比,当使用 PVA 时,微胶囊的蛋白质吸附(白蛋白和 IgG)明显减少,胶囊聚集得到防止。这些微胶囊(固体和 PFD 填充)在大鼠体内的静脉给药是成功的,其循环半衰期约为 1 小时。我们的数据清楚地表明,使用 PVA 制备的 PEG-PLGA 微胶囊是适合的生物相容性、长循环药物载体,适用于静脉给药。

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