Percutaneous absorption of vanilloids: In vivo and in vitro studies

被引:34
|
作者
Kasting, GB
Francis, WR
Bowman, LA
Kinnett, GO
机构
[1] Procter and Gamble Company, Miami Valley Laboratories, Cincinnati
关键词
D O I
10.1021/js950484a
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
The percutaneous absorption of three highly lipophilic analogs of capsaicin-vanillylnonanamide (VN), olvanil, and NE-21610-was 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 approximate to 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 who 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 viva absorption rates for all three compounds.
引用
收藏
页码:142 / 146
页数:5
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