脂质体
透皮
色谱法
生物利用度
延胡索乙素
体内
化学
Zeta电位
磷脂酰胆碱
药理学
材料科学
膜
医学
生物化学
中医药
病理
生物技术
纳米颗粒
纳米技术
替代医学
磷脂
延胡索
生物
作者
Guizhen Zhang,Xuejian Li,Chunyun Huang,Yuanyuan Jiang,Jian Su,Ying Hu
摘要
Purpose:The aim of this study was to develop a liposome gel containing levo-tetrahydropalmatine (l-THP) and evaluate its transdermal properties.Methods: A L 16 (4 3 ) orthogonal experiment was conducted to optimize the preparation of l-THP liposomes and assess their characterization and stability in a gel.The transdermal features were analyzed through in vivo and in vitro experiments on rats and Strat-M ® membrane, respectively.The metabolism of l-THP in liver and skin S9 fractions was also studied. Results:The optimization of the orthogonal experiment revealed that the ideal mass ratio of phosphatidylcholine, cholesterol, and l-THP during preparation was 10:1:3.The resulting liposome exhibited a particle size of 68 nm, a PDI of 0.27, a drug loading of 4.33%, an encapsulation of 18.79%, and a zeta potential of -41.27 mV.Both the l-THP and its liposome-gel formulation were found to be stable for a duration of 45 days at 4 °C and 30 °C.During the in vivo transdermal study, the maximum concentration (C max ) of l-THP from the liposome gel was 0.16 μg/mL, and the time to reach this maximum concentration (t max ) was 1.2 hours.The relative bioavailability of l-THP in the liposome gel was 233.8% compared to the emulsion.The concentration of l-THP (prepared in PBS) decreased at a rate of 0.0067 μg/mL/min in the liver S9 fraction and 0.0027 μg/mL/min in the skin S9 fraction, however, this difference was not observed when l-THP was encapsulated in liposomes.l-THP passed through the Strat-M ® membrane at a rate of 0.0032 mg/cm 2 /h and 0.002 mg/cm 2 /h for the emulsion and liposome gel, respectively. Conclusion:The optimal process for the preparation of l-THP liposomes was obtained.Compared to the emulsion, the liposomes provided greater bioavailability when used transdermally.The liposomes also provided greater stability for l-THP during storage.
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