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Development of ethosomes with taguchi robust design-based studies for transdermal delivery of alfuzosin hydrochloride

机译:用基于Taguchi的稳健设计为基础的研究开发用于透皮递送盐酸阿夫唑嗪的脂质体的开发

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In the present investigation efficiency of ethosomes as novel lipid carriers for transdermal delivery of Alfuzosin Hydrochloride (AH) has been evaluated. Taguchi robust design method was used for optimization of ethosomal formulations. Phospholipid type, concentration of phospholipid and concentration of ethanol was selected as independent variables and their effect on the dependent variables (entrapment efficiency and flux) was studied. Ethosomal formulation (EA8) with soya phosphatidylcholine (3%) and ethanol 20% were optimized. Vesicles were spherical, unilamellar with smooth surface. The optimized formulation exhibited vesicle size (6.85 ± 1.35μm), zeta potential (-8.14 ± 0.62mv), entrapment efficiency (91.86 ± 3.25%), flux (27.42 ± 0.04μg/cm2/hr), lag time (0.26±0.20hr) and skin deposition (298.01 ± 15.4μg/g). Transdermal flux was enhanced by 6.92 times over drug solution. Vesicle skin interaction studies showed fatty change in the dermis. The formulations were stable at 4°C for 120 days. Results suggested ethosomes as efficient carriers for AH transdermal delivery.DOI:?http://dx.doi.org/10.3329/icpj.v1i11.12063 International Current Pharmaceutical Journal 2012, 1(11): 370-375
机译:在本研究中,已经评估了作为一种脂质载体的脂质体用于透皮递送盐酸阿夫唑嗪(AH)的效率。 Taguchi稳健的设计方法用于优化酶体制剂。选择磷脂类型,磷脂浓度和乙醇浓度作为自变量,并研究它们对因变量(包埋效率和通量)的影响。优化了含大豆磷脂酰胆碱(3%)和20%乙醇的酶体制剂(EA8)。囊泡为球形,单层,表面光滑。优化的制剂具有囊泡大小(6.85±1.35μm),ζ电位(-8.14±0.62mv),包封效率(91.86±3.25%),通量(27.42±0.04μg/ cm2 / hr),滞后时间(0.26±0.20) hr)和皮肤沉积(298.01±15.4μg/ g)。透皮通量比药物溶液提高了6.92倍。囊泡皮肤相互作用研究显示真皮中的脂肪变化。该制剂在4℃下稳定120天。结果表明,脂质体是AH透皮递送的有效载体.DOI:?http://dx.doi.org/10.3329/icpj.v1i11.12063 International Current Pharmaceutical Journal 2012,1(11):370-375

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