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甲磺酸雷沙吉兰的控释促进鱼藤酮诱导的帕金森病晚期模型中的神经保护作用。

Controlled release of rasagiline mesylate promotes neuroprotection in a rotenone-induced advanced model of Parkinson's disease.

机构信息

Departamento de Farmacia y Tecnología Farmacéutica, Facultad de Farmacia, Universidad Complutense de Madrid, Madrid, Spain.

出版信息

Int J Pharm. 2012 Nov 15;438(1-2):266-78. doi: 10.1016/j.ijpharm.2012.09.024. Epub 2012 Sep 15.

DOI:10.1016/j.ijpharm.2012.09.024
PMID:22985602
Abstract

Microencapsulation of rasagiline mesylate (RM) into PLGA microspheres was performed by method A (O/W emulsion) and method B (W/O/W double emulsion). The best formulation regarding process yield, encapsulation efficiency and in vitro drug release was that prepared with method A, which exhibited constant drug release for two weeks (K(0)=62.3 μg/day/20mg microspheres). Exposure of SKN-AS cells to peroxide-induced oxidative stress (1 mM) resulted in cell apoptosis which was significantly reduced by RM (40.7-102.5 μM) as determined by cell viability, ROS production and DNA fragmentation. Daily doses of rotenone (2 mg/kg) given i.p. to rats for 45 days induced neuronal and behavioral changes similar to those occurring in PD. Once an advanced stage of PD was achieved, animals received RM in saline (1 mg/kg/day) or encapsulated within PLGA microspheres (amount of microspheres equivalent to 15 mg/kg RM given on days 15 and 30). After 45 days RM showed a robust effect on all analytical outcomes evaluated with non-statistically significant differences found between its administration in solution or within microparticles however; with this controlled release system administration of RM could be performed every two weeks thereby making this new therapeutic system an interesting approach for the treatment of PD.

摘要

甲磺酸雷沙吉兰(RM)的 PLGA 微球的微囊化是通过方法 A(O/W 乳液)和方法 B(W/O/W 双重乳液)进行的。就工艺收率、包封效率和体外药物释放而言,最好的配方是用方法 A 制备的,其表现出持续两周的恒速药物释放(K(0)=62.3μg/天/20mg 微球)。SKN-AS 细胞暴露于过氧化物诱导的氧化应激(1mM)导致细胞凋亡,RM(40.7-102.5μM)显著降低了细胞凋亡,这可以通过细胞活力、ROS 产生和 DNA 片段化来确定。腹腔内给予每日剂量的鱼藤酮(2mg/kg)45 天可诱导类似于 PD 发生的神经元和行为变化。一旦达到 PD 的晚期阶段,动物接受 RM 在生理盐水中(1mg/kg/天)或包封在 PLGA 微球内(相当于在第 15 天和第 30 天给予 15mg/kg RM 的微球数量)。在 45 天之后,RM 对所有评估的分析结果都表现出强大的作用,其在溶液中或微球内的给药之间没有发现统计学上的显著差异;然而,通过这种控释系统可以每两周给予 RM,从而使这种新的治疗系统成为治疗 PD 的一种有趣方法。

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