Establishment and validation of a bioinformatics ferroptosis gene diagnostic model for myocardial infarction and immunological analysis_Chinese Journal of Clinical Thoracic and Cardiovascular Surgery

Authors：

GONG Yufang ¹ ,  DENG Haixia ² , LU Yan ¹ , ZHOU wei ¹

1. Guigang City People's Hospital, Guigang, 537000, Guangxi, P. R. China;
2. Emergency Department, The First Affiliated Hospital of Guangxi University of Traditional Chinese Medicine, Nanning, 530022, P. R. China;

Corresponding author：

DENG Haixia, Email: denghaixia118@163.com

Keywords：

Bioinformatics; acute myocardial infarction; ferroptosis; artificial neural network; immune infiltration

DOI：

10.7507/1007-4848.202312017

Video：

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Objective To establish and validate the diagnostic model of ferroptosis genes for acute myocardial infarction (AMI) based on bioinformatics. Methods Five AMI gene expression data were obtained from Gene Expression Omnibus (GEO), namely GSE66360, GSE48060, GSE60993, GSE83500, GSE34198. Among them, GSE66360 was used as the training set to perform differential analysis, and intersection of differential genes and ferroptosis genes was taken to obtain differentially expressed ferroptosis genes in AMI. GO and KEGG enrichment analysis was performed using Metascape website. Subsequently, random forest (RF) algorithm was used to screen out key genes with high classification performance according to the Keeny coefficient score, and artificial neural network (ANN) diagnostic model of AMI ferroptosis feature gene was constructed by model group GSE83500. The area under the receiver operating characteristic curve (AUC) of 10-fold cross-validation was used to evaluate the performance and generalization ability of the model, and 3 external independent datasets were used to verify the diagnostic performance of this model. The single sample gene setenrichment analysis was used to explore the difference in immune cell infiltration between infarcted myocardium and normal myocardium after AMI. In addition, correlation analysis between immune cells and key genes was also conducted. Finally, potential drugs that would prevent and treat AMI by regulating ferroptosis were screened out from the Coremin Medical platform. Results A total of 16 differentially expressed ferroptosis genes were obtained in the training set, GO enrichment analysis showed that they mainly participated in biological functions such as cellular response to biological stimuli and chemical stress, regulation of interleukin 17, etc. KEGG enrichment analysis showed that these genes were significantly enriched in NOD-like receptor signaling pathway, programmed cell necrosis, Leishmaniasis and other pathways. Four genes with good classification performance were screened out using RF algorithm, namely EPAS1, SLC7A5, FTH1, and ZFP36. The results of 10-fold cross-validation showed that the minimum AUC value was 0.746, the maximum value was 0.906, and the average value was 0.805. The AUC of the ANN model was 0.859, and the AUC values of the three independent validation sets were 0.763 (GSE48060), 0.673 (GSE60993), 0.698 (GSE34198). Immune cell infiltration found that macrophages, mast cells and monocytes were significantly active after AMI. Correlation analysis found that there were positive correlations between 4 key genes and activated dendritic cells, eosinophils and γδT cells. A total of 20 potential western medicines were predicted which could prevent and treat AMI by regulating ferroptosis, and the predicted potential Chinese medicine was mainly heat-clearing and detoxifying and blood-activating and removing blood stasis drugs. Conclusion The identified AMI ferroptosis genes by bioinformatics method have certain diagnostic significance, which provides a reference for disease diagnosis and treatment.

