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首页> 外文期刊>European review for medical and pharmacological sciences. >Up?regulation of lncRNA PXN-AS1-L is associated with unfavorable prognosis in patients suffering from glioma
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Up?regulation of lncRNA PXN-AS1-L is associated with unfavorable prognosis in patients suffering from glioma

机译:UP?LNCRNA PXN-AS1-L的调节与患有胶质瘤的患者的不利预后有关

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OBJECTIVE: Growing evidence has proved that long noncoding RNAs (lncRNAs) act as novel regulators in the progression of various tumors by modulating miRNAs and tumor-related genes. However, the potential function of lncRNA PXN-AS1-L (PXN-AS1-L) in glioma remains unknown. Hence, we aimed to determine whether PXN-AS1-L was dysregulated in glioma and further preliminarily explored its prognostic value in glioma patients. PATIENTS AND METHODS: RT-PCR was used for the assessment of PXN-AS1-L levels in glioma tissue and matched normal tissues from our hospital. Chi-square test was applied to explore the possible association between PXN-AS1-L expressions and clinical factors. Kaplan-Meier survival analysis was carried out to determine the influence of PXN-AS1-L expressions on the survival rate of glioma patients. Survival data were further evaluated through univariate and multivariate analyses. RESULTS: PXN-AS1-L levels were differentially upregulated in glioma specimens compared with paired non-tumor specimens. Higher levels of PXN-AS1-L in glioma were observed to be positively associated with WHO grade (p = 0.019), KPS (p = 0.008)and tumor recurrence (p = 0.019). Survival assays revealed that glioma patients with higher PXN-AS1-L expressions had worse overall survival rates. In multivariate analysis, upregulation of PXN-AS1-L expressions (Risk ratio = 2.663, 1.218-4.532, p = 0.014) in glioma tissues was confirmed to be an independent prognostic factor of overall survival in patients. CONCLUSIONS: We firstly suggested that PXN-AS1-L was overexpressed in glioma, and could be used as a novel marker of unfavorable outcome in glioma patients.
机译:目的:越来越多的证据证明,通过调节miRNA和肿瘤相关基因,长期非编码RNA(LNCRNA)作为各种肿瘤进展中的新型调节因子。然而,胶质瘤中LNCRNA PXN-AS1-L(PXN-AS1 -L)的潜在功能仍然未知。因此,我们旨在确定PXN-AS1-L是否在胶质瘤中讨论并进一步初步探讨了胶质瘤患者的预后价值。患者及方法:RT-PCR用于评估胶质瘤组织中的PXN-AS1-L水平,并从我们院匹配正常组织。应用Chi-Square测试探讨PXN-AS1-L表达和临床因素之间的可能关联。进行了Kaplan-Meier存活分析,以确定PXN-AS1-L表达对胶质瘤患者的存活率的影响。通过单变量和多变量分析进一步评估存活数据。结果:与配对的非肿瘤标本相比,PXN-AS1-L水平在胶质瘤样本中差异上调。观察到胶质瘤中的较高水平的PXN-AS1-L,与世卫组织(P = 0.019),KPS(P = 0.008)和肿瘤复发(P = 0.019)正相关。存活测定显示,具有较高PXN-AS1-L表达的胶质瘤患者的整体生存率差。在多变量分析中,胶质瘤组织中的PXN-AS1-L表达(风险比率= 2.663,1.218-4.532,P = 0.014)被证实是患者整体存活的独立预后因素。结论:我们首先建议PXN-AS1-L在胶质瘤中过表达,并且可以用作胶质瘤患者不利结果的新标记。

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