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首页> 外文期刊>Genes, Chromosomes and Cancer >miR-221/222 cluster expression improves clinical stratification of non-muscle invasive bladder cancer (TaT1) patients' risk for short-term relapse and progression
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miR-221/222 cluster expression improves clinical stratification of non-muscle invasive bladder cancer (TaT1) patients' risk for short-term relapse and progression

机译:miR-221/222簇表达改善了非肌肉侵袭性膀胱癌(TAT1)患者短期复发和进展风险的临床分层

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摘要

Clinical heterogeneity of bladder cancer prognosis requires the identification of bladder tumors' molecular profile to improve the prediction value of the established and clinically used markers. In this study, we have analyzed miR-221/222 cluster expression in bladder tumors and its clinical significance for patients' prognosis and disease outcome. The study included 387 tissue specimens. Following extraction, total RNA was polyadenylated at 3'-end and reversed transcribed. SYBR-Green based qPCR assays were performed for the quantification of miR-221/222 expression. Extensive statistical analysis was completed for the evaluation of miR-221/222 cluster's clinical significance. The expression of miR-221/222 is significantly downregulated in tumors compared to normal urothelium, while ROC curve and logistic regression analysis highlighted cluster's discriminatory ability. However, miR-222 levels were increased in muscle-invasive (T2-T4) compared to superficial tumors (TaT1), and in high compared to low-grade tumors. Kaplan-Meier survival curves and Cox regression analysis revealed the stronger risk of TaT1 patients overexpressing miR-222 for disease short-term relapse and progression following treatment. Moreover, multivariate Cox models highlighted the independent prognostic value of miR-222 overexpression for TaT1 patients' poor prognosis. Finally, the analysis of miR-222 expression improved significantly the positive prediction strength of the clinically used prognostic markers of tumor stage, grade, EORTC risk-stratification and recurrence at the first follow-up cystoscopy for TaT1 patients' outcome, and resulted to higher clinical net benefit following decision curve analysis. In conclusion, the expression of miR-221/222 cluster is deregulated in bladder tumors and miR-222 overexpression results to a superior positive prediction of TaT1 patients' short-term relapse and progression.
机译:膀胱癌预后的临床异质性需要鉴定膀胱肿瘤的分子曲线,以改善已建立和临床使用的标志物的预测值。在这项研究中,我们在膀胱肿瘤中分析了miR-221/222簇表达及其对患者预后和疾病结果的临床意义。该研究包括387个组织标本。提取后,在3'-末端的总RNA聚酰胺化并反转转录。对MiR-221/222表达的定量进行SYBR-Green基QPCR测定。完成了广泛的统计分析,用于评估miR-221/222簇的临床意义。与正常的尿路鞘相比,MIR-221/222的表达在肿瘤中显着下调,而ROC曲线和逻辑回归分析突出显示集群的歧视能力。然而,与浅表肿瘤(TAT1)相比,肌肉侵袭性(T2-T4)中的miR-222水平增加,与低级肿瘤相比,高。 Kaplan-Meier生存曲线和Cox回归分析显示,疾病短期复发和进展过表达MIR-222的TAT1患者的风险较强。此外,多元COX模型强调了MIR-222过表达对TAT1患者预后的独立预后价值。最后,MiR-222表达的分析显着改善了肿瘤阶段,等级,EORTC风险分层和复发的临床使用预测强度,在第一次随访膀胱镜检查中进行TAT1患者的结果,导致更高判决曲线分析后的临床净利润。总之,MiR-221/222簇的表达在膀胱肿瘤中解毒,miR-222过表达导致TAT1患者短期复发和进展的优异阳性预测。

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