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一项计算机模拟分析揭示了中风后人类大脑中神经保护基因的持续上调。

An In Silico Analysis Reveals Sustained Upregulation of Neuroprotective Genes in the Post-Stroke Human Brain.

作者信息

Betto Federica, Chiricosta Luigi, Mazzon Emanuela

机构信息

IRCCS Centro Neurolesi "Bonino-Pulejo", Via Provinciale Palermo, Contrada Casazza, 98124 Messina, Italy.

出版信息

Brain Sci. 2023 Jun 23;13(7):986. doi: 10.3390/brainsci13070986.

Abstract

Ischemic stroke is a cerebrovascular disease caused by an interruption of blood flow to the brain, thus determining a lack of oxygen and nutrient supply. The ischemic event leads to the activation of several molecular signaling pathways involved in inflammation and the production of reactive oxygen species, causing irreversible neuronal damage. Several studies have focused on the acute phase of ischemic stroke. It is not clear if this traumatic event can influence some of the molecular processes in the affected area even years after the clinical event. In our study, we performed an in silico analysis using freely available raw data with the purpose of evaluating the transcriptomic state of post-mortem brain tissue. The samples were taken from non-fatal ischemic stroke patients, meaning that they suffered an ischemic stroke and lived for a period of about 2 years after the event. These samples were compared with healthy controls. The aim was to evaluate possible recovery processes useful to mitigating neuronal damage and the detrimental consequences of stroke. Our results highlighted differentially expressed genes codifying for proteins along with long non-coding genes with anti-inflammatory and anti-oxidant functions. This suggests that even after an amount of time from the ischemic insult, different neuroprotective mechanisms are activated to ameliorate brain conditions and repair post-stroke neuronal injury.

摘要

缺血性中风是一种由大脑血流中断引起的脑血管疾病,从而导致氧气和营养供应不足。缺血事件会导致参与炎症和活性氧生成的多种分子信号通路被激活,从而造成不可逆的神经元损伤。多项研究聚焦于缺血性中风的急性期。目前尚不清楚这种创伤性事件是否会在临床事件发生数年之后仍影响受影响区域的某些分子过程。在我们的研究中,我们使用公开可用的原始数据进行了一项计算机分析,目的是评估死后脑组织的转录组状态。样本取自非致命性缺血性中风患者,也就是说他们经历了缺血性中风,且在事件发生后存活了约2年时间。这些样本与健康对照进行了比较。目的是评估有助于减轻神经元损伤和中风有害后果的可能的恢复过程。我们的结果突出显示了编码蛋白质的差异表达基因以及具有抗炎和抗氧化功能的长链非编码基因。这表明即使在缺血性损伤后的一段时间,不同的神经保护机制也会被激活,以改善脑部状况并修复中风后的神经元损伤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81f7/10377198/3883cdef6733/brainsci-13-00986-g001.jpg

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