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白细胞介素-17 和谷氨酸兴奋性毒性在多发性硬化症发病机制中的作用。

IL-17 and glutamate excitotoxicity in the pathogenesis of multiple sclerosis.

机构信息

Department of Immunology, Medical Faculty, University of Nis, Nis, Serbia.

出版信息

Scand J Immunol. 2014 Mar;79(3):181-6. doi: 10.1111/sji.12147.

Abstract

Immunoinflammatory-mediated demyelination, the main pathological feature of multiple sclerosis (MS), is regularly accompanied by neurodegenerative processes, mostly in the form of axonal degeneration, which could be initiated by glutamate excitotoxicity. In the current study, the relationship between Th17-mediated inflammatory and excitotoxic events was investigated during an active phase of MS. Cerebrospinal fluid (CSF) of patients with MS and control subjects was collected, and IL-17A and glutamate levels were determined. IL-17A level was significantly higher in patients with MS; whereas no statistically significant changes in glutamate concentrations were found. There was a direct correlation between IL-17A and glutamate levels; IL-17A levels were also associated with the neutrophil expansion in CSF and blood-brain barrier disruption. However, IL-17A level and the number of neutrophils tended to fall with disease duration. The results suggest that Th17 cells might enhance and use glutamate excitotoxicity as an effector mechanism in the MS pathogenesis. Furthermore, Th17 immune response, as well as neutrophils, could be more important for MS onset rather than further disease development and progression, what could explain why some MS clinical trials, targeting Th17 cells in the later stage of the disease, failed to provide any clinical benefit.

摘要

免疫炎症介导的脱髓鞘是多发性硬化症(MS)的主要病理特征,常伴有神经退行性过程,主要表现为轴突变性,其可能由谷氨酸兴奋性毒性引发。在本研究中,我们研究了 MS 活动期 Th17 介导的炎症和兴奋性事件之间的关系。收集了 MS 患者和对照者的脑脊液(CSF),并测定了白细胞介素 17A(IL-17A)和谷氨酸的水平。MS 患者的 IL-17A 水平显著升高,而谷氨酸浓度没有统计学上的显著变化。IL-17A 水平与谷氨酸水平之间存在直接相关性;IL-17A 水平还与 CSF 和血脑屏障破坏时的中性粒细胞扩增有关。然而,IL-17A 水平和中性粒细胞数量随着疾病持续时间的延长而趋于下降。研究结果表明,Th17 细胞可能增强并利用谷氨酸兴奋性毒性作为 MS 发病机制中的效应机制。此外,Th17 免疫反应以及中性粒细胞可能对 MS 的发病更为重要,而不是疾病的进一步发展和进展,这可以解释为什么一些针对疾病后期 Th17 细胞的 MS 临床试验未能提供任何临床益处。

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