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The Merlin/NF2 Tumor Suppressor Functions through the YAP Oncoprotein to Regulate Tissue Homeostasis in Mammals

机译:merlin / NF2肿瘤抑制因子通过Yap癌蛋白调节哺乳动物的组织稳态

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摘要

The conserved Hippo signaling pathway regulates organ size in Drosophila and mammals. While a core kinase cascade leading from the protein kinase Hippo (Hpo) (Mst1 and Mst2 in mammals) to the transcription coactivator Yorkie (Yki) (YAP in mammals) has been established, upstream regulators of the Hippo kinase cascade are less well defined, especially in mammals. Using conditional knockout mice, we demonstrate that the Merlin/NF2 tumor suppressor and the YAP oncoprotein function antagonistically to regulate liver development. While inactivation of Yap led to loss of hepatocytes and biliary epithelial cells, inactivation of Nf2 led to hepatocellular carcinoma and bile duct hamartoma. Strikingly, the Nf2-deficient phenotypes in multiple tissues were largely suppressed by heterozygous deletion of Yap, suggesting that YAP is a major effector of Merlin/NF2 in growth regulation. Our studies link Merlin/NF2 to mammalian Hippo signaling and implicate YAP activation as a mediator of pathologies relevant to Neurofibromatosis 2. © 2010 Elsevier Inc.
机译:保守的河马信号通路调节果蝇和哺乳动物的器官大小。虽然已经建立了从蛋白激酶河马(Hpo)(在哺乳动物中为Mst1和Mst2)到转录共激活因子Yorkie(Yki)(在哺乳动物中为YAP)的核心激酶级联反应,但对河马激酶级联反应的上游调节子的定义尚不明确,特别是在哺乳动物中。使用条件基因敲除小鼠,我们证明了Merlin / NF2肿瘤抑制因子和YAP癌蛋白拮抗功能来调节肝脏的发育。 Yap失活导致肝细胞和胆管上皮细胞丢失,而Nf2失活导致肝细胞癌和胆管错构瘤。令人惊讶的是,Yap的杂合缺失在很大程度上抑制了多个组织中Nf2缺陷型,这表明YAP是Merlin / NF2在生长调节中的主要效应器。我们的研究将Merlin / NF2链接到哺乳动物的河马信号,并暗示YAP激活作为与神经纤维瘤病2相关的病理介质。©2010 Elsevier Inc.。

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