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High Keratin 8/18 Ratio Predicts Aggressive Hepatocellular Cancer Phenotype

机译:高角蛋白8/18比值可预测侵略性肝细胞癌的表型

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摘要

BACKGROUND & AIMS: Steatohepatitis (SH) and SH-associated hepatocellular carcinoma (HCC) are of considerable clinical significance. SH is morphologically characterized by steatosis, liver cell ballooning, cytoplasmic aggregates termed Mallory-Denk bodies (MDBs), inflammation, and fibrosis at late stage. Disturbance of the keratin cytoskeleton and aggregation of keratins (KRTs) are essential for MDB formation. METHODS: We analyzed livers of aged Krt18−/− mice that spontaneously developed in the majority of cases SH-associated HCC independent of sex. Interestingly, the hepatic lipid profile in Krt18−/− mice, which accumulate KRT8, closely resembles human SH lipid profiles and shows that the excess of KRT8 over KRT18 determines the likelihood to develop SH-associated HCC linked with enhanced lipogenesis. RESULTS: Our analysis of the genetic profile of Krt18−/− mice with 26 human hepatoma cell lines and with data sets of >300 patients with HCC, where Krt18−/− gene signatures matched human HCC. Interestingly, a high KRT8/18 ratio is associated with an aggressive HCC phenotype. CONCLUSIONS: We can prove that intermediate filaments and their binding partners are tightly linked to hepatic lipid metabolism and to hepatocarcinogenesis. We suggest KRT8/18 ratio as a novel HCC biomarker for HCC.
机译:背景与目的:脂肪性肝炎(SH)和与SH相关的肝细胞癌(HCC)具有重要的临床意义。 SH的形态学特征是脂肪变性,肝细胞膨胀,被称为Mallory-Denk体(MDB)的细胞质聚集体,炎症和晚期纤维化。角蛋白细胞骨架的紊乱和角蛋白(KRT)的聚集对于MDB的形成至关重要。方法:我们分析了在大多数情况下,SH相关的HCC独立于性别而衰老的Krt18 -/-小鼠的肝脏。有趣的是,积累了KRT8的Krt18 -/-小鼠的肝脂质谱非常类似于人的SH脂质谱,表明KRT8超过KRT18的过量程度决定了与SH相关的HCC发生的可能性。脂肪形成增强。结果:我们分析了Krt18 -/-小鼠的遗传学特征,该小鼠具有26例人类肝癌细胞系和数据集> 300例HCC患者,其中Krt18 -/-基因签名与人类肝癌相匹配。有趣的是,高KRT8 / 18比例与积极的HCC表型相关。结论:我们可以证明中间丝及其结合伙伴与肝脂质代谢和肝癌发生紧密相关。我们建议将KRT8 / 18比值作为HCC的新型HCC生物标志物。

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