Wang Yan Jiao, Wang Juan, Zhang Hong Yao, He Hai Bing, Tang Xing
Department of Pharmaceutics, School of Pharmacy, Shenyang Pharmaceutical University, 103 Wenhua Road, Shenyang 110016, PR China.
J Pharm Pharmacol. 2007 Mar;59(3):351-7. doi: 10.1211/jpp.59.3.0003.
The aim of this study was to investigate the feasibility of preparing flunarizine-loaded lipid microspheres. Lipid microspheres (LMs) are excellent drug carriers for drug delivery systems (DDS) and are relatively stable and easily mass-produced. They have no particular adverse effects. LMs have been widely studied as drug carriers for water-soluble drugs, lipid-soluble drugs and inadequately soluble (in water or in lipid) drugs, in that they have a lipid layer, a water layer and an emulsifier layer. Flunarizine (FZ), a poorly water-soluble drug, was incorporated in lipid microspheres to reduce side effects by avoiding the use of supplementary agents, compared with solution injection. After investigation, the final formulation was as follows: 10% oil phase (long-chain triglyceride (LCT); medium-chain fatty acid (MCT) = 50:50); 1.2% egg lecithin; 0.2% Tween-80; 2.5% glycerin; 0.3% dl-alpha-tocopherol; 0.02% EDTA; 0.03% sodium oleate; 0.1% FZ and double-distilled water to give a total volume of 100 mL. Homogenization was the main method of preparation and the best conditions were a temperature of 40 degrees C, a pressure of 700-800 bar and a suitable cycle frequency of about 10. The particle size distribution, zeta-potential and entrapment efficacy were found to be 198.7+/-54.0 nm, -26.4 mV and 96.2%, respectively. Its concentration in the preparation was 1.0 mg mL(-1). The lipid microspheres were stable during storage at 4 degrees C, 25 degrees C and 37 degrees C for 3 months. Pharmacokinetic studies were performed in rats using a dose of 1.0 mg kg(-1). The pharmacokinetic parameters were as follows: AUC(0-t) 6.13 mug.h mL(-1), t(1/2) 5.32 h and Ke 0.16 L h(-1). The preparation data fitted a two-compartment model estimated by using 3p87 analysis software. From the observed data, FZ encapsulated in LMs did not significantly alter the pharmacokinetic characteristic compared with the FZ solution injection and did not produce a delayed release effect, when it was released in-vivo in rats. However, the availability of the drug was increased. These results suggested that this LM system is a promising option for the preparation of the liquid form of FZ for intravenous administration.
本研究的目的是探讨制备氟桂利嗪脂质微球的可行性。脂质微球(LMs)是药物递送系统(DDS)中优秀的药物载体,相对稳定且易于大规模生产,无特殊不良反应。由于脂质微球具有脂质层、水层和乳化剂层,已被广泛研究作为水溶性药物、脂溶性药物以及难溶性(在水或脂质中)药物的载体。氟桂利嗪(FZ)是一种水溶性差的药物,与溶液注射相比,将其包封于脂质微球中可避免使用辅料从而减少副作用。经过研究,最终制剂配方如下:10%油相(长链甘油三酯(LCT);中链脂肪酸(MCT)=50:50);1.2%卵磷脂;0.2%吐温80;2.5%甘油;0.3%dl-α-生育酚;0.02%乙二胺四乙酸;0.03%油酸钠;0.1%FZ,加双蒸水至总体积100 mL。匀化是主要的制备方法,最佳条件为温度40℃、压力700 - 800 bar以及合适的循环频率约10次。发现粒径分布、ζ-电位和包封率分别为198.7±54.0 nm、-26.4 mV和96.2%。其在制剂中的浓度为1.0 mg mL-1。脂质微球在4℃、25℃和37℃储存3个月期间保持稳定。在大鼠中以1.0 mg kg-1的剂量进行了药代动力学研究。药代动力学参数如下:AUC(0 - t) 6.13 μg·h mL-1,t(1/2) 5.32 h,Ke 0.16 L h-1。制剂数据符合使用3p87分析软件估算的二室模型。从观察数据来看,与氟桂利嗪溶液注射相比,包封于脂质微球中的氟桂利嗪在大鼠体内释放时并未显著改变药代动力学特征,也未产生缓释效应。然而,药物的可用性增加了。这些结果表明,这种脂质微球系统是制备用于静脉给药的氟桂利嗪液体制剂的一个有前景的选择。
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