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首页> 外文期刊>Journal of Cancer >Identification of microRNA-92a and the related combination biomarkers as promising substrates in predicting risk, recurrence and poor survival of colorectal cancer
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Identification of microRNA-92a and the related combination biomarkers as promising substrates in predicting risk, recurrence and poor survival of colorectal cancer

机译:鉴定microRNA-92a和相关组合生物标志物作为预测结直肠癌风险,复发和不良生存的有前途的底物

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Background : Previous studies demonstrated that microRNA-92a (miR-92a) may serve as a novel promising biomarker in colorectal cancer (CRC) patients. However, a comprehensive analysis of the contribution of miR-92a in CRC is lacking. We aimed to systematically summarize the diagnostic and prognostic values of miR-92a in CRC. Methods : The diagnostic and prognostic roles of individual miR-92a and the combination biomarkers based on miR-92a were evaluated through comprehensive meta-analyses. Meanwhile, the function and potential mechanisms of miR-92a were assessed by an integrative bioinformatics analysis. Results : According to the results, we found that miR-92a yielded a pooled area under ROC curve (AUC) of 0.82 (sensitivity: 76%, specificity: 75%) in discriminating CRC from controls. Notably, the combination biomarkers based on miR-92a increased the diagnostic performance, yielding an AUC of 0.91, with a sensitivity of 83% and a specificity of 87%. For the prognostic meta-analysis, patients with higher expression of miR-92a had significant shorter overall survival (pooled HR: 2.30; 95% CI: 1.03-5.12). In addition, the regulated genes of miR-92a were retrieved and enriched through gene ontology and pathway analysis, indicating their correlations with the initiation and progression of CRC. Furthermore, protein-protein interaction network was set up with miR-92a targets and screened for hub nodes and significant modules, which were confirmed strongly involved in the occurrence and development of CRC again. Conclusions : Current evidences suggest miR-92a is a promising biomarker for early detection and prognosis of CRC while miRNA combination biomarkers may be considered as the right way for clinical practice. However, more prospective studies are required to highlight the theoretical strengths.
机译:背景:先前的研究表明,microRNA-92a(miR-92a)可以作为结直肠癌(CRC)患者的一种有前途的生物标志物。但是,缺乏对miR-92a在CRC中贡献的全面分析。我们旨在系统总结miR-92a在CRC中的诊断和预后价值。方法:通过全面的荟萃分析评估单个miR-92a的诊断和预后作用以及基于miR-92a的组合生物标记物。同时,通过综合生物信息学分析评估了miR-92a的功能和潜在机制。结果:根据结果,我们发现miR-92a在ROC曲线下的合并区域(AUC)为0.82(敏感性:76%,特异性:75%),可将CRC与对照区分开。值得注意的是,基于miR-92a的组合生物标志物可提高诊断性能,AUC为0.91,灵敏度为83%,特异性为87%。对于预后荟萃分析,miR-92a高表达患者的总生存期明显缩短(合并HR:2.30; 95%CI:1.03-5.12)。此外,通过基因本体论和途径分析检索和富集了miR-92a的调控基因,表明它们与CRC的发生和发展相关。此外,建立了具有miR-92a靶标的蛋白质-蛋白质相互作用网络,并筛选了枢纽节点和重要模块,这些已被证实再次参与了CRC的发生和发展。结论:目前的证据表明,miR-92a是用于CRC早期检测和预后的有前途的生物标志物,而miRNA组合生物标志物可能被认为是临床实践的正确方法。但是,需要更多的前瞻性研究来突出理论优势。

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