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Interaction of Dishevelled and Xenopus Axin-Related Protein Is Required for Wnt Signal Transduction

机译:Wnt信号转导需要蓬乱和非洲爪蟾毒素相关蛋白的相互作用

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摘要

Signaling by the Wnt family of secreted proteins plays an important role in animal development and is often misregulated in carcinogenesis. Wnt signal transduction is controlled by the rate of degradation of β-catenin by a complex of proteins including glycogen synthase kinase 3 (GSK3), adenomatous polyposis coli, and Axin. Dishevelled is required for Wnt signal transduction, and its activation results in stabilization of β-catenin. However, the biochemical events underlying this process remain largely unclear. Here we show that Xenopus Dishevelled (Xdsh) interacts with a Xenopus Axin-related protein (XARP). This interaction depends on the presence of the Dishevelled-Axin (DIX) domains in both XARP and Xdsh. Moreover, the same domains are essential for signal transduction through Xdsh. Finally, our data point to a possible mechanism for signal transduction, in which Xdsh prevents β-catenin degradation by displacing GSK3 from its complex with XARP.
机译:分泌蛋白的Wnt家族发出的信号在动物发育中起重要作用,并且在致癌过程中经常被错误调节。 Wnt信号转导受包括糖原合酶激酶3(GSK3),腺瘤性息肉病和Axin在内的蛋白质复合物降解β-catenin的速率控制。 Wnt信号转导需要弄乱,并且其激活可导致β-catenin稳定。但是,该过程的生化事件仍不清楚。在这里,我们显示非洲爪蟾Disheveled(Xdsh)与非洲爪蟾毒素相关蛋白(XARP)相互作用。这种相互作用取决于XARP和Xdsh中Dishevelled-Axin(DIX)域的存在。此外,相同的域对于通过Xdsh进行信号转导至关重要。最后,我们的数据指出了信号转导的可能机制,其中Xdsh通过将GSK3与XARP的复合物置换来防止β-catenin降解。

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