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司来吉兰(L-Deprenyl)减轻了氧化应激、认知障碍和大鼠的组织病理学改变:短暂性全脑缺血的替代治疗。

Selegiline (L-Deprenyl) Mitigated Oxidative Stress, Cognitive Abnormalities, and Histopathological Change in Rats: Alternative Therapy in Transient Global Ischemia.

机构信息

Zanjan Applied Pharmacology Research Center, Zanjan University of Medical sciences, Zanjan, Iran.

Department of Pharmacology and Toxicology, School of Pharmacy, Zanjan University of Medical Sciences, P.O. Box: 45139-56184, Zanjan, Iran.

出版信息

J Mol Neurosci. 2020 Oct;70(10):1639-1648. doi: 10.1007/s12031-020-01544-5. Epub 2020 Jun 1.

Abstract

Selegiline (L-deprenyl) is the major drug which is used in the treatment of Parkinson's disease because of its neurotrophic and antiapoptotic properties. Previous studies suggested that low dose of L-methamphetamine (L-METH) caused lower mortality rate in patients with severe traumatic brain injury. As L-methamphetamine is one of the metabolites of selegiline, the present study aims to examine whether L-deprenyl can improve cognitive, biochemical, and histopathological injury in animal model of transient global ischemia. The animals were randomized in ten groups orally gavaged three times a week for 28 days. Then, novel object recognition (NOR) was conducted to assess their behavioral abnormality. After scarification of the rats, their brains were divided into two sections to measure oxidative stress parameters and perform pathological evaluations in rats. Our data revealed the involvement of oxidative stress, behavioral despair, and pathological data in transient global ischemia rats. Significant recovery in cognitive behavior, oxidative stress biomarker, and number of dead cell in histopathological assay was observed in rats treated with 1,2 and 4 mg/kg of selegiline. So, selegiline appears to be useful in alternative therapy of transient global ischemia.

摘要

司来吉兰(L-丙炔苯丙胺)是一种用于治疗帕金森病的主要药物,因为它具有神经营养和抗细胞凋亡的特性。先前的研究表明,低剂量的 L-甲基苯丙胺(L-METH)可降低严重创伤性脑损伤患者的死亡率。由于 L-甲基苯丙胺是司来吉兰的一种代谢物,本研究旨在检查 L-丙炔苯丙胺是否可以改善短暂性全脑缺血动物模型中的认知、生化和组织病理学损伤。动物随机分为十组,每周口服三次,共 28 天。然后,进行新物体识别(NOR)以评估它们的行为异常。在大鼠处死之后,将它们的大脑分为两部分,以测量氧化应激参数并进行大鼠的病理评估。我们的数据显示,氧化应激、行为绝望和短暂性全脑缺血大鼠的病理数据参与其中。在接受 1、2 和 4mg/kg 司来吉兰治疗的大鼠中,观察到认知行为、氧化应激生物标志物和组织病理学检测中死亡细胞数量的显著恢复。因此,司来吉兰似乎可用于短暂性全脑缺血的替代治疗。

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