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Identification of hub genes and potential ceRNA networks of diabetic cardiomyopathy

Jun Hou, Wan Yi Liang, Shiqiang Xiong, Pan Long, Tian Yue, Xudong Wen, Tianchen Wang, Haoyu Deng

2023Scientific Reports12 citationsDOIOpen Access PDF

Abstract

Diabetic cardiomyopathy (DCM), a common complication of diabetes, is defined as ventricular dysfunction in the absence of underlying heart disease. Noncoding RNAs (ncRNAs), including long noncoding RNAs (lncRNAs) and microRNAs (miRNAs), play a crucial role in the development of DCM. Weighted Gene Co-Expression Network Analysis (WGCNA) was used to identify key modules in DCM-related pathways. DCM-related miRNA-mRNA network and DCM-related ceRNA network were constructed by miRNA-seq to identify hub genes in these modules. We identified five hub genes that are associated with the onset of DCM, including Troponin C1 (Tnnc1), Phospholamban (Pln), Fatty acid binding proteins 3 (Fabp3), Popeye domain containing 2 (Popdc2), and Tripartite Motif-containing Protein 63 (Trim63). miRNAs that target the hub genes were mainly involved in TGF-β and Wnt signaling pathways. GO BP enrichment analysis found these miRNAs were involved in the signaling of TGF-β and glucose homeostasis. Q-PCR results found the gene expressions of Pln, Fabp3, Trim63, Tnnc1, and Popdc2 were significantly increased in DCM. Our study identified five hub genes (Tnnc1, Pln, Fabp3, Popdc2, Trim63) whose associated ceRNA networks are responsible for the onset of DCM.

Topics & Concepts

microRNABiologyGeneCompeting endogenous RNAComputational biologyWnt signaling pathwayDiabetic cardiomyopathyGeneticsBioinformaticsCardiomyopathyDownregulation and upregulationLong non-coding RNAMedicineInternal medicineHeart failureCancer-related molecular mechanisms researchRNA modifications and cancerCircular RNAs in diseases
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