氧化应激和炎症在一系列致痫性皮质发育畸形中的作用:对其相互依赖性的分子认识。
Oxidative stress and inflammation in a spectrum of epileptogenic cortical malformations: molecular insights into their interdependence.
机构信息
Department of (Neuro-)Pathology, Amsterdam UMC, University of Amsterdam, Amsterdam Neuroscience, Meibergdreef 9, Amsterdam, the Netherlands.
Department of Biochemical Sciences, Sapienza University of Rome, Rome, Italy.
出版信息
Brain Pathol. 2019 May;29(3):351-365. doi: 10.1111/bpa.12661. Epub 2018 Nov 20.
Oxidative stress (OS) occurs in brains of patients with epilepsy and coincides with brain inflammation, and both phenomena contribute to seizure generation in animal models. We investigated whether expression of OS and brain inflammation markers co-occurred also in resected brain tissue of patients with epileptogenic cortical malformations: hemimegalencephaly (HME), focal cortical dysplasia (FCD) and cortical tubers in tuberous sclerosis complex (TSC). Moreover, we studied molecular mechanisms linking OS and inflammation in an in vitro model of neuronal function. Untangling interdependency and underlying molecular mechanisms might pose new therapeutic strategies for treating patients with drug-resistant epilepsy of different etiologies. Immunohistochemistry was performed for specific OS markers xCT and iNOS and brain inflammation markers TLR4, COX-2 and NF-κB in cortical tissue derived from patients with HME, FCD IIa, IIb and TSC. Additionally, we studied gene expression of these markers using the human neuronal cell line SH-SY5Y in which OS was induced using H O . OS markers were higher in dysmorphic neurons and balloon/giant cells in cortex of patients with FCD IIb or TSC. Expression of OS markers was positively correlated to expression of brain inflammation markers. In vitro, 100 µM, but not 50 µM, of H O increased expression of TLR4, IL-1β and COX-2. We found that NF-κB signaling was activated only upon stimulation with 100 µM H O leading to upregulation of TLR4 signaling and IL-1β. The NF-κB inhibitor TPCA-1 completely reversed this effect. Our results show that OS positively correlates with neuroinflammation and is particularly evident in brain tissue of patients with FCD IIb and TSC. In vitro, NF-κB is involved in the switch to an inflammatory state after OS. We propose that the extent of OS can predict the neuroinflammatory state of the brain. Additionally, antioxidant treatments may prevent the switch to inflammation in neurons thus targeting multiple epileptogenic processes at once.
氧化应激(OS)发生在癫痫患者的大脑中,与脑炎症同时发生,这两种现象都有助于动物模型中的癫痫发作。我们研究了氧化应激和脑炎症标志物的表达是否也同时存在于癫痫性皮质发育不良的患者切除的脑组织中:巨脑回畸形(HME)、局灶性皮质发育不良(FCD)和结节性硬化症(TSC)的皮质结节。此外,我们在神经元功能的体外模型中研究了将 OS 与炎症联系起来的分子机制。理清相互依存关系和潜在的分子机制可能为治疗不同病因耐药性癫痫患者提出新的治疗策略。免疫组织化学用于检测来自 HME、FCD IIa、IIb 和 TSC 患者的皮质组织中特定的 OS 标志物 xCT 和 iNOS 以及脑炎症标志物 TLR4、COX-2 和 NF-κB。此外,我们使用人类神经元细胞系 SH-SY5Y 研究了这些标志物的基因表达,在该细胞系中,使用 H O 诱导 OS。在 FCD IIb 或 TSC 患者的皮质中,畸形神经元和气球/巨细胞中的 OS 标志物更高。OS 标志物的表达与脑炎症标志物的表达呈正相关。在体外,100µM 的 H O 而非 50µM 的 H O 增加了 TLR4、IL-1β 和 COX-2 的表达。我们发现,只有在受到 100µM 的 H O 刺激时,NF-κB 信号才被激活,导致 TLR4 信号和 IL-1β 的上调。NF-κB 抑制剂 TPCA-1 完全逆转了这种效应。我们的结果表明,OS 与神经炎症呈正相关,在 FCD IIb 和 TSC 患者的脑组织中尤为明显。在体外,NF-κB 参与了 OS 后向炎症状态的转变。我们提出,OS 的程度可以预测大脑的神经炎症状态。此外,抗氧化治疗可能会阻止神经元向炎症状态的转变,从而同时针对多种致痫过程。
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