Coronavirus disease 2019-related myocarditis genes contribute to ECMO prognosis.

Publication date: Jul 19, 2024

Acute myocardial injury, cytokine storms, hypoxemia and pathogen-mediated damage were the major causes responsible for mortality induced by coronavirus disease 2019 (COVID-19)-related myocarditis. These need ECMO treatment. We investigated differentially expressed genes (DEGs) in patients with COVID-19-related myocarditis and ECMO prognosis. GSE150392 and GSE93101 were analyzed to identify DEGs. A Venn diagram was used to obtain the same transcripts between myocarditis-related and ECMO-related DEGs. Enrichment pathway analysis was performed and hub genes were identified. Pivotal miRNAs, transcription factors, and chemicals with the screened gene interactions were identified. The GSE167028 dataset and single-cell sequencing data were used to validate the screened genes. Using a Venn diagram, 229 overlapping DEGs were identified between myocarditis-related and ECMO-related DEGs, which were mainly involved in T cell activation, contractile actin filament bundle, actomyosin, cyclic nucleotide phosphodiesterase activity, and cytokine-cytokine receptor interaction. 15 hub genes and 15 neighboring DEGs were screened, which were mainly involved in the positive regulation of T cell activation, integrin complex, integrin binding, the PI3K-Akt signaling pathway, and the TNF signaling pathway. Data in GSE167028 and single-cell sequencing data were used to validate the screened genes, and this demonstrated that the screened genes CCL2, APOE, ITGB8, LAMC2, COL6A3 and TNC were mainly expressed in fibroblast cells; IL6, ITGA1, PTK2, ITGB5, IL15, LAMA4, CAV1, SNCA, BDNF, ACTA2, CD70, MYL9, DPP4, ENO2 and VEGFC were expressed in cardiomyocytes; IL6, PTK2, ITGB5, IL15, APOE, JUN, SNCA, CD83, DPP4 and ENO2 were expressed in macrophages; and IL6, ITGA1, PTK2, ITGB5, IL15, VCAM1, LAMA4, CAV1, ACTA2, MYL9, CD83, DPP4, ENO2, VEGFC and IL32 were expressed in vascular endothelial cells. The screened hub genes, IL6, ITGA1, PTK2, ITGB3, ITGB5, CCL2, IL15, VCAM1, GZMB, APOE, ITGB8, LAMA4, LAMC2, COL6A3 and TNFRSF9, were validated using GEO dataset and single-cell sequencing data, which may be therapeutic targets patients with myocarditis to prevent MI progression and adverse cardiovascular events.

Open Access PDF

Concepts Keywords
Cardiomyocytes COVID-19
Coronavirus Databases, Genetic
Gse150392 ECMO
Myocarditis Extracorporeal Membrane Oxygenation
Gene Expression Profiling
Gene Regulatory Networks
Humans
Integrin
Myocarditis
Myocarditis
Pathway enrichment analysis
Prognosis
SARS-CoV-2
Single-cell sequencing
TNF family
Transcriptome

Semantics

Type Source Name
disease MESH Coronavirus disease 2019
disease MESH myocarditis
disease MESH cytokine storms
disease IDO pathogen
disease MESH causes
drug DRUGBANK Huperzine B
disease VO gene
disease IDO cell
pathway KEGG Cytokine-cytokine receptor interaction
pathway KEGG PI3K-Akt signaling pathway
pathway KEGG TNF signaling pathway
drug DRUGBANK Coenzyme M
disease MESH Emergency
disease MESH pneumonia
disease MESH complications
disease MESH infection
disease MESH morbidity
disease MESH acute respiratory distress syndrome
disease MESH septic shock
disease MESH multiple organ failure
disease VO organ
disease MESH inflammation
drug DRUGBANK MCC
disease IDO homo sapiens
drug DRUGBANK NADH
pathway KEGG Oxidative phosphorylation
disease VO leukocyte
pathway KEGG Focal adhesion
disease IDO biological process
drug DRUGBANK Trestolone
drug DRUGBANK L-Tyrosine
drug DRUGBANK Angiotensin II
disease VO population
disease VO URE
disease VO macrophage
disease IDO symptom
disease IDO immunosuppression
disease MESH fibrosis
disease MESH atherogenesis
disease VO vaccination
drug DRUGBANK Esomeprazole
disease MESH weaning
disease VO time
drug DRUGBANK (S)-Des-Me-Ampa
drug DRUGBANK Carboxyamidotriazole
disease MESH severe acute respiratory syndrome
disease MESH metabolic diseases
disease MESH respiratory failure
disease MESH syndrome
disease VO organization
disease MESH cardiomyopathy
drug DRUGBANK Linagliptin
drug DRUGBANK Xanthine
drug DRUGBANK Inosine
drug DRUGBANK Guanosine
disease MESH cardiovascular diseases
disease MESH Pericarditis
disease MESH Pericardial effusion
disease MESH cardiac tamponade
disease VO vaccine
disease VO report

Original Article

(Visited 2 times, 1 visits today)