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首页> 外文期刊>Drug Design, Development and Therapy >Controlled release of optimized electroporation enhances the transdermal efficiency of sinomenine hydrochloride for treating arthritis in vitro and in clinic
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Controlled release of optimized electroporation enhances the transdermal efficiency of sinomenine hydrochloride for treating arthritis in vitro and in clinic

机译:优化电穿孔的控制释放提高了青藤碱盐酸盐在体外和临床中治疗关节炎的透皮效率

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Sinomenine hydrochloride (SH) is an ideal drug for the treatment of rheumatoid arthritis and osteoarthritis. However, high plasma concentration of systemically administered SH can release histamine, which can cause rash and gastrointestinal side effects. Topical delivery can increase SH concentration in the synovial fluid without high plasma level, thus minimizing systemic side effects. However, passive diffusion of SH was found to be inefficient because of the presence of the stratum corneum layer. Therefore, an effective method is required to compensate for the low efficiency of SH passive diffusion. In this study, transdermal experiments in vitro and clinical tests were utilized to explore the optimized parameters for electroporation of topical delivery for SH. Fluorescence experiment and hematoxylin and eosin staining analysis were performed to reveal the mechanism by which electroporation promoted permeation. In vitro, optimized electroporation parameters were 3 KHz, exponential waveform, and intensity 10. Using these parameters, transdermal permeation of SH was increased by 1.9–10.1 fold in mice skin and by 1.6–47.1 fold in miniature pig skin compared with passive diffusion. After the electroporation stimulation, the intercellular intervals and epidermal cracks in the skin increased. In clinical tests, SH concentration in synovial fluid was 20.84 ng/mL after treatment with electroporation. Therefore, electroporation with optimized parameters could significantly enhance transdermal permeation of SH. The mechanism by which electroporation promoted permeation was that the electronic pulses made the skin structure looser. To summarize, electroporation may be an effective complementary method for transdermal permeation of SH. The controlled release of electroporation may be a promising clinical method for transdermal drug administration.
机译:盐酸青藤碱(SH)是治疗类风湿关节炎和骨关节炎的理想药物。然而,全身给药的SH的高血浆浓度会释放组胺,这可能引起皮疹和胃肠道副作用。局部给药可增加滑膜液中SH的浓度,而无高血浆水平,从而使全身性副作用降至最低。然而,由于角质层的存在,SH的被动扩散效率低下。因此,需要一种有效的方法来补偿SH无源扩散的低效率。在这项研究中,利用体外和临床试验的透皮实验来探索用于SH局部递送电穿孔的优化参数。进行荧光实验以及苏木精和曙红染色分析以揭示电穿孔促进渗透的机理。在体外,优化的电穿孔参数为3 KHz,指数波形和强度10。使用这些参数,与被动扩散相比,小鼠皮肤中SH的透皮渗透增加了1.9-10.1倍,小型猪皮肤中SH的透皮渗透增加了1.6-47.1倍。电穿孔刺激后,皮肤的细胞间隔和表皮裂纹增加。在临床测试中,电穿孔治疗后滑液中SH浓度为20.84 ng / mL。因此,具有优化参数的电穿孔可以显着增强SH的透皮渗透性。电穿孔促进渗透的机制是电子脉冲使皮肤结构松弛。综上所述,电穿孔可能是SH透皮渗透的有效补充方法。电穿孔的控制释放可能是用于经皮给药的有前途的临床方法。

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