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首页> 外文期刊>Neurochemical Research >Changes in iNOS, GFAP and NR1 Expression in Various Brain Regions and Elevation of Sphingosine-1-phosphate in Serum after Immobilized Stress
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Changes in iNOS, GFAP and NR1 Expression in Various Brain Regions and Elevation of Sphingosine-1-phosphate in Serum after Immobilized Stress

机译:固定应激后各脑区iNOS,GFAP和NR1表达的变化及血清1-磷酸鞘氨醇水平的升高

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摘要

Several studies have been suggested that long-term exposure to stress has detrimental effects on various brain functions and leads to neurodegenerative changes. However, the precise mechanism by which stress induces brain damage or neurodegenerative change is still a matter of debate. This study investigated the damage of neuronal cells involving in the expression of iNOS, NR1, and GFAP in various brain regions and characterized the change of sphingolipid metabolites as a biomarker of physiological change in serum after 3 weeks of repeated immobilization. In this report, the expression of iNOS, GFAP and NR1 in the brain of rats exposed to chronic immobilization stress was investigated. The expression of iNOS, GFAP and NR1 was elevated in the cortex and hippocampal area after 3 weeks of repeated immobilization. Immunoreactivity for GFAP and vimentin, as a marker of reactive gliosis, was also elevated in the cortex and hippocampus. The level of sphingolipids was measured in order to assess the changes in sphingolipid metabolites in the serum of rats exposed to stress. Interestingly, the level of So-1-P was increased in the plasma of rats subjected to 6-h immobilization stress than repeated immobilization. To further investigate the modulating effect of increased So-1-P in various brain regions, So-1-P was infused into the lateral cerebroventricle at a rate of 100 pmol/10 μl/h for 7 days. The expression of iNOS and NR1 was elevated in the cortex, hippocampus, striatum, and cerebellum after So-1-P infusion into the cerebroventricle, while the level of GFAP was elevated in the hippocampus and striatum. Interestingly, the expression levels of iNOS, GFAP, and NR1 were increased by the direct application of So-1-P to cultured cortical cells. These results suggest that NO production via iNOS expression, the NR1 expression, the activation of astrocytes, and the elevation of So-1-P may cause neurodegenerative changes in rats subjected to chronic immobilization and that the elevation of So-1-P by stress exposure would be one of the stress signal molecules.
机译:已有多项研究表明,长期暴露于压力下会对各种大脑功能产生有害影响,并导致神经退行性改变。但是,压力引起脑损伤或神经退行性改变的确切机制仍是一个有争议的问题。这项研究调查了涉及iNOS,NR1和GFAP在各个大脑区域表达的神经元细胞的损伤,并表征了鞘脂代谢产物的变化是反复固定3周后血清生理变化的生物标志。在本报告中,研究了iNOS,GFAP和NR1在慢性固定应激大鼠脑中的表达。重复固定3周后,皮质和海马区iNOS,GFAP和NR1的表达升高。作为反应性胶质增生的标志物,GFAP和波形蛋白的免疫反应性在皮质和海马中也升高。测量鞘脂的水平以评估暴露于应激的大鼠血清中鞘脂代谢产物的变化。有趣的是,与反复固定相比,在6 h固定压力下大鼠血浆中So-1-P的水平增加了。为了进一步研究增加的So-1-P在大脑各个区域的调节作用,将So-1-P以100 pmol / 10μl/ h的速率注入脑侧脑室,持续7天。 So-1-P输注到脑室内后,iNOS和NR1的表达在皮质,海马,纹状体和小脑中升高,而在海马和纹状体中GFAP的水平升高。有趣的是,通过将So-1-P直接应用于培养的皮层细胞,iNOS,GFAP和NR1的表达水平得以提高。这些结果表明,通过iNOS表达,NR1表达,星形胶质细胞活化以及So-1-P升高引起的NO产生可能导致慢性固定大鼠的神经退行性改变,以及应激导致So-1-P升高暴露将是压力信号分子之一。

著录项

  • 来源
    《Neurochemical Research》 |2008年第5期|842-851|共10页
  • 作者单位

    Department of Neuroscience and Medical Research Institute School of Medicine Ewha Womans University Mok-dong Yangchon-ku Seoul 158-710 Korea;

    Department of Physiology School of Medicine Ewha Womans University Seoul 158-710 Korea;

    College of Pharmacy Chungbuk National University Cheongju 361-763 Korea;

    College of Pharmacy Chungbuk National University Cheongju 361-763 Korea;

    Department of Neuroscience and Medical Research Institute School of Medicine Ewha Womans University Mok-dong Yangchon-ku Seoul 158-710 Korea;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Sphingolipid; Stress; iNOS; GFAP; NR1;

    机译:鞘脂;应力;iNOS;GFAP;NR1;

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