The Interplay Between Epilepsy and Parkinson's Disease: Gene Expression Profiling and Functional Analysis.

IF 2.4 4区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Molecular Biotechnology Pub Date : 2025-03-01 Epub Date: 2024-03-07 DOI:10.1007/s12033-024-01103-y

Xiaolong Wu, Kailiang Wang, Jingjing Wang, Penghu Wei, Huaqiang Zhang, Yanfeng Yang, Yinchun Huang, Yihe Wang, Wenli Shi, Yongzhi Shan, Guoguang Zhao

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Abstract

The results of many epidemiological studies suggest a bidirectional causality may exist between epilepsy and Parkinson's disease (PD). However, the underlying molecular landscape linking these two diseases remains largely unknown. This study aimed to explore this possible bidirectional causality by identifying differentially expressed genes (DEGs) in each disease as well as their intersection based on two respective disease-related datasets. We performed enrichment analyses and explored immune cell infiltration based on an intersection of the DEGs. Identifying a protein-protein interaction (PPI) network between epilepsy and PD, and this network was visualised using Cytoscape software to screen key modules and hub genes. Finally, exploring the diagnostic values of the identified hub genes. NetworkAnalyst 3.0 and Cytoscape software were also used to construct and visualise the transcription factor-micro-RNA regulatory and co-regulatory networks, the gene-microRNA interaction network, as well as gene-disease association. Based on the enrichment results, the intersection of the DEGs mainly revealed enrichment in immunity-, phosphorylation-, metabolism-, and inflammation-related pathways. The boxplots revealed similar trends in infiltration of many immune cells in epilepsy and Parkinson's disease, with greater infiltration in patients than in controls. A complex PPI network comprising 186 nodes and 512 edges were constructed. According to node connection degree, top 15 hub genes were considered the kernel targets of epilepsy and PD. The area under curve values of hub gene expression profiles confirmed their excellent diagnostic values. This study is the first to analyse the molecular landscape underlying the epidemiological link between epilepsy and Parkinson's disease. The two diseases are closely linked through immunity-, inflammation-, and metabolism-related pathways. This information was of great help in understanding the pathogenesis, diagnosis, and treatment of the diseases. The present results may provide guidance for further in-depth analysis about molecular mechanisms of epilepsy and PD and novel potential targets.

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癫痫与帕金森病之间的相互作用：基因表达谱分析和功能分析

许多流行病学研究结果表明，癫痫和帕金森病（PD）之间可能存在双向因果关系。然而，连接这两种疾病的潜在分子图谱在很大程度上仍不为人所知。本研究旨在基于两种疾病相关的数据集，通过识别每种疾病中的差异表达基因（DEGs）及其交叉点，探索这种可能的双向因果关系。我们根据 DEGs 的交叉点进行了富集分析并探索了免疫细胞浸润。确定了癫痫和帕金森病之间的蛋白-蛋白相互作用（PPI）网络，并使用Cytoscape软件将该网络可视化，以筛选关键模块和枢纽基因。最后，探索已确定的中心基因的诊断价值。NetworkAnalyst 3.0和Cytoscape软件还被用于构建和可视化转录因子-微RNA调控和共调控网络、基因-微RNA相互作用网络以及基因-疾病关联。根据富集结果，DEGs 的交叉点主要富集在免疫、磷酸化、代谢和炎症相关通路中。方框图显示，癫痫和帕金森病中许多免疫细胞的浸润趋势相似，患者的浸润程度高于对照组。研究人员构建了一个由 186 个节点和 512 条边组成的复杂 PPI 网络。根据节点连接度，前15个中枢基因被认为是癫痫和帕金森病的内核靶点。中枢基因表达谱的曲线下面积值证实了其卓越的诊断价值。这项研究首次分析了癫痫与帕金森病之间流行病学联系的分子图谱。这两种疾病通过免疫、炎症和新陈代谢相关通路密切相关。这些信息对了解疾病的发病机制、诊断和治疗有很大帮助。本研究结果可为进一步深入分析癫痫和帕金森病的分子机制以及新的潜在靶点提供指导。

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来源期刊

Molecular Biotechnology 医学-生化与分子生物学

CiteScore

4.10

自引率

3.80%

发文量

165

审稿时长

6 months

期刊介绍： Molecular Biotechnology publishes original research papers on the application of molecular biology to both basic and applied research in the field of biotechnology. Particular areas of interest include the following: stability and expression of cloned gene products, cell transformation, gene cloning systems and the production of recombinant proteins, protein purification and analysis, transgenic species, developmental biology, mutation analysis, the applications of DNA fingerprinting, RNA interference, and PCR technology, microarray technology, proteomics, mass spectrometry, bioinformatics, plant molecular biology, microbial genetics, gene probes and the diagnosis of disease, pharmaceutical and health care products, therapeutic agents, vaccines, gene targeting, gene therapy, stem cell technology and tissue engineering, antisense technology, protein engineering and enzyme technology, monoclonal antibodies, glycobiology and glycomics, and agricultural biotechnology.