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Microarray analysis reveals a potential role of lncRNA expression in remote ischemic preconditioning in myocardial ischemia-reperfusion injury

机译:微阵列分析显示LNCRNA表达在心肌缺血再灌注损伤中远程缺血预处理中的潜在作用

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The challenge to avoid or reduce cardiopulmonary bypass-related injuries in cardiovascular surgery remains a major issue. Remote ischemic preconditioning (RIPC) remains a promising strategy whose clinical applications appear to be significantly more realistic and extensive as compared with other conservative or surgical strategies. However, considering its underlying mechanism(s) are still unclear, novel ideas and methods must be explored to enhance its potential in clinical applications. Long noncoding RNAs (LncRNAs) are a kind of RNAs that have been implicated in the occurrence and development of cardiovascular diseases. The differently expressed LncRNAs and their biological effects during RIPC have not been explored previously. In this study, mouse and human LncRNA microarrays were used to investigate the expression signatures of LncRNAs and mRNAs in the myocardial tissue after RIPC. Therafter, homology comparisons were used to screen homologous genes from differentially expressed LncRNAs. Competing endogenous RNA (ceRNA) mechanism analysis were employed to find the matching relationship among homologous LncRNA, mRNA and microRNA. 554 differentially expressed mouse LncRNAs (281 up-regulated/273 down-regulated) and 1392 differentially expresssed human LncRNAs (635 up-regulated/757 down-regulated) were selected for further analysis. Quantitative real-time polymerase chain reaction (qRT-PCR) was used to quantify these LncRNAs, homology comparison and ceRNA mechanism analysis provided a pair of homologous LncRNAs (ENST00000574727 & ENSMUST00000123752) for further research investigation. Overall, in this study, a number of differentially expressed LncRNAs were identified which may play an important role the regulation of both inflammation and cell proliferation. The findings may thus unveil the mystery of RIPC and discover a novel protective mechanism for the mitigation of cardiovascular ischemia-reperfusion disease.
机译:避免或减少心血管外科手术中有相关的相关伤害的挑战仍然是一个主要问题。远程缺血预处理(RIPC)仍然是一个有希望的战略,其临床应用与其他保守或外科策略相比,临床应用似乎明显更加现实和广泛。然而,考虑到其潜在机制尚不清楚,必须探索新的思路和方法,以提高其在临床应用中的潜力。长时间的NOODING RNA(LNCRNA)是一种涉及心血管疾病的发生和发展的一种RNA。以前尚未探讨不同表达的LNCRNA及其在RIPC期间的生物效应。在该研究中,使用小鼠和人LNCRNA微阵列来研究RIPC后心肌组织中LNCRNA和MRNA的表达签名。其,同源性比较用于筛选来自差异表达的LNCRNA的同源基因。使用竞争内源性RNA(Cerna)机制分析来找到同源LNCRNA,mRNA和MicroRNA之间的匹配关系。 554差异表达的小鼠LNCRNA(281上调/ 273下调)和1392个差异表达的人LNCRNA(635次调节/ 757下调)进行进一步分析。定量实时聚合酶链反应(QRT-PCR)用于量化这些LNCRNA,同源性比较和Cerna机制分析提供了一对同源LNCRNA(ENST00000574727和ENSMUST00000123752),用于进一步研究调查。总体而言,在本研究中,鉴定了许多差异表达的LNCRNA,其可能起到调节炎症和细胞增殖的重要作用。因此,调查结果可以揭示RIPC的谜团,并发现一种用于减轻心血管缺血再灌注疾病的新型保护机制。

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