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首页> 外文期刊>Journal of Pharmacy and Pharmacology >Improved oral bioavailability of breviscapine via a Pluronic P85-modified liposomal delivery system
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Improved oral bioavailability of breviscapine via a Pluronic P85-modified liposomal delivery system

机译:通过Pluronic P85修饰的脂质体递送系统改善灯盏花素的口服生物利用度

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Objectives Breviscapine, a hydrophobic drug used for treating cardiovascular disease, was encapsulated in liposomes to improve its pharmaceutical characteristics. This study describes a novel liposome composition approach to specifically inhibit the P-glycoprotein efflux system. Methods Breviscapine-loaded Pluronic P85-coated liposomes were prepared by the thin film hydration technique. The particle size, zeta potential and encapsulation efficiency of the formulations were characterized. In-vitro drug release and permeability of Caco-2 cells were investigated. In-vitro characteristics and pharmacokinetics of the liposomes were evaluated in rat studies. Key findings The Pluronic P85-modified liposomes dispersed individually and had an approximate diameter of 118.8 ± 4.9 nm and a zeta potential of -35.4 ± 1.5 mV. Encapsulation efficiency was more than 90%. The use of the P85-coated liposomes resulted in significantly (P < 0.05) increased absorption of breviscapine in Caco-2 cells and in 5.6-fold enhancement in its oral bioavailability in rats. Conclusion The P85-modified liposomes for the oral delivery of breviscapine were prepared using l-α-phosphatidylcholine (soy-hydrogenated) and cholesterol with a narrow size distribution. This method seems to effectively enhance the bioavailability of breviscapine in rats.
机译:目的灯盏花素是一种用于治疗心血管疾病的疏水性药物,被包裹在脂质体中以改善其药物特性。这项研究描述了一种新型的脂质体组成方法,可特异性抑制P-糖蛋白外排系统。方法采用薄膜水化技术制备负载灯盏花素的Pluronic P85脂质体。表征了制剂的粒度,ζ电势和包封效率。研究了体外药物释放和Caco-2细胞的通透性。在大鼠研究中评估了脂质体的体外特性和药代动力学。主要发现Pluronic P85修饰的脂质体单独分散,直径约为118.8±4.9 nm,ζ电位为-35.4±1.5 mV。封装效率超过90%。使用涂有P85的脂质体可显着(P <0.05)增加灯盏花素在Caco-2细胞中的吸收,并使大鼠口服生物利用度提高5.6倍。结论使用α-磷脂酰胆碱(大豆氢化)和胆固醇制备了P85修饰的灯盏花素口服脂质体,其粒径分布较窄。这种方法似乎可以有效提高灯盏花素在大鼠中的生物利用度。

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