MicroRNAs Expression Profile in Young Patients with Acute Myocardial Infarction

Nurul Ashikin Muhammad Musa, N. Abdullah, Norlelawati A. Talib, Azarisman Shah Mohd. Shah, Aszrin Abdullah, A. M. Mohd. Shah
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Abstract

Introduction: Acute myocardial infarction (AMI) is a severe coronary heart disease.   Targeted miRNAs studies implicated two main pathways in the regulation of AMI namely pro-apoptosis (miR-29b and miR-194-5p on PTEN) and pro-necroptosis (miR-325 & miR-105 on RIPK3 ) pathways. This study aims to profile the miRNAs in Healthy Controls, Young AMI, and Mature AMI patients with matching criteria. MATERIALS AND Methods: Total RNA was extracted from plasma and the miRNA expression profiling using small RNA was done on the BGISEQ500 SE5 sequencing platform with BGI sequencing libraries.  The sequence data were analysed using Gene Ontology (GO) to determine the function of the differently expressed genes, while Kyoto Encyclopaedia of Genes and Genomes (KEGG) enrichment analyses were applied to identify the biological pathways in Young AMI against Mature AMI. Results: Of 1497 differentially expressed miRNAs, 1090 miRNAs were upregulated, and 407 miRNAs were downregulated in Young AMI against Mature AMI.  The top 10 upregulated miRNAs were miR-552, miR-4446-3p, miR-432-5p, miR-548j-5p, miR-219, miR-982, miR-181a-2-3p, miR-654-5p, miR-58 and miR-548k; while the top 10 downregulated were miR-16-5p, miR-1064, miR-431-5p, miR-790 miR-1177, miR-201, miR-105, miR-518, miR-419 and miR-1103.  There were 9 novel miRNAs discovered in this study; miR-58, miR-982, miR-548k, miR-1064, miR-790, miR-1177, miR-201, miR-419, and miR-1103.  The target genes of differentially expressed miRNAs that were mapped to the signal transduction pathway in KEGG indicated that 346 classes were enriched. Conclusion: Our miRNA profiling revealed differentially expressed miRNAs including 9 novel miRNAs in Young and Mature AMI that require further evaluations for their roles in AMI.   
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年轻急性心肌梗死患者的MicroRNAs表达谱
简介:急性心肌梗死(AMI)是一种严重的冠心病。靶向mirna研究表明AMI的调控有两种主要途径,即促凋亡(PTEN上的miR-29b和miR-194-5p)和促坏死(RIPK3上的miR-325和miR-105)途径。本研究旨在分析符合标准的健康对照、年轻AMI和成熟AMI患者的mirna。材料与方法:从血浆中提取总RNA,利用小RNA在BGISEQ500 SE5测序平台上与华大基因测序文库进行miRNA表达谱分析。利用基因本体(GO)分析序列数据,确定不同表达基因的功能;利用京都基因与基因组百科全书(KEGG)富集分析,确定年轻AMI与成熟AMI的生物学途径。结果:1497个差异表达的mirna中,1090个mirna上调,407个mirna下调。上调前10位的mirna分别是miR-552、miR-4446-3p、miR-432-5p、miR-548j-5p、miR-219、miR-982、miR-181a-2-3p、miR-654-5p、miR-58和miR-548k;下调前10位的分别是miR-16-5p、miR-1064、miR-431-5p、miR-790、miR-1177、miR-201、miR-105、miR-518、miR-419和miR-1103。本研究共发现9个新的mirna;miR-58、miR-982、miR-548k、miR-1064、miR-790、miR-1177、miR-201、miR-419和miR-1103。在KEGG中定位到信号转导通路的差异表达mirna靶基因显示,346个类被富集。结论:我们的miRNA分析揭示了在年轻和成熟AMI中表达差异的miRNA,包括9个新的miRNA,需要进一步评估它们在AMI中的作用。
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