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7.	Fang X, Wang H, Han D, et al. Ferroptosis as a target for protection against cardiomyopathy. Proc Natl Acad Sci U S A, 2019, 116(7): 2672-2680.
8.	Wang F, Wang Y, Ji X, et al. Effective macrosomia prediction using random forest algorithm. Int J Environ Res Public Health, 2022, 19(6): 3245.
9.	Xiao Y. Application of neural network algorithm in medical artificial intelligence product development. Comput Math Methods Med, 2022, 2022: 5413202.
10.	Liu C, Zhang X, Chai H, et al. Identification of immune cells and key genes associated with Alzheimer's Disease. Int J Med Sci, 2022, 19(1): 112-125.
11.	Zuo S, Wei M, Wang S, et al. Pan-cancer analysis of immune cell infiltration identifies a prognostic Immune-Cell Characteristic Score (ICCS) in lung adenocarcinoma. Front Immunol, 2020, 11: 1218.
12.	Tian Y, Yang J, Lan M, et al. Construction and analysis of a joint diagnosis model of random forest and artificial neural network for heart failure. Aging (Albany NY), 2020, 12(24): 26221-26235.
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15.	Li H, Ding J, Liu W, et al. Plasma exosomes from patients with acute myocardial infarction alleviate myocardial injury by inhibiting ferroptosis through miR-26b-5p/SLC7A11 axis. Life Sci, 2023, 322: 121649.
16.	Young JM, Williams DR, Thompson AAR. Thin air, thick vessels: Historical and current perspectives on hypoxic pulmonary hypertension. Front Med (Lausanne), 2019, 6: 93.
17.	Sun H, Pratt RE, Dzau VJ, et al. Neonatal and adult cardiac fibroblasts exhibit inherent differences in cardiac regenerative capacity. J Biol Chem, 2023, 299(5): 104694.
18.	Kanai Y. Amino acid transporter LAT1 (SLC7A5) as a molecular target for cancer diagnosis and therapeutics. Pharmacol Ther, 2022, 230: 107964.
19.	Li C, Chen S, Jia W, et al. Identify metabolism-related genes IDO1, ALDH2, NCOA2, SLC7A5, SLC3A2, LDHB, and HPRT1 as potential prognostic markers and correlate with immune infiltrates in head and neck squamous cell carcinoma. Front Immunol, 2022, 13: 955614.
20.	Gao X, Hu W, Qian D, et al. The mechanisms of ferroptosis under hypoxia. Cell Mol Neurobiol, 2023, 43(7): 3329-3341.
21.	Zhang R, Pan T, Xiang Y, et al. Curcumenol triggered ferroptosis in lung cancer cells via lncRNA H19/miR-19b-3p/FTH1 axis. Bioact Mater, 2021, 13: 23-36.
22.	Tian Y, Lu J, Hao X, et al. FTH1 inhibits ferroptosis through ferritinophagy in the 6-OHDA model of Parkinson's Disease. Neurotherapeutics, 2020, 17(4): 1796-1812.
23.	Ju J, Li XM, Zhao XM, et al. Circular RNA FEACR inhibits ferroptosis and alleviates myocardial ischemia/reperfusion injury by interacting with NAMPT. J Biomed Sci, 2023, 30(1): 45.
24.	Zhang Z, Guo M, Li Y, et al. RNA-binding protein ZFP36/TTP protects against ferroptosis by regulating autophagy signaling pathway in hepatic stellate cells. Autophagy, 2020, 16(8): 1482-1505.
25.	Cao Y, Huang W, Wu F, et al. ZFP36 protects lungs from intestinal I/R-induced injury and fibrosis through the CREBBP/p53/p21/Bax pathway. Cell Death Dis, 2021, 12(7): 685.
26.	Taylor GA, Carballo E, Lee DM, et al. A pathogenetic role for TNF alpha in the syndrome of cachexia, arthritis, and autoimmunity resulting from tristetraprolin (TTP) deficiency. Immunity, 1996, 4(5): 445-454.
27.	Kubota A, Frangogiannis NG. Macrophages in myocardial infarction. Am J Physiol Cell Physiol, 2022, 323(4): C1304-C1324.
28.	Feng Q, Li Q, Zhou H, et al. The role of major immune cells in myocardial infarction. Front Immunol, 2023, 13: 1084460.
29.	Farbehi N, Patrick R, Dorison A, et al. Single-cell expression profiling reveals dynamic flux of cardiac stromal, vascular and immune cells in health and injury. Elife, 2019, 8: e43882.
30.	Li J, Liang C, Yang KY, et al. Specific ablation of CD4+ T-cells promotes heart regeneration in juvenile mice. Theranostics, 2020, 10(18): 8018-8035.
31.	Guo S, Wu J, Zhou W, et al. Identification and analysis of key genes associated with acute myocardial infarction by integrated bioinformatics methods. Medicine (Baltimore), 2021, 100(15): e25553.
32.	Chen Y, Tao Y, Zhang L, et al. Diagnostic and prognostic value of biomarkers in acute myocardial infarction. Postgrad Med J, 2019, 95(1122): 210-216.
33.	Shi G, Liu G, Gao Q, et al. A random forest algorithm-based prediction model for moderate to severe acute postoperative pain after orthopedic surgery under general anesthesia. BMC Anesthesiol, 2023, 23(1): 361.

