Expression changes and clinical significance of miR⁃5196⁃5p and miR⁃652⁃5p in dilated cardiomyopathy patients
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摘要:
目的:通过miRNA Array芯片技术,了解扩张型心肌病(dilated cardiomyopathy,DCM)患者血浆miRNA表达谱的差异,探索这种差异与左室舒张末内径(left ventricular end-diastolic dimension,LVEDd)、左室射血分数(left ventricular ejection fraction,LVEF)及N末端脑钠肽前体(N-terminal of the prohormone brain natriuretic peptide,NT-proBNP)等心衰指标的关系,并预测其作用靶基因。方法:入选南京胸科医院心脏科收住的8例明确诊断的DCM患者,抽提血浆总RNA,采用Agilent Human miRNAs Array(V19.0)芯片技术,与4例健康对照进行表达谱的差异筛选,对改变最明显的miRNA进行30例患者的进一步验证。检测两组受检者生化指标、NT-proBNP,测量LVEDd、LVEF,并进行变量间的相关分析。TargetScan和miRBD数据库预测靶基因。结果:与对照组相比,病例组中共发现36个有意义的miRNAs表达差异,其中25个上调的miRNA中,miR-5196-5p上调最明显,下调的miRNA中,miR-652-5p下调最明显。该结果在后续30例DCM患者的验证中也得到证实。Pearson线性相关分析显示,miR-5196-5p上调水平与LVEDd呈正相关,miR-652-5p水平与LVEDd、NT-proBNP呈负相关,与LVEF呈正相关。靶基因分别预测到DCM相关基因VCL、RBM20等。结论:DCM患者血浆中miR-5196-5p表达明显上调,miR-652-5p表达下调,并与左室功能、心室重构相关。进一步研究有可能揭示miR-5196-5p、miR-652-5p在心衰致病中的机制,并有可能成为评估疾病疗效及预后的新指标或潜在治疗靶点。
Abstract:
Objective:The study aimed to investigate differentially expressed microRNAs(miRNAs)and their association with left ventricular end-diastolic dimension(LVEDd),left ventricular ejection fraction(LVEF),N-terminal of the prohormone brain natriuretic peptide(NT-proBNP)in human dilated cardiomyopathy(DCM)by miRNAs array,and to predict their target gene. Methods:The expression levels of plasma miRNAs of 8 DCM patients and 4 healthy controls were detected by using the Agilent human miRNAs array(V19.0),followed by real-time RT-PCR analysis to validate the expression changes of miRNAs. NT-proBNP,LVEDd and LVEF were measured and analyzed using Pearson linear correlation analysis. The prediction analysis for microarrays(PAM)method was used to identify the differentially expressed miRNAs. Results:Thirty-six differentially expressed miRNAs were identified. There were 25 upregulated and 11 downregulated human miRNAs,of which miR-5196-5p and miR-652-5p were the most significant. Pearson linear correlation analysis showed that miR-5196-5p level was positively correlated with LVEDd,whereas miR-652-5p was positively correlated with LVEF values and negatively correlated with NT-proBNP and LVEDd. Moreover,correlative genes such as VCL and RBM20 related with DCM were predicted. Conclusion:The screened differentially expressed miRNAs may be involved in the development of DCM. Specific miRNAs,such as miR-5196-5p and miR-652-5p,may be considered as new targets for the diagnosis and treatment of human DCM.
