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Diagnostic Value of Circulating microRNAs for In-Stent Restenosis in Patients with Lower Extremity Arterial Occlusive Disease

机译:循环microRNA对下肢动脉阻塞性疾病患者支架内再狭窄的诊断价值

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In-stent restenosis (ISR) is still a major cause of failure of endovascular stenting treatment in patients with lower extremity arterial occlusive disease (LEAOD). Sensitive and reliable biomarkers for early diagnosis to predict ISR should be considered. This study was conducted to explore the diagnostic value of microRNA in predicting ISR in patients with LEAOD after endovascular stenting treatment. From March 2014 to July 2016, 208 patients (170 males and 38 females) with LEAOD undergoing interventional treatment were enrolled in this research. Patients were divided into the restenosis and non-restenosis groups according to routine postoperative angiography. Circulating microRNAs expression were detected in 208 participants, including 78 ISR patients, 68 non-ISR patients and 62 healthy volunteers. We selected 6 microRNAs from microarray screening as candidates for further testing via qRT-PCR. A receiver operating characteristic (ROC) curve was generated to assess the diagnostic value of circulating microRNAs in predicting ISR for LEAOD patients. The results showed that circulating microRNA-320a and microRNA-572 in patients with ISR (n?=?78) had significantly higher expression levels than it from non-ISR and healthy volunteers. By receiver operating characteristic curve analysis, the sensitivity was 82.1% and the specificity was 63.8% for microRNA-320a; the sensitivity was 69.2% and the specificity was 68.9% for microRNA-572, and the AUC was 0.766 and 0.690 for detection of ISR, respectively. Furthermore, 78 patients with ISR had significantly higher circulating expression levels of microRNA-3937 and microRNA-642a-3p and lower circulating expression levels of microRNA-4669 and microRNA-3138 compared with 68 non-ISR patients and 62 healthy volunteers, but they have no significant difference. We found that differential circulating microRNA expression in patients after stenting with ISR, and the data indicate that circulating microRNA-320a and microRNA-572 have promising value in diagnosing ISR in patients with LEAOD.
机译:支架内再狭窄(ISR)仍然是下肢动脉闭塞性疾病(LEAOD)患者进行血管内支架治疗失败的主要原因。应考虑用于早期诊断以预测ISR的灵敏可靠的生物标志物。本研究旨在探讨microRNA在血管内支架治疗后对LEAOD患者的ISR预测中的诊断价值。 2014年3月至2016年7月,本研究纳入了208例接受干预性治疗的LEAOD患者(170例男性和38例女性)。根据常规术后血管造影将患者分为再狭窄和非再狭窄组。在208名参与者中检测到循环microRNA的表达,包括78名ISR患者,68名非ISR患者和62名健康志愿者。我们从微阵列筛选中选择了6个microRNA作为通过qRT-PCR进行进一步测试的候选对象。生成了接收器操作特征(ROC)曲线,以评估循环微RNA在预测LEAOD患者的ISR中的诊断价值。结果表明,ISR患者(n == 78)的循环microRNA-320a和microRNA-572的表达水平明显高于非ISR和健康志愿者。通过受体工作特征曲线分析,对microRNA-320a的敏感性为82.1%,特异性为63.8%;对microRNA-572的敏感性为69.2%,特异性为68.9%,用于检测ISR的AUC分别为0.766和0.690。此外,与68名非ISR患者和62名健康志愿者相比,有78名ISR患者的microRNA-3937和microRNA-642a-3p的循环表达水平显着较高,而microRNA-4669和microRNA-3138的循环表达水平则较低。无明显差异。我们发现ISR支架置入患者后循环microRNA表达差异,数据表明循环microRNA-320a和microRNA-572在LEAOD患者的ISR诊断中具有广阔的应用前景。

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