1. Salari N, Morddarvanjoghi F, Abdolmaleki A, et al. The global prevalence of myocardial infarction: A systematic review and meta-analysis. BMC Cardiovasc Disord, 2023, 23(1): 206.
2. Liu K, Chen S, Lu R. Identification of important genes related to ferroptosis and hypoxia in acute myocardial infarction based on WGCNA. Bioengineered, 2021, 12(1): 7950-7963.
3. Reed GW, Rossi JE, Cannon CP. Acute myocardial infarction. Lancet, 2017, 389(10065): 197-210.
4. Braunwald E. Unstable angina and non-ST elevation myocardial infarction. Am J Respir Crit Care Med, 2012, 185(9): 924-932.
5. Kobayashi M, Suhara T, Baba Y, et al. Pathological roles of iron in cardiovascular disease. Curr Drug Targets, 2018, 19(9): 1068-1076.
6. Wang XD, Kang S. Ferroptosis in myocardial infarction: Not a marker but a maker. Open Biol, 2021, 11(4): 200367.
7. Fang X, Wang H, Han D, et al. Ferroptosis as a target for protection against cardiomyopathy. Proc Natl Acad Sci U S A, 2019, 116(7): 2672-2680.
8. Wang F, Wang Y, Ji X, et al. Effective macrosomia prediction using random forest algorithm. Int J Environ Res Public Health, 2022, 19(6): 3245.
9. Xiao Y. Application of neural network algorithm in medical artificial intelligence product development. Comput Math Methods Med, 2022, 2022: 5413202.
10. Liu C, Zhang X, Chai H, et al. Identification of immune cells and key genes associated with Alzheimer's Disease. Int J Med Sci, 2022, 19(1): 112-125.
11. Zuo S, Wei M, Wang S, et al. Pan-cancer analysis of immune cell infiltration identifies a prognostic Immune-Cell Characteristic Score (ICCS) in lung adenocarcinoma. Front Immunol, 2020, 11: 1218.
12. Tian Y, Yang J, Lan M, et al. Construction and analysis of a joint diagnosis model of random forest and artificial neural network for heart failure. Aging (Albany NY), 2020, 12(24): 26221-26235.
13. She J, Su D, Diao R, et al. A joint model of random forest and artificial neural network for the diagnosis of endometriosis. Front Genet, 2022, 13: 848116.
14. Bai T, Li M, Liu Y, et al. Inhibition of ferroptosis alleviates atherosclerosis through attenuating lipid peroxidation and endothelial dysfunction in mouse aortic endothelial cell. Free Radic Biol Med, 2020, 160: 92-102.
15. Li H, Ding J, Liu W, et al. Plasma exosomes from patients with acute myocardial infarction alleviate myocardial injury by inhibiting ferroptosis through miR-26b-5p/SLC7A11 axis. Life Sci, 2023, 322: 121649.
16. Young JM, Williams DR, Thompson AAR. Thin air, thick vessels: Historical and current perspectives on hypoxic pulmonary hypertension. Front Med (Lausanne), 2019, 6: 93.
17. Sun H, Pratt RE, Dzau VJ, et al. Neonatal and adult cardiac fibroblasts exhibit inherent differences in cardiac regenerative capacity. J Biol Chem, 2023, 299(5): 104694.
18. Kanai Y. Amino acid transporter LAT1 (SLC7A5) as a molecular target for cancer diagnosis and therapeutics. Pharmacol Ther, 2022, 230: 107964.
