Andrographolide-loaded ethosomal gel for transdermal application: Formulation and in vitro penetration study

Q4 Pharmacology, Toxicology and Pharmaceutics Infarma Pharmaceutical Sciences Pub Date : 2021-11-30 DOI:10.34172/ps.2021.76

Nooryza Martihandini, Silvia Surini, A. Bahtiar

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引用次数: 1

Abstract

Background: Andrographolide is a phytoconstituent with anti-inflammatory activity, however, the compound’s poor oral bioavailability has hindered its effective formulation for oral administration. This study, therefore, aims to develop an ethosome for improving andrographolide penetration through the transdermal delivery system. Methods: This study developed 3 ethosome formulas with different andrographolide-phospholipid weight ratios (1:8, 1:9; 1:10), using the thin-layer dispersion-sonication method. Subsequently, the ethosomes were evaluated for particle size, polydispersity index, zeta potential, morphology, as well as entrapment efficiency, and incorporated into a gel dosage form. Subsequently, an in vitro penetration study was performed using Franz diffusion cells for 24 hours and the stability of the gels at 5 ± 2°C, 30 ± 2°C, and 40 ± 2°C, were studied for 3 months. Results: The results showed the optimal formula was E2, a 1:9 weight ratio formula of andrographolide and phospholipid. Based on the transmission electron micrograph, E2 possessed unilamellar, as well as spherical-shaped vesicles, and exhibited superior characteristics for transdermal delivery, with a particle size of 89.95 ± 0.75 nm, polydispersity index of 0.254 ± 0.020, a zeta potential of -39.3 ± 0.82 mV, and entrapment efficiency of 97.89 ± 0.02%. Furthermore, the cumulative andrographolide penetration and transdermal flux for the ethosomal gel of E2 (EG2) were 129.25 ± 4.66 µg/cm2 and 5.16 ± 0.10 µg/cm2/hours, respectively. All the ethosomal gel formulations exhibited improved penetration enhancement of andrographolide, compared to the nonethosomal formulations. Also, the andrographolide levels in the ethosomal and nonethosomal gels after 3 months ranged from 98.13 to 104.19%, 97.93 to 104.01%, and 97.23 to 102.26% at storage temperatures of 5 ± 2°C, 30 ± 2°C/RH 65% ± 5%, and 40 ± 2°C/RH 75% ± 5%, respectively. Conclusions: This study concluded that encapsulation into ethosome enhances andrographolide delivery through the skin.

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穿心莲内酯经皮凝胶:配方及体外渗透研究

背景:穿心莲内酯是一种具有抗炎活性的植物成分，然而，该化合物较差的口服生物利用度阻碍了其口服给药的有效配方。因此，本研究旨在开发一种改善穿心莲内酯通过透皮给药系统渗透的酶体。方法:研制出3种穿心莲内酯-磷脂质量比(1:8、1:9;1:10)，采用薄层分散-超声法。随后，对酶体的粒径、多分散性指数、zeta电位、形态以及包封效率进行评估，并将其掺入凝胶剂型。随后，使用Franz扩散池进行24小时的体外渗透研究，并在5±2°C, 30±2°C和40±2°C下研究凝胶的稳定性3个月。结果:穿心莲内酯与磷脂质量比为1:9的最佳配方为E2。透射电镜显示，E2具有单层和球形囊泡，具有良好的透皮传递特性，粒径为89.95±0.75 nm，多分散指数为0.254±0.020,zeta电位为-39.3±0.82 mV，包封效率为97.89±0.02%。E2 (EG2)的累计穿心术内酯渗透和透皮通量分别为129.25±4.66µg/cm2和5.16±0.10µg/cm2/h。与非乙醇体制剂相比，所有乙醇体凝胶制剂均表现出穿心莲内酯的渗透增强。在5±2℃、30±2℃/RH 65%±5%、40±2℃/RH 75%±5%的贮藏温度下，3个月后龙心体凝胶和非龙心体凝胶中穿心莲内酯含量分别为98.13 ~ 104.19%、97.93 ~ 104.01%和97.23 ~ 102.26%。结论:经皮囊化后，穿心莲内酯可通过皮肤传递。

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