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新型川芎嗪储库型透皮贴剂与川芎嗪磷酸盐口服片剂在健康正常志愿者中的单、多剂量药代动力学及体外/体内相关性。

Single- and multiple-dose pharmacokinetics of a novel tetramethylpyrazine reservoir-type transdermal patch versus tetramethylpyrazine phosphate oral tablets in healthy normal volunteers, and in vitro/in vivo correlation.

机构信息

Key Laboratory of Smart Drug Delivery, Ministry of Education & PLA, Department of Pharmaceutics, School of Pharmacy, Fudan University, Shanghai, China.

出版信息

Biol Pharm Bull. 2013;36(6):931-7. doi: 10.1248/bpb.b12-00909. Epub 2013 Mar 19.

Abstract

A novel reservoir-type transdermal system of 2,3,5,6-tetramethylpyrazine (TMP) was developed containing eucalyptus oil as a penetration enhancer. The single and multiple-dose pharmacokinetic profiles of TMP administrated by TMP transdermal patch were characterized in healthy volunteers using an in vivo, randomized, open-label, two-way crossover design. 2,3,5,6-Tetramethylpyrazine phosphate (TMPP) oral tablets were chosen as reference. Following single/multiple oral administration of 200/100 mg TMPP tablets, a TMP C(max) of 1284/613.5 ng/mL was observed within 0.75 h. Single/multiple applications of the TMP patch yielded mean C(max) of 309/325 ng/mL at a median T(max) of 5/4 h, with steady state achieved at second application. The mean C(min) of the patch was 131±30.38 ng/mL, contrasting to nearly zero for the tablet. Multiple applications of patch produced an accumulative effect over single application. At steady state 250 mg/20 cm(2) TMP patch given daily provided comparable exposure to 100 mg TMPP tablets three times daily (3753.91 versus 3563.67 ng·h/mL). TMP tablets and patch yielded similar steady-state plasma concentrations: C(av) (148.48±51.27, 156.41±40.31 ng/mL). The results demonstrated that TMP patch can achieve a therapeutic effect that is comparable to oral administration, exhibited prolonged and sustained plasma levels, fewer drug fluctuations, lower adverse effects, more convenience, and improved patient compliance. In-vitro permeation through human skin demonstrated zero-order kinetics with the flux of 364 µg/cm(2)/h. The predicted C(av) (163.9 ng/mL) was in agreement with the observed C(av) (156.4 ng/mL).

摘要

开发了一种含有桉树油作为渗透促进剂的新型 2,3,5,6-四甲基吡嗪(TMP)储库型透皮贴剂。采用体内、随机、开放标签、两交叉设计,在健康志愿者中对 TMP 透皮贴剂给予 TMP 的单剂量和多剂量药代动力学特征进行了描述。选择 2,3,5,6-四甲基吡嗪磷酸盐(TMPP)口服片剂作为参比制剂。给予 200/100mg TMPP 片剂单/多次口服后,在 0.75h 内观察到 TMP 的 Cmax 为 1284/613.5ng/mL。TMP 贴剂单/多次应用的 Cmax 均值分别为 309/325ng/mL,Tmax 中位数分别为 5/4h,第二次应用时达到稳态。贴剂的 Cmin 均值为 131±30.38ng/mL,而片剂则接近零。贴剂多次应用产生的蓄积效应超过单次应用。在稳态下,每天给予 250mg/20cm2 的 TMP 贴剂可提供与每日三次给予 100mg TMPP 片剂(3753.91 与 3563.67ng·h/mL)相当的暴露量。TMP 片剂和贴剂产生相似的稳态血浆浓度:Cav(148.48±51.27,156.41±40.31ng/mL)。结果表明,TMP 贴剂可以达到与口服相当的治疗效果,表现出延长和持续的血浆水平、较少的药物波动、较低的不良反应、更方便、提高患者依从性。体外经人皮肤渗透实验显示零级动力学,通量为 364µg/cm2/h。预测的 Cav(163.9ng/mL)与观察到的 Cav(156.4ng/mL)一致。

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