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Comparison of human skin or epidermis models with human and animal skin in in-vitro percutaneous absorption

人体皮肤 皮肤当量 克霉唑 水杨酸 表皮(动物学) 体外 化学 渗透 体内 吸收(声学) 猪皮 皮肤病科 渗透(战争) 药理学 角质形成细胞 医学 生物 生物化学 解剖 抗真菌 材料科学 生物技术 复合材料 工程类 遗传学 运筹学 食品科学
作者
Fritz P. Schmook,Josef G. Meingassner,Andreas Billich
出处
期刊:International Journal of Pharmaceutics [Elsevier BV]
卷期号:215 (1-2): 51-56 被引量:511
标识
DOI:10.1016/s0378-5173(00)00665-7
摘要

For the study of in-vitro skin penetration of candidate drugs, excised animal skin is frequently used as a replacement for human skin. Reconstructed human skin or epidermis equivalents have been proposed as alternatives. We compared the penetration properties of human, pig and rat skin with the Graftskin™ LSE™ (living skin equivalent) and the Skinethic™ HRE (human reconstructed epidermis) models using four topical dermatological drugs (salicylic acid, hydrocortisone, clotrimazole and terbinafine) with widely varying polarity. In agreement with published data, pig skin appeared as the most suitable model for human skin: the fluxes through the skin and concentrations in the skin were of the same order of magnitude for both tissues, with differences of at most two- or fourfold, respectively. Graftskin™ LSE™ provided an adequate barrier to salicylic acid, but was very permeable for the more hydrophobic compounds (e.g. about 900-fold higher flux and 50-fold higher skin concentrations of clotrimazole as compared to human skin), even more than rat skin. In the case of the Skinethic™ HRE, we found similar concentrations of salicylic acid as in human skin and an approximately sevenfold higher flux. In contrast, the permeation of hydrophobic compounds through the epidermal layer was vastly higher than through split-thickness human skin (up to a factor of about 800). To conclude, currently available reconstituted skin models cannot be regarded as generally useful for in-vitro penetration studies.
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