首页> 美国卫生研究院文献>International Journal of Chronic Obstructive Pulmonary Disease >Pri-microRNA-124 rs531564 polymorphism minor allele increases the risk of pulmonary artery hypertension by abnormally enhancing proliferation of pulmonary artery smooth muscle cells
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Pri-microRNA-124 rs531564 polymorphism minor allele increases the risk of pulmonary artery hypertension by abnormally enhancing proliferation of pulmonary artery smooth muscle cells

机译:Pri-microRNA-124 rs531564多态性次要等位基因通过异常增强肺动脉平滑肌细胞的增殖而增加了发生肺动脉高压的风险

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摘要

MicroRNA-124 (miR-124) has been reported to be downregulated in the cells exposed to hypoxia, which was confirmed in our study. We then used online microRNA target prediction tools to identify GRB2, SMAD5, and JAG1 as the candidate target genes of miR-124, and we next validated GRB2 as a direct gene by using luciferase reporter system. We also established the regulatory relationship between miR-124 and GRB2 by showing the negative linear relationship between GRB2 and miR-124 expression. Furthermore, we investigated the miR-124 and GRB2 expression levels of different genotypes including CC (n=30), GC (n=18), and GG (n=4), which supported the hypothesis that the presence of minor allele (C) of rs531564 polymorphism compromised the expression of miR-124. Meanwhile, we also conducted real-time polymerase chain reaction and Western blot analysis to study the expression of GRB2 among different genotypes or pulmonary artery smooth muscle cells (PASMCs) treated with miR-124 mimics, GRB2 small interfering RNA, and miR-124 inhibitors, respectively, and found that introduction of miR-124 or GRB2 small interfering RNA could reduce the expression of GRB2 and inhibit the proliferation of PASMCs, while miR-124 upregulated the expression of GRB2 and promoted the proliferation of PASMCs. A total of 412 COPD patients with PAH (n=182) or without PAH (n=230) were recruited in this study, and more individuals carrying at least one minor allele of rs531564 were found in the COPD patients with PAH than in those without PAH (odds ratio: 0.61, 95% confidence interval: 0.41–0.91; P=0.166). In conclusion, the presence of rs531564 minor allele may increase the risk of PAH in COPD by reducing miR-124 expression, increasing GRB2 expression, and promoting the proliferation of PASMCs.
机译:据报道,在暴露于低氧的细胞中,MicroRNA-124(miR-124)被下调,这在我们的研究中得到了证实。然后,我们使用在线microRNA靶标预测工具将GRB2,SMAD5和JAG1鉴定为miR-124的候选靶标基因,然后我们通过使用荧光素酶报告系统将GRB2验证为直接基因。通过显示GRB2和miR-124表达之间的负线性关系,我们还建立了miR-124和GRB2之间的调节关系。此外,我们调查了不同基因型的miR-124和GRB2表达水平,包括CC(n = 30),GC(n = 18)和GG(n = 4),这支持了未成年人等位基因(C )的rs531564多态性损害了miR-124的表达。同时,我们还进行了实时聚合酶链反应和Western印迹分析,以研究GRB2在miR-124模拟物,GRB2小干扰RNA和miR-124抑制剂处理的不同基因型或肺动脉平滑肌细胞(PASMC)中的表达。分别发现,miR-124或GRB2小干扰RNA的引入可以降低GRB2的表达并抑制PASMCs的增殖,而miR-124上调GRB2的表达并促进PASMCs的增殖。这项研究共招募了412名患有PAH(n = 182)或没有PAH(n = 230)的COPD患者,并且在患有PAH的COPD患者中,发现携带至少一个rs531564次要等位基因的个体PAH(赔率:0.61,95%置信区间:0.41-0.91; P = 0.166)。总之,rs531564次要等位基因的存在可能通过减少miR-124表达,增加GRB2表达并促进PASMC增殖而增加COPD中PAH的风险。

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