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FGF-20 and DKK1 are transcriptional targets of β-catenin and FGF-20 is implicated in cancer and development

机译:FGF-20和DKK1是β-catenin的转录靶标而FGF-20与癌症和发育有关

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摘要

β-catenin is the major effector of the canonical Wnt signaling pathway. Mutations in components of the pathway that stabilize β-catenin result in augmented gene transcription and play a major role in many human cancers. We employed microarrays to identify transcriptional targets of deregulated β-catenin in a human epithelial cell line (293) engineered to produce mutant β-catenin and in ovarian endometrioid adenocarcinomas characterized with respect to mutations affecting the Wnt/β-catenin pathway. Two genes strongly induced in both systems—FGF20 and DKK1—were studied in detail. Elevated levels of FGF20 RNA were also observed in adenomas from mice carrying the ApcMinallele. Both XFGF20 and Xdkk-1 are expressed early in Xenopus embryogenesis under the control of the Wnt signaling pathway. Furthermore, FGF20 and DKK1 appear to be direct targets for β-catenin/TCF transcriptional regulation via LEF/TCF-binding sites. Finally, by using small inhibitory RNAs specific for FGF20, we show that continued expression of FGF20 is necessary for maintenance of the anchorage-independent growth state in RK3E cells transformed by β-catenin, implying that FGF-20 may be a critical element in oncogenesis induced by the Wnt signaling pathway.
机译:β-catenin是经典Wnt信号通路的主要效应物。使β-catenin稳定的途径成分中的突变导致基因转录增强,并在许多人类癌症中发挥重要作用。我们在人上皮细胞系(293)中设计了微阵列,以鉴定失调的β-catenin的转录靶标,该细胞系经工程改造可产生突变的β-catenin和卵巢内膜样腺癌,其特征在于影响Wnt /β-catenin途径的突变。详细研究了两个系统中强烈诱导的两个基因-FGF20和DKK1。在携带Apc Min 等位基因的小鼠的腺瘤中也观察到FGF20 RNA水平升高。 XFGF20和Xdkk-1都在Wnt信号通路的控制下在非洲爪蟾胚胎发生早期表达。此外,FGF20和DKK1似乎是通过LEF / TCF结合位点进行β-catenin/ TCF转录调控的直接靶标。最后,通过使用特异于FGF20的小抑制性RNA,我们表明FGF20的持续表达对于维持由β-catenin转化的RK3E细胞的锚定非依赖性生长状态是必要的,这暗示FGF-20可能是肿瘤发生的关键因素由Wnt信号通路诱导。

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