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经皮传递硫酸阿托品的离子电渗和微针介导技术。

Iontophoretic and microneedle mediated transdermal delivery of glycopyrrolate.

机构信息

Department of Pharmaceutical Sciences, Mercer University, 3001 Mercer University Drive, Atlanta, GA 30341, USA.

出版信息

Pharmaceutics. 2014 Dec 22;6(4):663-71. doi: 10.3390/pharmaceutics6040663.

Abstract

PURPOSE

The objective of this study was to investigate the use of iontophoresis, soluble microneedles and their combination for the transdermal delivery of glycopyrrolate.

METHODS

In vitro permeation was tested using full thickness porcine ear skin mounted onto Franz diffusion cells. Iontophoresis (0.5 mA/cm2) was done for 4 h using Ag/AgCl electrodes. For microneedles, three line array (27 needles/line) of maltose microneedles were used to microporate the skin prior to mounting. Pore uniformity was determined by taking fluorescent images of distribution of calcein into pores and processing the images using an image analysis tool, which measured the fluorescent intensity in and around each pore to provide a pore permeability index (PPI). The donor chamber contained 500 µL of a 1 mg/mL solution of glycopyrrolate, and the receptor chamber contained 5 mL of 50 mM NaCl in deionized water. Samples were collected at predetermined time points over a period of 24 h and analyzed by HPLC. Skin irritation testing was performed with a 3D cell culture kit of human skin. MTT assay determined cell viability; viability less than 50% was considered irritant.

RESULTS

A control experiment which investigated passive permeation of glycopyrrolate delivered an average cumulative amount of 24.92 ± 1.77 µg/cm2 at 24 h, while microneedle pretreatment increased permeability to 46.54 ± 6.9 µg/cm2. Both iontophoresis (158.53 ± 17.50 µg/cm2) and a combination of iontophoresis and microneedles (182.43 ± 20.06 µg/ cm2) significantly increased delivery compared to passive and microneedles alone. Glycopyrrolate solution was found to be nonirritant with cell viability of 70.4% ± 5.03%.

CONCLUSION

Iontophoresis and a combination of iontophoresis with microneedle pretreatment can be effectively used to enhance the transdermal delivery of glycopyrrolate. Glycopyrrolate was found to be non-irritant to skin.

摘要

目的

本研究旨在探讨离子导入、可溶性微针及其联合应用于硫酸阿托品透皮给药的效果。

方法

采用全层猪耳皮肤进行Franz 扩散池体外渗透实验。Ag/AgCl 电极进行 0.5 mA/cm2 的离子导入 4 小时。对于微针,使用 3 行(每行 27 针)麦芽糖微针预先刺穿皮肤。通过将 calcein 分布到毛孔中的荧光图像进行处理,使用图像分析工具测量每个毛孔内及周围的荧光强度,以提供毛孔渗透率指数(PPI)来确定毛孔均匀性。供体室含有 500µL 浓度为 1mg/mL 的硫酸阿托品溶液,受体室含有 5mL 去离子水中的 50mM NaCl。在 24 小时的预定时间点收集样品,并通过 HPLC 进行分析。采用人皮肤 3D 细胞培养试剂盒进行皮肤刺激性测试。MTT 测定细胞活力;活力低于 50%被认为是刺激性的。

结果

一项研究硫酸阿托品被动渗透的对照实验显示,24 小时时平均累积量为 24.92±1.77µg/cm2,而微针预处理可将透皮通量提高至 46.54±6.9µg/cm2。离子导入(158.53±17.50µg/cm2)和离子导入与微针联合应用(182.43±20.06µg/cm2)均显著增加了药物递送量,优于被动和单独使用微针的情况。硫酸阿托品溶液对细胞活力为 70.4%±5.03%,无刺激性。

结论

离子导入和离子导入联合微针预处理可有效增强硫酸阿托品的透皮传递。硫酸阿托品对皮肤无刺激性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2950/4279139/5549a9a0ce49/pharmaceutics-06-00663-g001.jpg

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