Orexin-A通过调节小胶质细胞和星形胶质细胞的氧化应激和抑制ERK/NF-κB信号通路减轻败血症相关脑病的炎症反应

IF 4.8 1区 医学 Q1 NEUROSCIENCES CNS Neuroscience & Therapeutics Pub Date : 2024-11-07 DOI:10.1111/cns.70096
Jing Guo, Dexun Kong, Junchi Luo, Tao Xiong, Fang Wang, Mei Deng, Zhuo Kong, Sha Yang, Jingjing Da, Chaofei Chen, Jinhai Lan, Liangzhao Chu, Guoqiang Han, Jian Liu, Ying Tan, Jiqin Zhang
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引用次数: 0

摘要

背景:氧化应激诱导的炎症是败血症相关脑病(SAE)的主要致病机制。我们假设神经肽奥曲肽-A对活性氧(ROS)的调节可预防脓毒症相关脑病诱发的氧化应激和炎症。因此,本研究旨在探讨奥曲肽-A对小鼠SAE氧化应激和炎症的影响:用奥曲肽-A(250 μg/kg,鼻内给药)治疗成年雄性小鼠,建立盲肠结扎穿孔(CLP)模型。我们进行了行为测试,观察了海马区神经元的损伤,测量了 ROS 和 NOX2 的水平,并通过透射电子显微镜观察了线粒体的结构。然后,我们检测了炎症因子TNF-α和IL-1β、小胶质细胞和星形胶质细胞的活化、ERK/NF-κB、C3和S100A10的表达以及A1型星形胶质细胞和A2型星形胶质细胞的存在:结果:奥曲肽-A治疗改善了CLP诱导的SAE小鼠的认知能力,减轻了海马区神经元凋亡,改善了ROS水平和线粒体损伤程度,降低了海马组织中NOX2的蛋白表达。此外,奥曲肽-A还能显著降低小胶质细胞和星形胶质细胞的活化,抑制P-ERK和NF-κB的水平,减少IL-1β和TNF-α的释放。最后,奥曲肽-A能显著减少C3/胶质纤维酸性蛋白(GFAP)阳性细胞的数量,并增加S100A10/GFAP阳性细胞的数量:我们的数据表明,奥曲肽-A可通过抑制CLP诱导的NOX2的产生来减少ROS的表达,从而减轻线粒体损伤和神经元凋亡。它对小胶质细胞和 A1 型星形胶质细胞活化和炎症的抑制与 ERK/NF-κB 通路有关。这表明奥曲肽-A可通过减少氧化应激诱导的炎症来减轻SAE的认知障碍。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Orexin-A Attenuates the Inflammatory Response in Sepsis-Associated Encephalopathy by Modulating Oxidative Stress and Inhibiting the ERK/NF-κB Signaling Pathway in Microglia and Astrocytes

Background

Oxidative stress-induced inflammation is a major pathogenic mechanism in sepsis-associated encephalopathy (SAE). We hypothesized that regulation of reactive oxygen species (ROS) by the neuropeptide orexin-A could prevent SAE-induced oxidative stress and inflammation. Therefore, the aim of this study was to investigate the effects of orexin-A on oxidative stress and inflammation in SAE in mice.

Methods

Adult male mice were treated with orexin-A (250 μg/kg, intranasal administration) to establish a cecal ligation perforation (CLP) model. We performed behavioral tests, observed neuronal damage in the hippocampal region, measured the levels of ROS, NOX2, and observed the structure of mitochondria by transmission electron microscopy. We then examined the inflammatory factors TNF-α and IL-1β, the activation of microglia and astrocytes, the expression of ERK/NF-κB, C3, and S100A10, and the presence of A1 type astrocytes and A2 type astrocytes.

Results

Orexin-A treatment improved cognitive performance in CLP-induced SAE mice, attenuated neuronal apoptosis in the hippocampal region, ameliorated ROS levels and the extent of mitochondrial damage, and reduced protein expression of NOX2 in hippocampal tissue. In addition, orexin-A treatment significantly reduced microglia and astrocyte activation, inhibited the levels of P-ERK and NF-κB, and reduced the release of IL-1β and TNF-α, which were significantly increased after CLP. Finally, Orexin-A treatment significantly decreased the number of C3/glial fibrillary acidic protein (GFAP)-positive cells and increased the number of S100A10/GFAP-positive cells.

Conclusion

Our data suggest that orexin-A reduces ROS expression by inhibiting CLP-induced NOX2 production, thereby attenuating mitochondrial damage and neuronal apoptosis. Its inhibition of microglial and A1-type astrocyte activation and inflammation was associated with the ERK/NF-κB pathway. These suggest that orexin-A may reduce cognitive impairment in SAE by reducing oxidative stress-induced inflammation.

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来源期刊
CNS Neuroscience & Therapeutics
CNS Neuroscience & Therapeutics 医学-神经科学
CiteScore
7.30
自引率
12.70%
发文量
240
审稿时长
2 months
期刊介绍: CNS Neuroscience & Therapeutics provides a medium for rapid publication of original clinical, experimental, and translational research papers, timely reviews and reports of novel findings of therapeutic relevance to the central nervous system, as well as papers related to clinical pharmacology, drug development and novel methodologies for drug evaluation. The journal focuses on neurological and psychiatric diseases such as stroke, Parkinson’s disease, Alzheimer’s disease, depression, schizophrenia, epilepsy, and drug abuse.
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