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新型脂质扩散增强剂经皮递送至人指甲板的环吡酮胺。

Ciclopirox delivery into the human nail plate using novel lipid diffusion enhancers.

机构信息

Dermatology Department, University of California , San Francisco, CA , USA and.

出版信息

Drug Dev Ind Pharm. 2014 Jun;40(6):838-44. doi: 10.3109/03639045.2013.788016. Epub 2013 Apr 19.

DOI:10.3109/03639045.2013.788016
PMID:23600655
Abstract

CONTEXT

Onychomycosis is a common fungal infection of the nail plate and bed that affects up to 14% of the population and can have a substantial impact on the quality of life of those affected.

OBJECTIVE

This study compared the onychopharmacokinetics, nail absorption, nail distribution, and nail penetration of [(14)C]-ciclopirox dissolved in novel lipid diffusion enhancers with that of a commercial ciclopirox nail lacquer using the in vitro finite dose model.

MATERIALS AND METHODS

The penetration rate of ciclopirox was determined by applying doses of topical formulation twice daily to human nail plates for 11 d. Drug absorption was then measured by monitoring its rate of appearance in each nail layer and in the cotton pad/nail supporting bed.

RESULTS

After a multiple day treatment, cumulative concentrations of ciclopirox formulated with lipid enhancers in the deep nail layer and the nail bed were significantly greater than cumulative concentrations of the commercial ciclopirox lacquer (p < 0.001) as well as several orders of magnitude greater than the minimal inhibitory concentration (MIC) deemed necessary to inhibit the growth of the causative dermatophyte species.

CONCLUSION

When formulated with lipid enhancers, the amount of ciclopirox in the ventral/intermediate layer and supporting bed dramatically exceed the inhibitory concentration of ciclopirox for the most common onychomycosis organisms. These results suggest that topical ciclopirox with lipid enhancers has the potential to be an effective topical treatment for onychomycosis, and the lipidic pathway of the nail can be utilized as a means of effective transungual delivery.

摘要

背景

甲真菌病是一种常见的指甲板和床板真菌感染,影响人群高达 14%,会对受影响人群的生活质量产生重大影响。

目的

本研究通过体外有限剂量模型,比较了新型脂质扩散增强剂溶解的 [(14)C]-环吡酮与商业环吡酮指甲油中甲环吡酮的药代动力学、指甲吸收、指甲分布和指甲渗透。

材料和方法

通过每天两次将局部制剂涂抹于人指甲板 11 天来确定环吡酮的渗透速率。然后通过监测其在每个指甲层和棉花垫/指甲支撑床上的出现速度来测量药物吸收。

结果

经过多日治疗,含有脂质增强剂的环吡酮在深层指甲层和指甲床上的累积浓度明显高于商业环吡酮漆(p<0.001),并且比抑制引起甲真菌病的最常见物种生长所需的最小抑菌浓度(MIC)高出几个数量级。

结论

当与脂质增强剂联合配制时,环吡酮在腹侧/中间层和支撑床上的含量大大超过了环吡酮对最常见甲真菌病生物的抑制浓度。这些结果表明,含有脂质增强剂的局部环吡酮有可能成为甲真菌病的有效局部治疗方法,并且指甲的脂质途径可以作为有效的透皮递送手段。

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