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基于热塑性弹性体的药物粘附基质:经皮吸收、粘附和皮肤刺激性评价。

A drug-in-adhesive matrix based on thermoplastic elastomer: evaluation of percutaneous absorption, adhesion, and skin irritation.

机构信息

School of Pharmacy, East China University of Science and Technology, Shanghai, 200237, China.

出版信息

AAPS PharmSciTech. 2012 Dec;13(4):1179-89. doi: 10.1208/s12249-012-9849-5. Epub 2012 Sep 8.

Abstract

A novel drug-in-adhesive matrix was designed and prepared. A thermoplastic elastomer, styrene-isoprene-styrene (SIS) block copolymer, in combination with tackifying resin and plasticizer, was employed to compose the matrix. Capsaicin was selected as the model drug. The drug percutaneous absorption, adhesion properties, and skin irritation were investigated. The results suggested that the diffusion through SIS matrix was the rate-limiting step of capsaicin percutaneous absorption. [SI] content in SIS and SIS proportions put important effects on drug penetration and adhesion properties. The chemical enhancers had strong interactions with the matrix and gave small effect on enhancement of drug skin permeation. The in vivo absorption of samples showed low drug plasma peaks and a steady and constant plasma level for a long period. These results suggested that the possible side effects of drug were attenuated, and the pharmacological effects were enhanced with an extended therapeutic period after application of SIS matrix. The significant differences in pharmacokinetic parameters produced by different formulations demonstrated the influences of SIS copolymer on drug penetrability. Furthermore, the result of skin toxicity test showed that no skin irritation occurred in guinea pig skin after transdermal administration of formulations.

摘要

设计并制备了一种新型的药物粘附基质。采用热塑性弹性体苯乙烯-异戊二烯-苯乙烯(SIS)嵌段共聚物,并结合增粘树脂和增塑剂来组成基质。辣椒素被选为模型药物。考察了药物经皮吸收、粘附性能和皮肤刺激性。结果表明,SIS 基质的扩散是辣椒素经皮吸收的限速步骤。SIS 中的[SI]含量和 SIS 比例对药物渗透和粘附性能有重要影响。化学增强剂与基质具有强烈的相互作用,对药物皮肤渗透的增强作用较小。体内吸收研究表明,样品的药物血浆峰浓度较低,且在较长时间内呈现稳定且持续的血浆水平。这些结果表明,应用 SIS 基质后,药物的可能副作用减轻,药效增强,治疗期延长。不同配方的药代动力学参数的显著差异表明 SIS 共聚物对药物渗透性的影响。此外,皮肤毒性试验结果表明,经皮给予制剂后豚鼠皮肤无刺激性。

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