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首页> 外文期刊>Scientific reports. >The positive correlation of TIPRL with LC3 and CD133 contributes to cancer aggressiveness: potential biomarkers for early liver cancer
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The positive correlation of TIPRL with LC3 and CD133 contributes to cancer aggressiveness: potential biomarkers for early liver cancer

机译:Tiprl与LC3和CD133的正相关有助于癌症侵袭性:潜在的早期肝癌生物标志物

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摘要

Studies have reported dysregulation of TIPRL, LC3 and CD133 in liver cancer tissues. However, their respective relationships to liver cancer and roles as biomarkers for prognosis and diagnosis of liver cancer have never been studied. Here we report that the level of TIPRL is significantly correlated with levels of LC3 (Spearman r?=?0.9) and CD133 (r?=?0.7) in liver cancer tissues. We observed significant upregulations of TIPRL, LC3 and CD133 in hepatocellular carcinomas (HCCs) compared with adjacent normal tissues. Importantly, TIPRL, tested among additional variables, showed a significant impact on the prognosis of HCC patients. TIPRL knockdown significantly reduced expressions of LC3, CD133, stemness-related genes, as well as viability and stemness of liver cancer cell-lines, which were promoted by ectopic TIPRL expression. Either alone or as a combination, TIPRL, LC3 and CD133 showed significant values of area under the curve (AUC) and sensitivity/specificity in early liver cancer tissues. Furthermore, the statistical association and the diagnostic efficacies of TIPRL, LC3 and CD133 in HCC tissues were confirmed in a different IHC cohort. This data demonstrates that the complex involvement of TIPRL/LC3/CD133 in liver cancer aggressiveness can together or individually serve as potential biomarkers for the early detection of liver cancer.
机译:研究报道了肝癌组织中Tiprl,LC3和CD133的困难化。然而,他们对肝癌和角色的各自关系从未研究过肝癌的生物标志物和肝癌的诊断。在这里,我们报告说,Tiprl的水平与肝癌组织中的LC3(Spearman R?= 0.9)和CD133(R?= 0.7)的水平显着相关。与相邻的正常组织相比,我们观察到肝细胞癌(HCCS)中的TiPRL,LC3和CD133的显着上调。重要的是,在额外变量中测试的TiPRL对HCC患者的预后表现出显着影响。 TIPRL敲低显着降低了LC3,CD133,茎干相关基因的表达,以及肝癌细胞系的活力和茎,其被异位铸模表达促进。单独或作为组合,Tiprl,Lc3和CD133显示出在曲线(AUC)下的面积显着的面积值和早期肝癌组织中的敏感性/特异性。此外,在不同的IHC队列中证实了HCC组织中TIPRL,LC3和CD133的统计关联和诊断效果。该数据表明,Tiprl / LC3 / CD133在肝癌中的复杂性累及可以一起或单独用作潜在的生物标志物,用于早期发现肝癌。

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