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优化与评价普朗尼克卵磷脂有机凝胶作为青藤碱透皮给药载体的性能

Optimization and evaluation of pluronic lecithin organogels as a transdermal delivery vehicle for sinomenine.

作者信息

Ba Wenqiang, Li Zhou, Wang Lisheng, Wang Ding, Liao Weiguo, Fan Wentao, Wu Yinai, Liao Fengyun, Yu Jianye

机构信息

a School of Chinese Materia Medica, Guangzhou University of Chinese Medicine , Guangzhou , Guangdong , China.

出版信息

Pharm Dev Technol. 2016 Aug;21(5):535-45. doi: 10.3109/10837450.2015.1022791. Epub 2015 Mar 11.

Abstract

The purpose of the present study was to prepare and optimize sinomenine (SIN) pluronic lecithin organogels system (PLO), and to evaluate the permeability of the optimized PLO in vitro and in vivo. Box-Behnken design was used to optimize the PLO and the optimized formulation was pluronic F127 of 19.61%, lecithin of 3.60% and SIN of 1.27%. The formulation was evaluated its skin permeation and drug deposition both in vitro and in vivo compared with gel. Permeation and deposition studies of PLO were carried out with Franz diffusion cells in vitro and with microdialysis in vivo. In vitro studies, permeation rate (Jss) of SIN from PLO was 146.55 ± 2.93 μg/cm(2)/h, significantly higher than that of gel (120.39 μg/cm(2)/h) and the amount of SIN deposited in skin from the PLO was 10.08 ± 0.86 μg/cm(2), significantly larger than that from gel (6.01 ± 0.04 μg/cm(2)). In vivo skin microdialysis studies showed that the maximum concentration (Cmax) of SIN from PLO in "permeation study" and "drug-deposition study" were 150.27 ± 20.85 μg/ml and 67.95 μg/ml, respectively, both significantly higher than that of SIN from gel (29.66 and 6.73 μg/ml). The results recommend that PLO can be used as an advantageous transdermal delivery vehicle to enhance the permeation and skin deposition of SIN.

摘要

本研究的目的是制备并优化青藤碱(SIN)泊洛尼克卵磷脂有机凝胶系统(PLO),并评估优化后的PLO在体外和体内的渗透性。采用Box-Behnken设计优化PLO,优化后的配方为19.61%的泊洛尼克F127、3.60%的卵磷脂和1.27%的SIN。与凝胶相比,对该配方进行了体外和体内皮肤渗透及药物沉积评估。PLO的渗透和沉积研究分别在体外使用Franz扩散池进行,在体内使用微透析进行。体外研究中,SIN从PLO的渗透速率(Jss)为146.55±2.93μg/cm²/h,显著高于凝胶(120.39μg/cm²/h),且SIN从PLO沉积在皮肤中的量为10.08±0.86μg/cm²,显著大于凝胶(6.01±0.04μg/cm²)。体内皮肤微透析研究表明,在“渗透研究”和“药物沉积研究”中,SIN从PLO的最大浓度(Cmax)分别为150.27±20.85μg/ml和67.95μg/ml,均显著高于SIN从凝胶中的浓度(29.66和6.73μg/ml)。结果表明,PLO可作为一种有利的透皮给药载体,以增强SIN的渗透和皮肤沉积。

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