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miRNAs as biomarkers for diagnosis of heart failure: A systematic review and meta-analysis

机译:miRNA作为生物标志物,用于诊断心力衰竭:系统评价和荟萃分析

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Background: With the rapid development of molecular biology, the kind of mircoRNA (miRNA) has been introduced into emerging role both in cardiac development and pathological procedure. Thus, we conduct this meta-analysis to find out the role of circulating miRNA as a biomarker in detecting heart failure. Methods: We searched PubMed, EMBASE, the Cochrane Central Register of Controlled Trials, and World Health Organization clinical trials registry center to identify relevant studies up to August 2016. We performed meta-analysis in a fixed/random-effect model using Meta-disc 1.4. We used STATA 14.0 to estimate the publication bias and meta-regression. Besides, we took use of SPSS 17.0 to evaluate variance between several groups. Information on true positive, false positive, false negative, and true negative, as well as the quality of research was extracted. Results: We use results from 10 articles to analyze the pooled accuracy. The overall performance of total mixed miRNAs (TmiRs) detection was: pooled sensitivity, 0.74 (95% confidence interval [CI], 0.72 to 0.75); pooled specificity, 0.69 (95%CI, 0.67 to 0.71); and area under the summary receiver operating characteristic curves value (SROC), 0.7991. The miRNA-423-5p (miR-423-5p) detection was: pooled sensitivity, 0.81 (95%CI, 0.76 to 0.85); pooled specificity, 0.67 (95%CI, 0.61 to 0.73); and SROC, 0.8600. However, taken the same patients population, we extracted the data of BNP for detecting heart failure and performed meta-analysis with acceptable SROC as 0.9291. Among the variance analysis, the diagnostic performance of miR-423-5p claimed significant advantages of other pooled results. However, the combination of miRNAs and BNP could increase the accuracy of detecting of heart failure. Unfortunately, there was no dramatic advantage of miR-423-5p compared to BNP protocol. Conclusion: Despite interstudy variability, the performance test of miRNA for detecting heart failure revealed that miR-423-5p demonstrated the potential to be a biomarker. However, other miRNAs were not able to provide enough evidence on promising diagnostic value for heart failure based on the current data. Moreover, the combination of miRNAs and BNP could work as a better method to detection. Unfortunately, BNP was still the most convinced biomarker for such disease.
机译:背景:随着分子生物学的快速发展,在心脏发育和病理程序中,已经引入了麦克罗尔纳(miRNA)的种类。因此,我们进行该荟萃分析以发现在检测心力衰竭时循环miRNA作为生物标志物的作用。方法:我们搜查了受控试验的PubMed,Embase,Cochrane中央登记册,世界卫生组织临床试验登记中心,以确定高达2016年8月的相关研究。我们使用Meta-Disc的固定/随机效果模型进行了Meta分析1.4。我们使用Stata 14.0估计出版物偏见和元回归。此外,我们使用SPSS 17.0来评估几个组之间的方差。真正阳性,假阳性,假阴性和真实负面的信息,以及提取了研究质量。结果:我们使用10条文章的结果分析汇集精度。总混合miRNA(TMIRS)检测的总体性能是:汇集灵敏度,0.74(95%置信区间[CI],0.72至0.75);汇集特异性,0.69(95%CI,0.67至0.71);和面积在总结接收器下操作特征曲线值(SROC),0.7991。 miRNA-423-5P(miR-423-5p)检测是:汇集灵敏度,0.81(95%CI,0.76至0.85);合并特异性,0.67(95%CI,0.61至0.73);和SROC,0.8600。然而,采取相同的患者群体,我们提取了BNP的数据,用于检测心力衰竭,并通过可接受的SROC进行元分析为0.9291。在方差分析中,MIR-423-5P的诊断性能索赔了其他合并结果的显着优势。然而,miRNA和BNP的组合可以提高检测心力衰竭的准确性。不幸的是,与BNP协议相比,MIR-423-5P没有显着的优势。结论:尽管具有缺口性变异性,但MiRNA检测心力衰竭的性能试验显示MIR-423-5P证明是生物标志物的可能性。然而,其他miRNA不能根据当前数据提供足够的诊断价值的有足够的证据。此外,miRNA和BNP的组合可以作为更好的检测方法。不幸的是,BNP仍然是这种疾病最令人信服的生物标志物。

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