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首页> 外文期刊>RSC Advances >Novel ginkgolide B derivative attenuated the function and expression of P-glycoprotein at the blood-brain barrier, presenting brain-targeting ability
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Novel ginkgolide B derivative attenuated the function and expression of P-glycoprotein at the blood-brain barrier, presenting brain-targeting ability

机译:新型银杏内酯B衍生物减弱了P-糖蛋白在血脑屏障中的功能和表达,具有大脑靶向能力

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摘要

A series of ginkgolide B derivatives (GBD) were designed for delivery of ginkgolide B (GB) across the blood-brain barrier to the brain. Three GBD had shown considerable brain-targeting ability in our previous study. Among them, the ginkgolide B pyrazine (PGB) derivative was selected as a promising novel GB derivative because of its highest brain distribution. Further investigations with regard to PGB and GB's effects on inhibiting the expression of P-gp and attenuating the efflux function of P-gp were reported in this study. They were considered a big step towards better understanding the relationship between GBD's brain-targeting behavior and P-gp regulation. Western blot analysis indicated that PGB was more effective in inhibiting the expression of P-gp than GB in rat brain microvessel endothelial cells (rBMECs) and rat cerebral cortexes and hippocampus. Moreover, the efflux function of P-gp via the transportation of rhodamine 123 was significantly inhibited in PGB-treated rat brains. Preventive medication with PGB induced a better protection of the integrity of the BBB in incomplete ischemia mice. Our findings revealed that an attenuated expression level and efflux function of P-gp and improved protective effect could be realized by the ginkgolide B derivative. These investigations will pave the way for designing more efficient brain-targeting derivatives of ginkgolide and some other central nervous system drugs.
机译:设计了一系列银杏内酯B衍生物(GBD),用于将银杏内酯B(GB)跨血脑屏障传递到大脑。在我们之前的研究中,三个GBD已显示出可观的大脑靶向能力。其中,由于银杏内酯B吡嗪(PGB)的最高脑分布,因此被选为有前途的新型GB衍生物。这项研究报道了有关PGB和GB抑制P-gp表达和减弱P-gp外排功能的进一步研究。他们被认为是更好地了解GBD的大脑靶向行为与P-gp调节之间关系的重要一步。 Western blot分析表明,在大鼠脑微血管内皮细胞(rBMECs)和大鼠大脑皮层和海马中,PGB比GB更有效地抑制P-gp的表达。此外,在PGB处理的大鼠脑中,通过若丹明123的转运,P-gp的外排功能被显着抑制。 PGB的预防性药物可在不完全缺血的小鼠中更好地保​​护BBB的完整性。我们的发现表明,银杏内酯B衍生物可实现P-gp的表达水平降低和外排功能增强,保护作用增强。这些研究将为设计更有效的银杏内酯和其他中枢神经系统药物的针对大脑的衍生物铺平道路。

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