Percutaneous Absorption of Vanilloids: In Vivo and in Vitro Studies

体内 化学 体外 吸收(声学) 色谱法 人体皮肤 渗透(战争) 生物化学 生物 材料科学 遗传学 生物技术 运筹学 工程类 复合材料
作者
Gerald B. Kasting,William R. Francis,Lisa A. Bowman,Gene O. Kinnett
出处
期刊:Journal of Pharmaceutical Sciences [Elsevier]
卷期号:86 (1): 142-146 被引量:42
标识
DOI:10.1021/js950484a
摘要

The percutaneous absorption of three highly lipophilic analogs of capsaicinsvanillylnonanamide (VN), olvanil, and NE-21610swas measured in vivo in the CD:VAF rat, and in vitro through excised CD: VAF and SkH:Fz rat skin and human cadaver skin. Absorption and skin metabolism were monitored by radiolabel techniques. The rank order of penetration in all species was VN>olvanil>NE-21610, in accordance with that expected from their physical properties. Rat skin was more permeable than human skin by factors ranging from 4 to 8 for VN, 10 to 20 for olvanil, and ≈10 to 100 for NE-21610. All three compounds were extensively metabolized during passage through fresh SkH:Fz rat skin, with the primary route of degradation for at least two of the compounds involving hydrolysis of the amide bond (the metabolites of NE-21610 were not identified). For the in vitro studies a range of receptor solutions was employed to determine a set of conditions that best mimicked in vivo absorption. The results with phosphate-buffered saline containing a preservative and 1–6% polyoxyethylene-20 oleyl ether (Oleth-20) were in good agreement with in vivo results for all three compounds for periods up to 24 h post-dose; after this time, in vivo absorption rates declined but in vitro rates remained relatively constant. Buffered saline or saline containing 0.5% bovine serum albumin led to marked underestimates of in vivo penetration for olvanil and NE-21610, whereas a 1:1 ethanol: water solution led to gross overestimates of the in vivo absorption rates for all three compounds.
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