2025年4月2日 周三
Home > Archive>Volume 33, Issue 2, 2025 >135-143. DOI:10. 20039/ j. cnki. 1007-3949. 2025. 02. 006
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Correlation between N6-methyladenosine and ferroptosis in acute myocardial infarction
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1.Department of Cardiology, Urumqi, Xinjiang 830001, China;2.Catheter Laboratory, the Fifth Affiliated Hospital of Xinjiang Medical University, Urumqi, Xinjiang 830001, China)

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R5

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    Abstract:

    Aim To analyze the correlation between N6-methyladenosine (m6A) and ferroptosis in acute myocardial infarction (AMI). Methods Two microarray datasets GSE34198 and GSE59867 was explored from GEO database. Both AMI and control samples were analyzed for differentially expressed genes. GO, KEGG, and GSVA analysis of the screened differential genes was performed using R. Machine learning was used to screen ferroptosis associated genes for DRA, GBM, LASSO and randomForest characteristic genes. The expression data of the core ferroptosis gene and m6A-related genes were analyzed by Pearson correlation analysis, and the m6A modified genes and ferroptosis associated genes with strong correlation were screened. Finally, 10 cases of AMI and 10 control whole blood samples from the Fifth Affiliated Hospital of Xinjiang Medical University were collected, and the expression of related genes was verified by RT-qPCR and Western blot. Results 431 common differentially expressed genes were extracted from two datasets, GO and KEGG analysis showed that these genes were mainly enriched in TNF signaling pathway, FoxO signaling pathway and B cell receptor signaling pathway. The enrichment pathways of differentially expressed genes by GSVA were cuproptosis, netotic cell death, entotic cell death, alkaliptosis and ferroptosis. The characteristic genes of ferroptosis associated genes were screened by machine learning, and 19 core ferroptosis associated genes were screened from them. The expression data of ferroptosis associated genes and m6A-related genes were analyzed by Pearson correlation analysis. LRPPRC-IREB2, LRPPRC-ATG5, YTHDC2-IREB2, HNRNPA2B1-IREB2 and YTHDC2-ATG5 were the most correlated top five genes. The results of RT-qPCR and Western blot showed that the gene expression levels of LRPPRC, YTHDC2, HNRNPA2B1, IREB2 and ATG5 were significantly lower than those of the control group (P<0.001), which was consistent with the gene expression in the database. Conclusion m6A methylation is associated with ferroptosis in AMI. By regulating m6A methylation-related genes, ferroptosis in AMI can be regulated. It provides a new idea for the further study of the pathogenesis of the disease.

