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首页> 外文期刊>Hepatology: Official Journal of the American Association for the Study of Liver Diseases >Human hepatocellular carcinomas with 'Stemness'-related marker expression: keratin 19 expression and a poor prognosis.
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Human hepatocellular carcinomas with 'Stemness'-related marker expression: keratin 19 expression and a poor prognosis.

机译:具有“ Stemness”相关标志物表达的人肝细胞癌:角蛋白19表达且预后不良。

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摘要

There is a recently proposed subtype of hepatocellular carcinoma (HCC) that is histologically similar to usual HCC, but characterized by the expression of stemness was performed to investigate the clinicopathologic features and epithelial-mesenchymal transition (EMT)-related protein expression status of this subtype of HCCs. The expression status of stemness-related (e.g., keratin 19 [K19], cluster of differentiation [CD]133, epithelial cell adhesion molecule [EpCAM], and c-kit) and EMT-related markers (e.g., snail, S100A4, urokinase plasminogen activator receptor [uPAR], ezrin, vimentin, E-cadherin, and matrix metalloproteinase [MMP]2) were examined using tissue microarrays from cohort 1 HCCs (n = 137). K19 protein expression in cohort 2 HCCs (n = 237) was correlated with the clinicopathologic parameters and messenger RNA (mRNA) levels of K19, uPAR, VIL2, Snail, Slug, and Twist. K19, EpCAM, c-kit, and CD133 positivity were observed in 18.2%, 35.0%, 34.3%, and 24.8%, respectively. K19 was most frequently expressed in combination with at least one other stemness-related marker (92.0%). K19-positive HCCs demonstrated more frequent major vessel invasion and increased tumor size, compared to K19-negative HCCs (P < 0.05). K19 was most significantly associated with EMT-related protein expression (e.g., vimentin, S100A4, uPAR, and ezrin) (P < 0.05) and a poor prognosis (overall survival: P = 0.018; disease-free survival: P = 0.007) in cohort 1. In cohort 2, HCCs with high K19 mRNA levels demonstrated higher mRNA levels of Snail, uPAR, and MMP2 (P < 0.05). K19-positive HCCs demonstrated more frequent microvascular invasion, fibrous stroma, and less tumor-capsule formation, compared to K19-negative HCCs (P < 0.05). K19 expression was a significant independent predictive factor of poor disease-free survival (P = 0.032). CONCLUSION: K19 was well correlated with clinicopathologic features of tumor aggressiveness, compared to other stemness-related proteins. K19-positive HCCs showed significantly increased EMT-related protein and mRNA expression, suggesting that they may acquire more invasive characteristics, compared to K19-negative HCCs through the up-regulation of EMT-associated genes.
机译:最近有一种提议的肝细胞癌(HCC)亚型在组织学上与普通HCC类似,但以干表达为特征进行了研究,以研究该亚型的临床病理特征和上皮-间质转化(EMT)相关蛋白的表达状态HCC。干性相关(例如角蛋白19 [K19],分化簇[CD] 133,上皮细胞粘附分子[EpCAM]和c-kit)和EMT相关标记(例如蜗牛,S100A4,尿激酶)的表达状态使用来自队列1 HCC(n = 137)的组织微阵列检查了纤溶酶原激活剂受体[uPAR],ezrin,波形蛋白,E-钙粘着蛋白和基质金属蛋白酶[MMP] 2)。队列2 HCC中的K19蛋白表达(n = 237)与K19,uPAR,VIL2,Snail,Slug和Twist的临床病理参数和信使RNA(mRNA)水平相关。观察到K19,EpCAM,c-kit和CD133阳性率分别为18.2%,35.0%,34.3%和24.8%。 K19最常与至少一种其他与干性相关的标记结合在一起表达(92.0%)。与K19阴性的HCC相比,K19阳性的HCC表现出更频繁的主要血管浸润和肿瘤大小的增加(P <0.05)。 K19与EMT相关蛋白表达(例如波形蛋白,S100A4,uPAR和ezrin)最显着相关(P <0.05),且预后较差(总生存期:P = 0.018;无病生存期:P = 0.007)。队列1.在队列2中,具有高K19 mRNA水平的HCC表现出较高的Snail,uPAR和MMP2 mRNA水平(P <0.05)。与K19阴性的HCC相比,K19阳性的HCC表现出更频繁的微血管侵袭,纤维基质和较少的肿瘤包膜形成(P <0.05)。 K19表达是无病生存期差的重要独立预测因素(P = 0.032)。结论:与其他干性相关蛋白相比,K19与肿瘤侵袭性的临床病理特征密切相关。与通过EMT相关的基因上调相比,与K19阴性的HCC相比,K19阳性的HCC显着增加了EMT相关的蛋白和mRNA表达,这表明它们可能具有更多的侵袭性。

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