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WW Domain-Containing Proteins YAP and TAZ in the Hippo Pathway as Key Regulators in Stemness Maintenance, Tissue Homeostasis, and Tumorigenesis

机译:河马途径中包含WW域的蛋白质YAP和TAZ作为维持茎干,组织稳态和肿瘤发生的关键调节剂

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摘要

The Hippo pathway is a conserved signaling pathway originally defined in Drosophila melanogaster two decades ago. Deregulation of the Hippo pathway leads to significant overgrowth in phenotypes and ultimately initiation of tumorigenesis in various tissues. The major WW domain proteins in the Hippo pathway are YAP and TAZ, which regulate embryonic development, organ growth, tissue regeneration, stem cell pluripotency, and tumorigenesis. Recent reports reveal the novel roles of YAP/TAZ in establishing the precise balance of stem cell niches, promoting the production of induced pluripotent stem cells (iPSCs), and provoking signals for regeneration and cancer initiation. Activation of YAP/TAZ, for example, results in the expansion of progenitor cells, which promotes regeneration after tissue damage. YAP is highly expressed in self-renewing pluripotent stem cells. Overexpression of YAP halts stem cell differentiation and yet maintains the inherent stem cell properties. A success in reprograming iPSCs by the transfection of cells with Oct3/4, Sox2, and Yap expression constructs has recently been shown. In this review, we update the current knowledge and the latest progress in the WW domain proteins of the Hippo pathway in relevance to stem cell biology, and provide a thorough understanding in the tissue homeostasis and identification of potential targets to block tumor development. We also provide the regulatory role of tumor suppressor WWOX in the upstream of TGF-β, Hyal-2, and Wnt signaling that cross talks with the Hippo pathway.
机译:河马途径是保守的信号传导途径,最初在二十多年前在果蝇中定义。 Hippo通路的失调导致表型明显过度生长,并最终在各种组织中引发肿瘤发生。 Hippo途径中主要的WW域蛋白是YAP和TAZ,它们调节胚胎发育,器官生长,组织再生,干细胞多能性和肿瘤发生。最近的报道揭示了YAP / TAZ在建立干细胞生态位的精确平衡,促进诱导多能干细胞(iPSC)的产生以及激发再生和癌症引发信号方面的新颖作用。例如,YAP / TAZ的激活导致祖细胞的扩增,从而促进组织损伤后的再生。 YAP在自我更新的多能干细胞中高度表达。 YAP的过表达可阻止干细胞分化,并保持固有的干细胞特性。最近显示了通过用Oct3 / 4,Sox2和Yap表达构建体转染细胞成功重编程iPSC的成功。在这篇综述中,我们更新了与干细胞生物学相关的Hippo途径的WW域蛋白的最新知识和最新进展,并提供了对组织稳态的全面了解,并确定了阻止肿瘤发展的潜在靶标。我们还提供了肿瘤抑制因子WWOX在TGF-β,Hyal-2和Wnt信号通路上游的调控作用,这些信号通路与Hippo通路相互干扰。

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