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Proteomic screen with the proto-oncogene beta-catenin identifies interaction with Golgi coatomer complex I

机译:用原癌基因β-catenin进行蛋白质组学筛选可鉴定与高尔基涂层复合物I的相互作用

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摘要

Beta-catenin is well-known as a key effector of Wnt signalling and aberrant expression is associated with several human cancers. Stabilisation of and atypical subcellular localisation of beta-catenin, regulated in part through specific protein-protein interactions has been linked to cancer development, however the mechanisms behind these pathologies is yet to be fully elucidated. Affinity purification and mass spectrometry were used to identify potential β-catenin interacting proteins in SW480 colon cancer cells. Recombinant β-catenin constructs were used to co-isolate interacting proteins from stable isotope labelled cells followed by detection using mass spectrometry. Several known and new putative interactors were observed. In particular, we identified interaction with a set of coatomer complex I subunits implicated in retrograde transport at the Golgi, and confirmed endogenous interaction of β-catenin with coatomer subunit COPB using immunoprecipitation assays and immunofluorescence microscopy. These observations suggest a hitherto unrecognised role for β-catenin in the secretory pathway and warrant further functional studies to unravel its activity at this cellular location.
机译:β-catenin是Wnt信号的关键效应子,众所周知,异常表达与几种人类癌症有关。 β-catenin的稳定和非典型亚细胞定位(部分通过特定的蛋白质-蛋白质相互作用来调节)与癌症的发展有关,但是这些病理现象背后的机制尚待充分阐明。亲和纯化和质谱用于鉴定SW480结肠癌细胞中潜在的β-catenin相互作用蛋白。重组β-catenin构建体用于从稳定同位素标记的细胞中共分离相互作用的蛋白质,然后使用质谱检测。观察到了几种已知的和新的假定的相互作用子。特别是,我们确定了与高尔基体逆行运输牵涉的一组涂料复合物I亚基的相互作用,并使用免疫沉淀测定法和免疫荧光显微镜证实了β-连环蛋白与涂料亚基COPB的内源性相互作用。这些观察结果表明β-catenin在分泌途径中的作用迄今尚未被认识,并有待进一步的功能研究来揭示其在该细胞位置的活性。

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