    Reference
    [1] RALAPANAWA U, SIVAKANESAN R.Epidemiology and the magnitude of coronary artery disease and acute coronary syndrome:a narrative review.J Epidemiol Glob Health, 1,1(2):169-177.
    [2] WANG J, LI L, MA N, et al.Clinical investigation of acute myocardial infarction according to age subsets.Exp Ther Med, 0,0(5):120.
    [3] LI W, FENG G, GAUTHIER J M, et al.Ferroptotic cell death and TLR4/Trif signaling initiate neutrophil recruitment after heart transplantation.J Clin Invest, 9,9(6):2293-2304.
    [4] ZHOU Y, ZHOU H, HUA L, et al.Verification of ferroptosis and pyroptosis and identification of PTGS2 as the hub gene in human coronary artery atherosclerosis.Free Radic Biol Med, 1,1:55-68.
    [5] 王丽雯, 刘惠美, 李兰芳, 等.铁死亡与动脉粥样硬化.中国动脉硬化杂志, 4,2(2):155-163.WANG L W, LIU H M, LI L F, et al.Ferroptosis and atherosclerosis.Chin J Arterioscler, 4,2(2):155-163.
    [6] 郝艺芳, 李婷, 牛枫楠, 等.铁死亡在心肌缺血再灌注损伤中的作用.中国动脉硬化杂志, 4,2(12):1097-1104.HAO Y F, LI T, NIU F N, et al.Role of ferroptosis in myocardial ischemia-reperfusion injury.Chin J Arterioscler, 4,2(12):1097-1104.
    [7] LAN Q, LIU P Y, HAASE J, et al.The critical role of RNA m6A methylation in cancer.Cancer Res, 9,9(7):1285-1292.
    [8] LIANG C, WANG S, ZHANG M, et al.Diagnosis, clustering, and immune cell infiltration analysis of m6A-related genes in patients with acute myocardial infarction:a bioinformatics analysis.J Thorac Dis, 2,4(5):1607-1619.
    [9] LIU L, LI H, HU D, et al.Insights into N6-methyladenosine and programmed cell death in cancer.Mol Cancer, 2,1(1):32.
    [10] THYGESEN K, ALPERT J S, JAFFE A S, et al.Fourth universal definition of myocardial infarction (2018).J Am Coll Cardiol, 8,2(18):2231-2264.
    [11] BROWN A K, WEBB A E.Regulation of FOXO factors in mammalian cells.Curr Top Dev Biol, 8,7:165-192.
    [12] TANG D, KANG R, BERGHE T V, et al.The molecular machinery of regulated cell death.Cell Res, 9,9(5):347-364.
    [13] CHAO Y, LI H B, ZHOU J.Multiple functions of RNA methylation in T cells:a review.Front Immunol, 1,2:627455.
    [14] BABA Y, HIGA J K, SHIMADA B K, et al.Protective effects of the mechanistic target of rapamycin against excess iron and ferroptosis in cardiomyocytes.Am J Physiol Heart Circ Physiol, 8,4(3):H659-H668.
    [15] WU J, CAI H, LEI Z, et al.Expression pattern and diagnostic value of ferroptosis-related genes in acute myocardial infarction.Front Cardiovasc Med, 2,9:993592.
    [16] HU S, SECHI M, SINGH P K, et al.A novel redox modulator induces a GPX4-mediated cell death that is dependent on iron and reactive oxygen species.J Med Chem, 0,3(17):9838-9855.
    [17] ZHU S, BAI L, PAN Y, et al.Integrative analysis of N6-methyladenosine RNA modifications related genes and their influences on immunoreaction or fibrosis in myocardial infarction.Int J Med Sci, 4,1(2):219-233.
    [18] MA L, ZHANG X, YU K, et al.Targeting SLC3A2 subunit of system XC- is essential for m6A reader YTHDC2 to be an endogenous ferroptosis inducer in lung adenocarcinoma.Free Radic Biol Med, 1,8:25-43.
    [19] WANG X, WU Y, GUO R, et al.Comprehensive analysis of N6-methyladenosine RNA methylation regulators in the diagnosis and subtype classification of acute myocardial infarction.J Immunol Res, 2,2:5173761.
    [20] JIANG J, ZHU J, QIU P, et al.HNRNPA2B1-mediated m6A modification of FOXM1 promotes drug resistance and inhibits ferroptosis in endometrial cancer via regulation of LCN2.Funct Integr Genomics, 3,4(1):3.
    [21] ZHU T, XIAO Z, YUAN H, et al.ACO1 and IREB2 downregulation confer poor prognosis and correlate with autophagy-related ferroptosis and immune infiltration in KIRC.Front Oncol, 2,2:929838.
    [22] XIA H, WU Y, ZHAO J, et al.N6-methyladenosine-modified circSAV1 triggers ferroptosis in COPD through recruiting YTHDF1 to facilitate the translation of IREB2.Cell Death Differ, 3,0(5):1293-1304.
    [23] HOU W, XIE Y, SONG X, et al.Autophagy promotes ferroptosis by degradation of ferritin.Autophagy, 6,2(8):1425-1428.
    [24] ZHANG Y, HE X, LI J, et al.Functional genetic variant in ATG5 gene promoter in acute myocardial infarction.Cardiol Res Pract, 0,0:9898301.
    [25] LI Y, GUO M, QIU Y, et al.Autophagy activation is required for N6-methyladenosine modification to regulate ferroptosis in hepatocellular carcinoma.Redox Biol, 4,9:102971.
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ZHANG Tingting, AN Lijuan, AZIGULI·Gulamujiang, ZAIMIRAN·Nuerta, ZHANG Yaling, LIU Gang, LUO Mei. Correlation between N6-methyladenosine and ferroptosis in acute myocardial infarction[J]. Editorial Office of Chinese Journal of Arteriosclerosis,2025,33(2):135-143.

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History
  • Received:May 17,2024
  • Revised:September 07,2024
  • Online: March 05,2025
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