首页> 美国卫生研究院文献>International Journal of Nanomedicine >Effects of Carbopol® 934 proportion on nanoemulsion gel for topical and transdermal drug delivery: a skin permeation study
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Effects of Carbopol® 934 proportion on nanoemulsion gel for topical and transdermal drug delivery: a skin permeation study

机译:Carbopol®934比例对用于局部和透皮给药的纳米乳胶的影响:皮肤渗透研究

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摘要

Nanoemulsions (NEs) are used as transdermal drug delivery systems for systematic therapeutic purposes. We hypothesized that the skin permeation profile of an NE could be modulated by incorporating it into a hydrogel containing differing proportions of thickening agent. The objectives of this study were as follows: 1) to determine the stability and skin irritability of NE gels (NGs) containing 1%, 2%, and 3% (w/w) Carbopol® 934 (CP934) (termed NG1, NG2, and NG3, respectively); 2) to compare the skin permeation profiles and drug deposition patterns of the NGs; and 3) to visualize the drug delivery routes of the NGs. Terbinafine and citral were incorporated into the NGs as model drugs. Ex vivo skin permeation tests indicated that the percutaneous flux rates of terbinafine decreased in the order NE (215 μg/cm2) > NG1 (213 μg/cm2) > NG2 (123 μg/cm2) > NG3 (74.3 μg/cm2). The flux rates of citral decreased in the order NE (1,026 μg/cm2) > NG1 (1,021 μg/cm2) > NG2 (541 μg/cm2) > NG3 (353 μg/cm2). The NGs accumulated greater amounts of the drugs in the stratum corneum and less in the epidermis/dermis than did the NE (P<0.05) over a period of 12 h. Laser scanning confocal microscopy indicated that the NGs altered the main drug delivery routes from skin appendages to intercellular paths. Histological images suggested that perturbations to the skin structure, specifically the size of the epidermal intercellular spaces and the separation distance of dermal collagen bundles, could be significantly minimized by increasing the proportion of CP934. These results suggest that adjustments of the CP934 proportions can be used to modulate the skin permeation profiles of NGs for specific therapeutic purposes.
机译:纳米乳剂(NEs)用作透皮给药系统的系统治疗用途。我们假设可以通过将NE掺入含有不同比例增稠剂的水凝胶中来调节NE的皮肤渗透特性。这项研究的目的如下:1)确定含有1%,2%和3%(w / w)Carbopol ® 934的NE凝胶(NG)的稳定性和皮肤刺激性( CP934)(分别称为NG1,NG2和NG3); 2)比较NGs的皮肤渗透曲线和药物沉积模式; 3)可视化NG的给药路径。将特比萘芬和柠檬醛作为模型药物掺入NG。离体皮肤渗透测试表明,特比萘芬的经皮通量速率以NE(215μg/ cm 2 )> NG1(213μg/ cm 2 )> NG2的顺序降低(123μg/ cm 2 )> NG3(74.3μg/ cm 2 )。柠檬酸的通量率以NE(1,026μg/ cm 2 )> NG1(1,021μg/ cm 2 )> NG2(541μg/ cm )的顺序降低2 )> NG3(353μg/ cm 2 )。在12小时内,NGs在NE角质层中积聚的药物量更多,而在表皮/真皮中积聚的药物较少(P <0.05)。激光扫描共聚焦显微镜检查表明,NGs改变了主要的药物输送途径,从皮肤附件到细胞间途径。组织学图像表明,通过增加CP934的比例,可以显着减小对皮肤结构的干扰,特别是表皮细胞间空间的大小和真皮胶原束的分离距离。这些结果表明,出于特定的治疗目的,可以将CP934比例的调整用于调节NGs的皮肤渗透曲线。

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