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Opposing Roles of the Forkhead Box Factors FoxM1 and FoxA2 in Liver Cancer

机译:Foxm1和Foxa2在肝癌中的反对角色

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The forkhead box transcription factor FoxM1 is essential for hepatocellular carcinoma (HCC) development, and its overexpression coincides with poor prognosis. Here, we show that the mechanisms by which FoxM1 drives HCC progression involve overcoming the inhibitory effects of the liver differentiation gene FoxA2. First, the expression patterns of FoxM1 and FoxA2 in human HCC are opposite. We show that FoxM1 represses expression of FoxA2 in G(1) phase. Repression of FoxA2 in G(1) phase is important, as it is capable of inhibiting expression of the pluripotency genes that are expressed mainly in S-G(2) phases. Using a transgenic mouse model for oncogenic Ras-driven HCC, we provide genetic evidence for a repression of FoxA2 by FoxM1. Conversely, FoxA2 inhibits expression of FoxM1 and inhibits FoxM1-induced tumorigenicity. Also, FoxA2 inhibits Ras-induced HCC progression that involves FoxM1.
机译:FORKHEAD箱转录因子FOXM1对于肝细胞癌(HCC)发育至关重要,其过度表达与预后不良吻合。 在这里,我们表明FOXM1驱动HCC进展的机制涉及克服肝脏分化基因FOXA2的抑制作用。 首先,人HCC中FOXM1和FOXA2的表达模式相反。 我们表明FOXM1在G(1)阶段中抑制FOXA2的表达。 抑制FOXA2在G(1)相中是重要的,因为它能够抑制主要在S-G(2)相中表达的多能性基因的表达。 使用对癌癌的转基因小鼠模型驱动的HCC,我们提供Foxm1抑制Foxa2的遗传证据。 相反,FOXA2抑制FOXM1的表达,并抑制FOXM1诱导的肿瘤瘤性。 此外,FOXA2抑制RAS诱导的HCC进展,涉及FOXM1。

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