Development and evaluation of emulsion-liposome blends for resveratrol delivery

Chi Feng Hung, Jan Kan Chen, Mei Hui Liao, Huey Ming Lo, Jia You Fang*

*此作品的通信作者

研究成果: 期刊稿件文章同行評審

92 引文 斯高帕斯(Scopus)

摘要

Nano- and submicron-sized vesicles are beneficial for the controlled delivery of drugs. Resveratrol, the main active polyphenol in red wine, was incorporated into various combinations of emulsions and liposomes to examine its physicochemical characteristics and cardiovascular protection. The blends of emulsion-liposome were composed of coconut oil, soybean lecithin, glycerol formal, and non-ionic surfactants. Multiple systems were assessed by evaluating the droplet size, surface charge, drug encapsulation, release rate, and stability. The vesicle diameter of the systems ranged from 114 to 195 nm. The liposomal vesicles in the systems had smaller diameters (of 43-56 nm) (F6 and F7 Drug encapsulation of ∼70% were achieved by the vesicles. The inclusion of resveratrol in these systems retarded the drug release in both the presence and absence of plasma in vitro. The emulsion-liposome blends which incorporated Brij 98 (F5) exhibited the slowest release at zero-order for resveratrol delivery. Treatment using resveratrol in the blended formulations dramatically inhibited vascular intimal thickening, which was tested in an experimental model in which endothelial injury was produced in normal rat carotid arteries. Intraperitoneal injection of the multiple systems was associated with no or negligible liver and kidney toxicity. We concluded that encapsulation by the emulsion-liposome blends is a potent way to enhance the preventative and therapeutic benefits of resveratrol.

原文英語
頁(從 - 到)2950-2958
頁數9
期刊Journal of Nanoscience and Nanotechnology
6
發行號9-10
DOIs
出版狀態已出版 - 09 2006

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