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Factorial design studies of antiretroviral drug-loaded stealth liposomal injectable: PEGylation, lyophilization and pharmacokinetic studies

机译:载有抗逆转录病毒药物的隐性脂质体注射剂的析因设计研究:聚乙二醇化,冻干和药代动力学研究

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The aim of the present study was to formulate and evaluate the ritonavir-loaded stealth liposomes by using 32 factorial design and intended to delivered by parenteral delivery. Liposomes were prepared by ethanol injection method using 32 factorial designs and characterized for various physicochemical parameters such as drug content, size, zeta potential, entrapment efficiency and in vitro drug release. The optimization process was carried out using desirability and overlay plots. The selected formulation was subjected to PEGylation using 10?% PEG-10000 solution. Stealth liposomes were characterized for the above-mentioned parameters along with surface morphology, Fourier transform infrared spectrophotometer, differential scanning calorimeter, stability and in vivo pharmacokinetic studies in rats. Stealth liposomes showed better result compared to conventional liposomes due to effect of PEG-10000. The in vivo studies revealed that stealth liposomes showed better residence time compared to conventional liposomes and pure drug solution. The conventional liposomes and pure drug showed dose-dependent pharmacokinetics, whereas stealth liposomes showed long circulation half-life compared to conventional liposomes and pure ritonavir solution. The results of statistical analysis showed significance difference as the p value is (
机译:本研究的目的是通过3 2 析因设计来配制和评估装载了利托那韦的隐形脂质体,并打算通过肠胃外给药进行递送。采用3 2 析因设计通过乙醇注射法制备脂质体,并表征了各种理化参数,如药物含量,大小,ζ电势,包封率和体外药物释放。优化过程是使用合意性和覆盖图进行的。使用10%的PEG-10000溶液对选择的制剂进行PEG化。隐身脂质体的上述参数以及表面形态,傅里叶变换红外分光光度计,差示扫描量热仪,稳定性和大鼠体内药代动力学研究均已表征。由于PEG-10000的作用,与常规脂质体相比,隐形脂质体显示出更好的结果。体内研究表明,与常规脂质体和纯药物溶液相比,隐形脂质体显示出更好的停留时间。与常规脂质体和纯利托那韦溶液相比,常规脂质体和纯药物显示出剂量依赖性药代动力学,而隐形脂质体显示出长的循环半衰期。统计分析结果表明,由于p值为(

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