神经炎症介导新生儿缺氧缺血性脑损伤向阿尔茨海默病的进展:一项生物信息学与实验研究
Neuroinflammation mediates the progression of neonate hypoxia-ischemia brain damage to Alzheimer's disease: a bioinformatics and experimental study.
作者信息
Zhang Shengjie, Zhang Ruqiu, Chen Zhaoqin, Shao Zihan, Li An, Li Fan, Huang Fang
机构信息
School of Medicine, Yunnan University, Kunming, China.
State Key Laboratory for Conservation and Utilization of Bio-resources in Yunnan, Yunnan University, Kunming, China.
出版信息
Front Aging Neurosci. 2025 Jan 13;16:1511668. doi: 10.3389/fnagi.2024.1511668. eCollection 2024.
BACKGROUND
Traumatic brain injury (TBI) can generally be divided into focal damage and diffuse damage, and neonate Hypoxia-Ischemia Brain Damage (nHIBD) is one of the causes of diffuse damage. Patients with nHIBD are at an increased risk of developing Alzheimer's disease (AD). However, the shared pathogenesis of patients affected with both neurological disorders has not been fully elucidated.
PURPOSE
We here aim to identify the shared molecular signatures between nHIBD and AD. We used an integrated analysis of the cortex gene expression data, targeting differential expression of genes related to the mechanisms of neurodegeneration and cognitive impairment following traumatic brain injury.
METHODS
The gene expression profiles of Alzheimer's disease (GSE203206) and that of Neonate Hypoxia-Ischemia Brain Damage (GSE23317) were obtained from the Gene Expression Omnibus (GEO) database. After identifying the common differentially expressed genes (DEGs) of Alzheimer's disease and neonate Hypoxia-Ischemia Brain Damage by limma package analysis, five kinds of analyses were performed on them, namely Gene Ontology (GO) and pathway enrichment analysis, protein-protein interaction network, DEG-transcription factor interactions and DEG-microRNA interactions, protein-drug interactions and protein-disease association analysis, and gene-inflammation association analysis and protein-inflammation association analysis.
RESULTS
In total, 12 common DEGs were identified including HSPB1, VIM, MVD, TUBB4A, AACS, ANXA6, DIRAS2, RPH3A, CEND1, KALM, THOP1, AREL1. We also identified 11 hub proteins, three central regulatory transcription factors, and three microRNAs encoded by the DEGs. Protein-drug interaction analysis showed that CYC1 and UQCRFS1 are associated with different drugs. Gene-disease association analysis shows Mammary Neoplasms, Neoplasm Metastasis, Schizophrenia, and Brain Ischemia diseases are the most relevant to the hub proteins we identified. Gene-inflammation association analysis shows that the hub gene AREL1 is related to inflammatory response, while the protein-inflammation association analysis shows that the hub proteins AKT1 and MAPK14 are related to inflammatory response.
CONCLUSION
This study provides new insights into the shared molecular mechanisms between AD and nHIBD. These common pathways and hub genes could potentially be used to design therapeutic interventions, reducing the likelihood of Alzheimer's disease development in survivors of neonatal Hypoxic-Ischemia brain injury.
背景
创伤性脑损伤(TBI)一般可分为局灶性损伤和弥漫性损伤,新生儿缺氧缺血性脑损伤(nHIBD)是弥漫性损伤的原因之一。nHIBD患者患阿尔茨海默病(AD)的风险增加。然而,这两种神经系统疾病患者的共同发病机制尚未完全阐明。
目的
我们旨在确定nHIBD和AD之间的共同分子特征。我们对皮质基因表达数据进行了综合分析,针对创伤性脑损伤后与神经退行性变和认知障碍机制相关的基因差异表达。
方法
从基因表达综合数据库(GEO)中获取阿尔茨海默病(GSE203206)和新生儿缺氧缺血性脑损伤(GSE23317)的基因表达谱。通过limma软件包分析确定阿尔茨海默病和新生儿缺氧缺血性脑损伤的共同差异表达基因(DEGs)后,对其进行了五种分析,即基因本体论(GO)和通路富集分析、蛋白质-蛋白质相互作用网络、DEG-转录因子相互作用和DEG-微小RNA相互作用、蛋白质-药物相互作用和蛋白质-疾病关联分析,以及基因-炎症关联分析和蛋白质-炎症关联分析。
结果
共鉴定出12个共同的DEGs,包括HSPB1、VIM、MVD、TUBB4A、AACS、ANXA6、DIRAS2、RPH3A、CEND1、KALM、THOP1、AREL1。我们还鉴定出11个枢纽蛋白、3个核心调控转录因子和3个由DEGs编码的微小RNA。蛋白质-药物相互作用分析表明CYC1和UQCRFS1与不同药物相关。基因-疾病关联分析表明乳腺肿瘤、肿瘤转移、精神分裂症和脑缺血疾病与我们鉴定的枢纽蛋白最相关。基因-炎症关联分析表明枢纽基因AREL1与炎症反应相关,而蛋白质-炎症关联分析表明枢纽蛋白AKT1和MAPK14与炎症反应相关。
结论
本研究为AD和nHIBD之间的共同分子机制提供了新的见解。这些共同途径和枢纽基因可能用于设计治疗干预措施,降低新生儿缺氧缺血性脑损伤幸存者患阿尔茨海默病的可能性。
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