19. Li C, Chen S, Jia W, et al. Identify metabolism-related genes IDO1, ALDH2, NCOA2, SLC7A5, SLC3A2, LDHB, and HPRT1 as potential prognostic markers and correlate with immune infiltrates in head and neck squamous cell carcinoma. Front Immunol, 2022, 13: 955614.
20. Gao X, Hu W, Qian D, et al. The mechanisms of ferroptosis under hypoxia. Cell Mol Neurobiol, 2023, 43(7): 3329-3341.
21. Zhang R, Pan T, Xiang Y, et al. Curcumenol triggered ferroptosis in lung cancer cells via lncRNA H19/miR-19b-3p/FTH1 axis. Bioact Mater, 2021, 13: 23-36.
22. Tian Y, Lu J, Hao X, et al. FTH1 inhibits ferroptosis through ferritinophagy in the 6-OHDA model of Parkinson's Disease. Neurotherapeutics, 2020, 17(4): 1796-1812.
23. Ju J, Li XM, Zhao XM, et al. Circular RNA FEACR inhibits ferroptosis and alleviates myocardial ischemia/reperfusion injury by interacting with NAMPT. J Biomed Sci, 2023, 30(1): 45.
24. Zhang Z, Guo M, Li Y, et al. RNA-binding protein ZFP36/TTP protects against ferroptosis by regulating autophagy signaling pathway in hepatic stellate cells. Autophagy, 2020, 16(8): 1482-1505.
25. Cao Y, Huang W, Wu F, et al. ZFP36 protects lungs from intestinal I/R-induced injury and fibrosis through the CREBBP/p53/p21/Bax pathway. Cell Death Dis, 2021, 12(7): 685.
26. Taylor GA, Carballo E, Lee DM, et al. A pathogenetic role for TNF alpha in the syndrome of cachexia, arthritis, and autoimmunity resulting from tristetraprolin (TTP) deficiency. Immunity, 1996, 4(5): 445-454.
27. Kubota A, Frangogiannis NG. Macrophages in myocardial infarction. Am J Physiol Cell Physiol, 2022, 323(4): C1304-C1324.
28. Feng Q, Li Q, Zhou H, et al. The role of major immune cells in myocardial infarction. Front Immunol, 2023, 13: 1084460.
29. Farbehi N, Patrick R, Dorison A, et al. Single-cell expression profiling reveals dynamic flux of cardiac stromal, vascular and immune cells in health and injury. Elife, 2019, 8: e43882.
30. Li J, Liang C, Yang KY, et al. Specific ablation of CD4+ T-cells promotes heart regeneration in juvenile mice. Theranostics, 2020, 10(18): 8018-8035.
31. Guo S, Wu J, Zhou W, et al. Identification and analysis of key genes associated with acute myocardial infarction by integrated bioinformatics methods. Medicine (Baltimore), 2021, 100(15): e25553.
32. Chen Y, Tao Y, Zhang L, et al. Diagnostic and prognostic value of biomarkers in acute myocardial infarction. Postgrad Med J, 2019, 95(1122): 210-216.
33. Shi G, Liu G, Gao Q, et al. A random forest algorithm-based prediction model for moderate to severe acute postoperative pain after orthopedic surgery under general anesthesia. BMC Anesthesiol, 2023, 23(1): 361.

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Latest ArticlesEstablishment and validation of a bioinformatics ferroptosis gene diagnostic model for myocardial infarction and immunological analysis

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