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首页> 外文期刊>Biological & pharmaceutical bulletin >Electrically-assisted skin permeation of two synthetic capsaicin derivatives, sodium nonivamide acetate and sodium nonivamide propionate, via rate-controlling polyethylene membranes.
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Electrically-assisted skin permeation of two synthetic capsaicin derivatives, sodium nonivamide acetate and sodium nonivamide propionate, via rate-controlling polyethylene membranes.

机译:通过速率控制聚乙烯膜对两种合成的辣椒素衍生物(壬酸酰胺乙酸钠和壬酸酰胺丙酸钠)进行电辅助皮肤渗透。

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摘要

The objective of this study was to examine the transdermal delivery of sodium nonivamide acetate (SNA) using iontophoresis and electroporation with ultra high molecular weight polyethylene membranes (Solupor) to achieve controlled transdermal drug delivery. A derivative of SNA, sodium nonivamide propionate (SNP), was also used as a model drug in this investigation. Iontophoresis increased the transdermal permeation of SNA as compared to passive diffusion. Most Solupor membranes were rate-limiting for the iontophoretic permeation of SNA except for Solupor 8P07, which showed negligible resistance to SNA delivery. The tortuosity (Gurley number), pore size, and the current density-induced attachments on the surface of the Solupor membranes may have been important for their rate-controlling effect. The trends for inhibiting or controlling SNA permeation were similar for both iontophoretic and electroporation applications. The higher molecular size and lower hydrophilicity of SNP compared to SNA resulted in lower permeation of SNP using electrically-assisted methods. Moreover, the various types of Solupor membranes showed similar trends for both SNA and SNP. This present study indicates that Solupor membranes act as rate-limiting membranes for controlling the release and skin permeation of both SNA and SNP by electrically-assisted methods.
机译:这项研究的目的是使用离子电渗疗法和超高分子量聚乙烯膜(Solupor)的电穿孔技术来检查壬基酰胺乙酸钠(SNA)的透皮给药,以实现受控的透皮给药。 SNA的衍生物壬酸酰胺丙酸钠(SNP)也用作本研究的模型药物。与被动扩散相比,离子电渗疗法增加了SNA的透皮渗透性。除Solupor 8P07表现出对SNA传递的阻力可忽略不计外,大多数Solupor膜都限制了SNA的电渗渗透。曲折度(Gurley数),孔径和Solupor膜表面上电流密度引起的附着可能对它们的速率控制效果很重要。对于离子电渗疗法和电穿孔应用,抑制或控制SNA渗透的趋势相似。与SNA相比,SNP的分子大小较高且亲水性较低,因此使用电辅助方法可降低SNP的渗透性。而且,各种类型的Solupor膜对SNA和SNP都显示出相似的趋势。本研究表明Solupor膜可作为限速膜,通过电辅助方法控制SNA和SNP的释放和皮肤渗透。

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