Effect of menthone and related compounds on skin permeation of drugs with different lipophilicity and molecular organization of stratum corneum lipids

亲脂性 门托 化学 角质层 薄荷醇 渗透 普勒贡 冰片 透皮 药理学 色谱法 有机化学 立体化学 生物化学 精油 医学 替代医学 病理 中医药
作者
Yi Lan,Jingyan Wang,Hui Li,Yewen Zhang,Yanyan Chen,Bochen Zhao,Qing Wu
出处
期刊:Pharmaceutical Development and Technology [Taylor & Francis]
卷期号:: 1-10 被引量:27
标识
DOI:10.3109/10837450.2015.1011660
摘要

The objective of this article was to investigate the enhancing effect of menthone, menthol and pulegone on the transdermal absorption of drugs with different lipophilicity and probe their mechanisms of action at molecular level. Five model drugs, namely osthole, tetramethylpyrazine, ferulic acid, puerarin and geniposide, which were selected based on their lipophilicity denoted by logKo/w, were tested using in vitro permeation studies in which Franz diffusion cells and rat skin were employed. Infrared spectroscopy and molecular dynamic simulation were used to investigate the effect of these enhancers on the stratum corneum (SC) lipids, respectively. Three compounds could effectively promote the transdermal absorption of drugs with different lipophilicity, and the overall promoting capacities were in the following increasing order: pulegone < menthol < menthone. The penetration enhancement ratio was roughly in parabolic curve relationships with the drug lipophilicity after treatment with menthol or menthone, while the penetration enhancement effect of pulegone hardly changed with the alteration of the drug lipophilicity. The molecular mechanism studies suggested that menthone and menthol enhanced the skin permeability by disordering the ordered organization of SC lipids and extracted part of SC lipids, while pulegone appeared to promote drug transport across the skin only by extracting part of SC lipids.
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