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Self-association of the APC tumor suppressor is required for the assembly, stability, and activity of the Wnt signaling destruction complex

机译:Ant肿瘤抑制因子的自缔合是Wnt信号破坏复合物的组装,稳定性和活性所必需的

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The tumor suppressor adenomatous polyposis coli (APC) is an essential negative regulator of Wnt signaling through its activity in the destruction complex with Axin, GSK3β, and CK1 that targets β-catenin/Armadillo (β-cat/Arm) for proteosomal degradation. The destruction complex forms macromolecular particles we termed the destructosome. Whereas APC functions in the complex through its ability to bind both β-cat and Axin, we hypothesize that APC proteins play an additional role in destructosome assembly through self-association. Here we show that a novel N-terminal coil, the APC self-association domain (ASAD), found in vertebrate and invertebrate APCs, directly mediates self-association of Drosophila APC2 and plays an essential role in the assembly and stability of the destructosome that regulates β-cat degradation in Drosophila and human cells. Consistent with this, removal of the ASAD from the Drosophila embryo results in β-cat/Arm accumulation and aberrant Wnt pathway activation. These results suggest that APC proteins are required not only for the activity of the destructosome, but also for the assembly and stability of this macromolecular machine.
机译:抑癌性腺瘤性息肉病大肠杆菌(APC)是Wnt信号的重要负调节剂,它具有与Axin,GSK3β和CK1的破坏复合物的活性,该复合物靶向蛋白链降解的β-catenin/ Armadillo(β-cat/ Arm)。破坏复合物形成大分子颗粒,我们称之为破坏小体。尽管APC通过结合β-cat和Axin的能力而在复合物中发挥功能,但我们假设APC蛋白通过自缔合在破坏小体的组装中起着另外的作用。在这里,我们显示在脊椎动物和无脊椎动物APC中发现的新型N末端线圈APC自缔合域(ASAD),直接介导果蝇APC2的自缔合,并在破坏性小体的组装和稳定性中起重要作用调节果蝇和人类细胞中的β-cat降解。与此相一致,从果蝇胚胎中去除ASAD会导致β-cat/ Arm积累和Wnt途径异常激活。这些结果表明,APC蛋白不仅对于破坏小体的活性是必需的,而且对于这种大分子机器的组装和稳定性也是必需的。

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