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(Xenical+GSF) 对缺血再灌注引起的血脑屏障破坏、离子水肿、脂质失调和神经炎症的保护作用。

Protective effect of (Xenical+GSF) against I/R-induced blood brain barrier disruption, ionic edema, lipid deregulation and neuroinflammation.

机构信息

Bioactive Substances Laboratory, Biotechnology Centre, Technopolis Borj-Cedria, BP-901, 2050 Hammam-Lif, Tunis, Tunisia.

Bioactive Substances Laboratory, Biotechnology Centre, Technopolis Borj-Cedria, BP-901, 2050 Hammam-Lif, Tunis, Tunisia.

出版信息

Microvasc Res. 2020 Nov;132:104054. doi: 10.1016/j.mvr.2020.104054. Epub 2020 Aug 5.

Abstract

Ischemic stroke is a leading cause of mortality worldwide that occurs following the reduction or interruption of blood brain supply, characterized by a cascade of early events as oxidative stress and ensuing neuro-inflammation, energy failure and the burst of intracellular Ca++ resulting in activation of phospholipases and large increase in FFA including arachidonic acid, ultimately leading to nervous cell death. Grape Seed Flour (GSF) is a complex polyphenolic mixture harboring antioxidant, anti-inflammatory and neuroprotective properties. Orlistat (Xenical ™,Xe) is a gastro-intestinal lipase inhibitor and an anti-obesity agent. In an earlier study we reported the higher efficiency in neuroprotection against HFD-induced brain lipotoxicity when combining the two drugs (GSF + Xe). As a result repurposing Xe as an adjunct to GSF therapy against stroke appeared relevant and worthy of investigation. I/R insult disrupted the blood brain barrier (BBB) as assessed by EB dye extravasation, increased water and Na within the brain. Ultrastructurally I/R altered the brain blood capillaries at the vicinity of hippocampus dentate gyrus area as assessed by transmission and scanning electron microscopy. I/R altered lipid metabolism as revealed by LDL/HDL ratio, lipase activity, and FFA profiles. Moreover, I/R induced neuro-inflammation as assessed by down-regulation of anti-inflammatory CD 56 and up-regulation of pro-inflammatory CD 68 antigen. Importantly almost all I/R-induced disturbances were retrieved partially upon Xe or GSF on their own, and optimally when combining the two drugs. Xe per se is protective against I/R injury and the best neuroprotection was obtained when associating low dosage Xe with high dosage GSF, enabling neuroprevention and cell survival within hippocampus dentate gyrus area as revealed by increased staining of Ki 67 proliferation biomarker.

摘要

缺血性中风是全球范围内导致死亡的主要原因,它发生在血液供应减少或中断后,其特征是一系列早期事件,如氧化应激和随之而来的神经炎症、能量衰竭以及细胞内 Ca++的爆发,导致磷脂酶的激活和大量游离脂肪酸(FFA)的增加,包括花生四烯酸,最终导致神经细胞死亡。葡萄籽粉(GSF)是一种复杂的多酚混合物,具有抗氧化、抗炎和神经保护作用。奥利司他(Xenical ™,Xe)是一种胃肠脂肪酶抑制剂和抗肥胖药物。在之前的一项研究中,我们报告了联合使用这两种药物(GSF+Xe)对高脂饮食诱导的脑脂毒性的神经保护作用更高。因此,将 Xe 重新用于与 GSF 联合治疗中风似乎是相关的,值得进一步研究。I/R 损伤破坏了血脑屏障(BBB),通过 EB 染料渗出来评估;增加了脑内的水和 Na。超微结构研究显示,I/R 通过透射和扫描电子显微镜改变了海马齿状回区附近的脑毛细血管。I/R 改变了脂质代谢,表现为 LDL/HDL 比值、脂肪酶活性和 FFA 谱的改变。此外,I/R 通过下调抗炎性 CD56 和上调促炎性 CD68 抗原诱导了神经炎症。重要的是,几乎所有的 I/R 诱导的紊乱在 Xe 或 GSF 单独使用时都部分恢复,当联合使用两种药物时恢复最佳。Xe 本身对 I/R 损伤有保护作用,当低剂量 Xe 与高剂量 GSF 联合使用时,神经保护效果最佳,这使得海马齿状回区的神经预防和细胞存活成为可能,这一点通过 Ki 67 增殖生物标志物的染色增加得到了证实。

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