Identifying key genes, pathways and screening therapeutic agents for manganese-induced Alzheimer disease using bioinformatics analysis

JunJun Ling; Shengyou Yang; Yi Huang; Dongfeng Wei; Weidong Cheng

doi:10.1097/MD.0000000000010775

Identifying key genes, pathways and screening therapeutic agents for manganese-induced Alzheimer disease using bioinformatics analysis

Medicine (Baltimore). 2018 Jun;97(22):e10775. doi: 10.1097/MD.0000000000010775.

Authors

JunJun Ling¹, Shengyou Yang, Yi Huang, Dongfeng Wei, Weidong Cheng

Affiliation

¹ Department of Traditional Chinese Medicine, Southern Medical University, Guangzhou Institute of Cancer, Xinqiao Hospital, Third Military Medical University, Chongqing Department of Medical Image, Guizhou Provincial People's Hospital Department of Internal Medicine, Affiliated Hospital of Guizhou Medical University, Guiyang Institute of Basic Research in Clinical Medicine, China Academy of Chinese Medical Sciences, Beijing, China.

Abstract

Alzheimer disease (AD) is a progressive neurodegenerative disease, the etiology of which remains largely unknown. Accumulating evidence indicates that elevated manganese (Mn) in brain exerts toxic effects on neurons and contributes to AD development. Thus, we aimed to explore the gene and pathway variations through analysis of high through-put data in this process.To screen the differentially expressed genes (DEGs) that may play critical roles in Mn-induced AD, public microarray data regarding Mn-treated neurocytes versus controls (GSE70845), and AD versus controls (GSE48350), were downloaded and the DEGs were screened out, respectively. The intersection of the DEGs of each datasets was obtained by using Venn analysis. Then, gene ontology (GO) function analysis and KEGG pathway analysis were carried out. For screening hub genes, protein-protein interaction network was constructed. At last, DEGs were analyzed in Connectivity Map (CMAP) for identification of small molecules that overcome Mn-induced neurotoxicity or AD development.The intersection of the DEGs obtained 140 upregulated and 267 downregulated genes. The top 5 items of biological processes of GO analysis were taxis, chemotaxis, cell-cell signaling, regulation of cellular physiological process, and response to wounding. The top 5 items of KEGG pathway analysis were cytokine-cytokine receptor interaction, apoptosis, oxidative phosphorylation, Toll-like receptor signaling pathway, and insulin signaling pathway. Afterwards, several hub genes such as INSR, VEGFA, PRKACB, DLG4, and BCL2 that might play key roles in Mn-induced AD were further screened out. Interestingly, tyrphostin AG-825, an inhibitor of tyrosine phosphorylation, was predicted to be a potential agent for overcoming Mn-induced neurotoxicity or AD development.The present study provided a novel insight into the molecular mechanisms of Mn-induced neurotoxicity or AD development and screened out several small molecular candidates that might be critical for Mn neurotoxicity prevention and Mn-induced AD treatment.

MeSH terms

Alzheimer Disease / chemically induced*
Alzheimer Disease / genetics*
Benzothiazoles / metabolism
Computational Biology / methods*
Gene Expression Profiling / methods
Gene Ontology
High-Throughput Screening Assays / methods
Humans
Manganese / metabolism
Manganese / toxicity*
Manganese Poisoning / metabolism
Manganese Poisoning / prevention & control
Phosphorylation / genetics
Protein Interaction Maps / genetics
Signal Transduction / genetics
Tyrphostins / metabolism
Up-Regulation / genetics

Substances

Benzothiazoles
Tyrphostins
tyrphostin AG825
Manganese