中链甘油酯增强罂粟碱的皮肤渗透性。

Drug design and delivery Pub Date : 1991-04-01
M Okumura, Y Nakamori, K Sugibayashi, Y Morimoto
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引用次数: 0

摘要

研究了中链甘油酯和强效透皮吸收促进剂Sefsol-318对盐酸罂粟碱体外通过无毛大鼠皮肤的作用模式和机制,并与laurocapram (Azone)进行了比较。在28小时内,从含有5% S-318或偶氮酮的药物水溶液中通过切除皮肤递送的药物总量分别比单独从溶液中递送的药物总量高820倍或420倍。以脂质体为模型的实验表明,两种增强剂均能显著提高脂质膜的流动性。无毛大鼠的皮肤电导测量表明,它们也增加了体内皮肤的保湿和保水能力。这些结果表明,Sefsol-318与Azone在促进皮肤渗透方面的作用机制相似。但在用5%的Sefsol-318和水乳液对切除皮肤进行体外预处理2小时后,在Sefsol-318存在的情况下,盐酸罂粟碱通过预处理皮肤的皮肤渗透性远低于未经处理的皮肤。相比之下,氮酮对预处理皮肤的增强作用与氮酮对体外未处理皮肤的增强作用相似。我们发现,与氮酮不同的是,Sefsol-318在体内用含有每种药物的水凝胶预处理皮肤24小时后1天从皮肤中完全消失。与此一致的是,用Sefsol-318进行体内预处理后1天切除皮肤的药物渗透与不使用Sefsol-318的未预处理对照组几乎相同。Sefsol-318和Azone在作用方式上的差异可能是由于这些增强剂在皮肤中停留时间的不同。
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Enhanced skin permeation of papaverine by a medium chain glyceride.

The mode and mechanism of action of Sefsol-318, a medium chain glyceride and a potent percutaneous absorption enhancer, on the in vitro permeation of papaverine hydrochloride through hairless rat skin were investigated and compared with those of laurocapram (Azone). The total amount of the drug delivered through excised skin over 28 h from aqueous solutions of the drug in which 5% S-318 or Azone was suspended was about 820 or 420 times higher, respectively, than from the solution alone. Experiments using liposomes as models, indicated that both the enhancers markedly increased the fluidity of lipid membranes. Skin conductance measurements in hairless rats indicated that they both also increased in vivo skin moisturizing and water holding capacity. These results suggest that the mechanism of action of Sefsol-318 and Azone in enhancing skin permeation are similar. But following in vitro pretreatment of the excised skin with 5% Sefsol-318 and aqueous emulsion for 2 h, skin permeation of papaverine hydrochloride through the pretreated skin was much lower than through non-treated skin in the presence of Sefsol-318. In contrast, the enhancing effect of Azone on the pretreated skin was similar to that of Azone on the in vitro non-treated skin. We found that, unlike Azone, Sefsol-318 disappeared from skin completely one day after 24 h-in vivo pretreatment of skin with aqueous gels containing each agent. In agreement, drug permeation through skin excised one day after the in vivo pretreatment with Sefsol-318 was almost the same as in non-pretreated controls without Sefsol-318. This difference in the mode of action of Sefsol-318 and Azone may arise from the difference in the residence times of these enhancers in skin.

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