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采用中心复合设计优化用于鼻内给药的载蒿甲醚纳米脂质载体

Optimization of artemether-loaded NLC for intranasal delivery using central composite design.

作者信息

Jain Kunal, Sood Sumeet, Gowthamarajan Kuppusamy

机构信息

a J.S.S. College of Pharmacy , Department of Pharmaceutics , Rocklands , Udhagamandalam , Tamil Nadu , India.

出版信息

Drug Deliv. 2015;22(7):940-54. doi: 10.3109/10717544.2014.885999. Epub 2014 Feb 10.

DOI:10.3109/10717544.2014.885999
PMID:24512368
Abstract

The objective of the study was to optimize artemether-loaded nanostructured lipid carriers (ARM-NLC) for intranasal delivery using central composite design. ARM-NLC was prepared by microemulsion method with optimized formulation having particle size of 123.4 nm and zeta potential of -34.4 mV. Differential scanning calorimetry and powder X-ray diffraction studies confirmed that drug existed in amorphous form in NLC formulation. In vitro cytotoxicity assay using SVG p12 cell line and nasal histopathological studies on sheep nasal mucosa indicated the developed formulations were non-toxic and safe for intranasal administration. In vitro release studies revealed that NLC showed sustained release up to 96 h. Ex vivo diffusion studies using sheep nasal mucosa revealed that ARM-NLC had significantly lower flux compared to drug solution (ARM-SOL). Pharmacokinetic and brain uptake studies in Wistar rats showed significantly higher drug concentration in brain in animals treated intranasally (i.n.) with ARM-NLC. Brain to blood ratios for ARM-NLC (i.n.), ARM-SOL (i.n.) and ARM-SOL (i.v.) were 2.619, 1.642 and 0.260, respectively, at 0.5 h indicating direct nose to brain transport of ARM. ARM-NLC showed highest drug targeting efficiency and drug transport percentage of 278.16 and 64.02, respectively, which indicates NLC had better brain targeting efficiency compared to drug solution.

摘要

本研究的目的是使用中心复合设计优化用于鼻内给药的载蒿甲醚纳米结构脂质载体(ARM-NLC)。通过微乳法制备ARM-NLC,优化后的制剂粒径为123.4 nm,zeta电位为-34.4 mV。差示扫描量热法和粉末X射线衍射研究证实药物在NLC制剂中以无定形形式存在。使用SVG p12细胞系进行的体外细胞毒性试验以及对绵羊鼻黏膜的鼻组织病理学研究表明,所开发的制剂对鼻内给药无毒且安全。体外释放研究表明,NLC显示出长达96小时的持续释放。使用绵羊鼻黏膜进行的离体扩散研究表明,与药物溶液(ARM-SOL)相比,ARM-NLC的通量显著更低。在Wistar大鼠中进行的药代动力学和脑摄取研究表明,经鼻内(i.n.)给予ARM-NLC治疗的动物脑中药物浓度显著更高。在0.5小时时,ARM-NLC(i.n.)、ARM-SOL(i.n.)和ARM-SOL(i.v.)的脑血比分别为2.619、1.642和0.260,表明ARM可直接从鼻到脑转运。ARM-NLC显示出最高的药物靶向效率和药物转运百分比,分别为278.6和64.02,这表明与药物溶液相比,NLC具有更好的脑靶向效率。

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