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Destruction complex dynamics: Wnt/beta-catenin signaling alters Axin-GSK3 beta interactions in vivo

机译:销毁复杂动态:Wnt /β-连环蛋白信号传导改变体内暂停-GSK3β相互作用

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The central regulator of the Wnt/beta-catenin pathway is the Axin/APC/GSK3 beta destruction complex (DC), which, under unstimulated conditions, targets cytoplasmic beta-catenin for degradation. How Wnt activation inhibits the DC to permit beta-catenin-dependent signaling remains controversial, in part because the DC and its regulation have never been observed in vivo. Using bimolecular fluorescence complementation (BiFC) methods, we have now analyzed the activity of the DC under near-physiological conditions in Drosophila. By focusing on well-established patterns of Wnt/Wg signaling in the developing Drosophila wing, we have defined the sequence of events by which activated Wnt receptors induce a conformational change within the DC, resulting in modified Axin-GSK3 beta interactions that prevent beta-catenin degradation. Surprisingly, the nucleus is surrounded by active DCs, which principally control the degradation of beta-catenin and thereby nuclear access. These DCs are inactivated and removed upon Wnt signal transduction. These results suggest a novel mechanistic model for dynamic Wnt signal transduction in vivo.
机译:Wnt /β-连环蛋白途径的中央调节剂是轴/ APC /GSK3ββ损伤复合物(DC),其在未刺激的条件下靶向细胞质β-连环蛋白进行降解。 WNT激活如何抑制DC允许β-连环蛋白依赖的信号传导仍然存在争议,部分是因为DC及其调节从未在体内观察过。使用双分子荧光互补(BIFC)方法,我们现在已经分析了DC在果蝇的近乎生理条件下的活性。通过专注于发展果蝇翼的Wnt / WG信号传导的良好模式,我们定义了活化的Wnt受体在DC内诱导构象变化的事件序列,导致预防β-的修饰的轴-GSK3β相互作用Catenin降解。令人惊讶的是,核被活性DC包围,主要控制β-连环蛋白的降解,从而核接入。在WNT信号转导时灭活并除去这些DC。这些结果表明了一种用于体内动态WNT信号转导的新型机制模型。

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