Identification of potential therapeutic targets for atherosclerosis by analysing the gene signature related to different immune cells and immune regulators in atheromatous plaques

Identification of potential therapeutic targets for atherosclerosis by analysing the gene signature related to different immune cells and immune regulators in atheromatous plaques

Atherosclerosis is a chronic inflammatory disease that affects multiple arteries. Numerous studies have shown the inherent immune diversity in atheromatous plaques and suggest that the dysfunction of different immune cells plays an important role in atherosclerosis. However, few comprehensive bioinf...

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Veröffentlicht in:BMC medical genomics 2021-06, Vol.14 (1), p.145-14, Article 145
Hauptverfasser: Shen, Yang, Xu, Li-Rong, Tang, Xiao, Lin, Chang-Po, Yan, Dong, Xue, Song, Qian, Rui-Zhe, Guo, Da-Qiao
Format: Artikel
Sprache:eng
Schlagworte:
Algorithms
Arteries
Arteriosclerosis
Atherosclerosis
Atherosclerosis - genetics
Atherosclerosis - immunology
Atherosclerosis - pathology
Atherosclerotic plaque
Bioinformatics
Care and treatment
Circadian clock
Circadian rhythm
Cluster analysis
Computational Biology
Correlation analysis
Datasets
Development and progression
ESTIMATE algorithm
Gene expression
Gene Expression Profiling
Gene Regulatory Networks
Gene set enrichment analysis
Genetic aspects
Health aspects
Histocompatibility antigen HLA
Humans
Immune checkpoint
Immune infiltration
Immune response
Infiltration
Inflammatory diseases
Interleukin 1
Interleukin 18
Janus kinase 2
Leukocytes
Lymphocytes T
Macrophages
Matrilysin
Monocytes
PD-1 protein
PD-L1 protein
Period 1 protein
Plaque, Atherosclerotic - genetics
Plaque, Atherosclerotic - immunology
Plaque, Atherosclerotic - pathology
Plaques
Plasma cells
Protein Interaction Maps
Regulation
Signal transduction
Stat1 protein
Therapeutic applications
Therapeutic targets
Transcriptome
Veins & arteries
γ-Interferon
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Zusammenfassung:Atherosclerosis is a chronic inflammatory disease that affects multiple arteries. Numerous studies have shown the inherent immune diversity in atheromatous plaques and suggest that the dysfunction of different immune cells plays an important role in atherosclerosis. However, few comprehensive bioinformatics analyses have investigated the potential coordinators that might orchestrate different immune cells to exacerbate atherosclerosis. Immune infiltration of 69 atheromatous plaques from different arterial beds in GSE100927 were explored by single-sample-gene-set enrichment analysis (presented as ssGSEA scores), ESTIMATE algorithm (presented as immune scores) and CIBERSORT algorithm (presented as relative fractions of 22 types of immune cells) to divide these plaques into ImmuneScoreL cluster (of low immune infiltration) and ImmuneScoreH cluster (of high immune infiltration). Subsequently, comprehensive bioinformatics analyses including differentially-expressed-genes (DEGs) analysis, protein-protein interaction networks analysis, hub genes analysis, Gene-Ontology-terms and KEGG pathway enrichment analysis, gene set enrichment analysis, analysis of expression profiles of immune-related genes, correlation analysis between DEGs and hub genes and immune cells were conducted. GSE28829 was analysed to cross-validate the results in GSE100927. Immune-related pathways, including interferon-related pathways and PD-1 signalling, were highly enriched in the ImmuneScoreH cluster. HLA-related (except for HLA-DRB6) and immune checkpoint genes (IDO1, PDCD-1, CD274(PD-L1), CD47), RORC, IFNGR1, STAT1 and JAK2 were upregulated in the ImmuneScoreH cluster, whereas FTO, CRY1, RORB, and PER1 were downregulated. Atheromatous plaques in the ImmuneScoreH cluster had higher proportions of M0 macrophages and gamma delta T cells but lower proportions of plasma cells and monocytes (p 
ISSN:1755-8794
1755-8794
DOI:10.1186/s12920-021-00991-2