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人类心肌病中心肌微小RNA与信使RNA的相互调控以及生物力学支持对微小RNA特征的逆转

Reciprocal regulation of myocardial microRNAs and messenger RNA in human cardiomyopathy and reversal of the microRNA signature by biomechanical support.

作者信息

Matkovich Scot J, Van Booven Derek J, Youker Keith A, Torre-Amione Guillermo, Diwan Abhinav, Eschenbacher William H, Dorn Lisa E, Watson Mark A, Margulies Kenneth B, Dorn Gerald W

机构信息

Center for Pharmacogenomics, Washington University, St Louis, MO 63110, USA.

出版信息

Circulation. 2009 Mar 10;119(9):1263-71. doi: 10.1161/CIRCULATIONAHA.108.813576. Epub 2009 Feb 23.

DOI:10.1161/CIRCULATIONAHA.108.813576
PMID:19237659
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2749457/
Abstract

BACKGROUND

Much has been learned about transcriptional control of cardiac gene expression in clinical and experimental congestive heart failure (CHF), but less is known about dynamic regulation of microRNAs (miRs) in CHF and during CHF treatment. We performed comprehensive microarray profiling of miRs and messenger RNAs (mRNAs) in myocardial specimens from human CHF with (n=10) or without (n=17) biomechanical support from left ventricular assist devices in comparison to nonfailing hearts (n=11).

METHODS AND RESULTS

Twenty-eight miRs were upregulated >2.0-fold (P<0.001) in CHF, with nearly complete normalization of the heart failure miR signature by left ventricular assist device treatment. In contrast, of 444 mRNAs that were altered by >1.3-fold in failing hearts, only 29 mRNAs normalized by as much as 25% in post-left ventricular assist device hearts. Unsupervised hierarchical clustering of upregulated miRs and mRNAs with nearest centroid analysis and leave-1-out cross-validation revealed that combining the miR and mRNA signatures increased the ability of RNA profiling to serve as a clinical biomarker of diagnostic group and functional class.

CONCLUSIONS

These results show that miRs are more sensitive than mRNAs to the acute functional status of end-stage heart failure, consistent with important functions for regulated miRs in the myocardial response to stress. Combined miR and mRNA profiling may have superior potential as a diagnostic and prognostic test in end-stage cardiomyopathy.

摘要

背景

在临床和实验性充血性心力衰竭(CHF)中,人们对心脏基因表达的转录调控已有诸多了解,但对于CHF及其治疗过程中微小RNA(miR)的动态调控却知之甚少。我们对来自接受(n = 10)或未接受(n = 17)左心室辅助装置生物力学支持的人类CHF心肌标本中的miR和信使核糖核酸(mRNA)进行了全面的微阵列分析,并与非衰竭心脏(n = 11)进行了比较。

方法与结果

28种miR在CHF中上调超过2.0倍(P<0.001),左心室辅助装置治疗后心力衰竭的miR特征几乎完全恢复正常。相比之下,在衰竭心脏中变化超过1.3倍的444种mRNA中,只有29种mRNA在左心室辅助装置治疗后的心脏中恢复正常达25%。对上调的miR和mRNA进行无监督层次聚类,并采用最近质心分析和留一法交叉验证,结果显示,将miR和mRNA特征相结合可提高RNA分析作为诊断组和功能类临床生物标志物的能力。

结论

这些结果表明,miR比mRNA对终末期心力衰竭的急性功能状态更敏感,这与受调控的miR在心肌应激反应中的重要功能一致。联合miR和mRNA分析在终末期心肌病的诊断和预后检测中可能具有更大的潜力。

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