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首页> 外文期刊>Frontiers in Cardiovascular Medicine >Circulating microRNAs may serve as biomarkers for hypertensive emergency end-organ injuries and address underlying pathways in an animal model
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Circulating microRNAs may serve as biomarkers for hypertensive emergency end-organ injuries and address underlying pathways in an animal model

机译:循环的microRNA可以用作高血压急性终端器官伤害的生物标志物,并在动物模型中寻址潜在的途径

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There is an incomplete understanding of the underlying pathophysiology in hypertensive emergencies, where severely elevated blood pressure causes acute end-organ injuries, as opposed to the long-term manifestations of chronic hypertension. Furthermore, current biomarkers are unable to detect early end-organ injuries like hypertensive encephalopathy and renal thrombotic microangiopathy. We hypothesized that circulating microRNAs (c-miRs) could identify acute and chronic complications of severe hypertension, and that combinations of c-miRs could elucidate important pathways involved. We studied the diagnostic accuracy of 145 c-miRs in Dahl salt-sensitive rats fed either a low-salt (N=20: 0.3% NaCl) or a high-salt (N=60: 8% NaCl) diet. Subclinical hypertensive encephalopathy and thrombotic microangiopathy were diagnosed by histopathology. In addition, heart failure with preserved ejection fraction was evaluated with echocardiography and N-terminal pro-brain natriuretic peptide; and endothelial dysfunction was studied using acetylcholine-induced aorta ring relaxation. Systolic blood pressure increased severely in animals on a high-salt diet (high-salt 205±20 mm Hg vs. low-salt 152±18 mm Hg, p0.001). Partial least squares discriminant analysis revealed 68 c-miRs discriminating between animals with and without hypertensive emergency complications. Twenty-nine c-miRs were strongly associated with hypertensive encephalopathy, 24 c-miRs with thrombotic microangiopathy, 30 c-miRs with heart failure with preserved ejection fraction, and 28 c-miRs with endothelial dysfunction. Hypertensive encephalopathy, thrombotic microangiopathy and heart failure with preserved ejection fraction were associated with deviations in many of the same c-miRs, whereas endothelial dysfunction was associated with a different set of c-miRs. Several of these c-miRs demonstrated fair to good diagnostic accuracy for a composite outcome of hypertensive encephalopathy, thrombotic microangiopathy and heart failure with preserved ejection fraction in receiver-operating-curve analyses (area-under-curve 0.75-0.88). Target prediction revealed an enrichment of genes related to several pathways relevant for cardiovascular disease (e.g. mucin type O-glycan biosynthesis, MAPK, Wnt, Hippo, and TGF-beta signaling). C-miRs could potentially serve as biomarkers of severe hypertensive end-organ injuries and elucidate important pathways involved.
机译:对高血压突发事件的潜在病理生理学有不完全了解,血压严重升高导致急性终端器官受伤,而不是慢性高血压的长期表现。此外,目前的生物标志物无法检测高血压脑病和肾血栓细胞病变等早期末端器官伤害。我们假设循环的microRNA(C-MIRS)可以鉴定严重高血压的急性和慢性并发症,并且C-MIR的组合可以阐明所涉及的重要途径。我们研究了喂食低盐(n = 20:0.3%NaCl)或高盐(n = 60:8%NaCl)饮食的Dahl盐敏感大鼠中145c-mirs的诊断精度。通过组织病理学诊断亚临床性高血压脑病和血栓性微盲。此外,用超声心动图和N-末端促脑利钠肽评价具有保存射血分数的心力衰竭;使用乙酰胆碱诱导的主动脉环弛豫研究了内皮功能障碍。在高盐饮食(高盐205±20mm Hg,低盐152±18 mm Hg,P <0.001)中,收缩压血压严重增加。偏最小二乘判别分析显示68个C-MIR,歧视动物之间,没有高血压的紧急并发症。二十九个C-MIR与高血压脑病,24例C-MIR有血栓形成微肺病,30个C-MIR,心力衰竭,具有保存的喷射分数,28个C-miR,具有内皮功能障碍。高血压性脑病,血栓形成微神经病症和保存的喷射部分的心力衰竭与许多相同的C-miR中的偏差有关,而内皮功能障碍与不同的C-mirs相关。这些C-MIR中的一些展示了良好的诊断准确性,用于高血压脑病,血栓形成微疾病和心力衰竭的综合诊断准确性,在接收器 - 操作曲线分析中保存射血分数(面积曲线0.75-0.88)。靶预测揭示了与对心血管疾病相关的几种途径有关的基因的富集(例如,粘蛋白型O-聚糖生物合成,MAPK,WNT,HIPPO和TGF-Beta信号传导)。 C-MIR可能潜入严重高血压末端器官伤害的生物标志物,并阐明所涉及的重要途径。

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