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Deciphering preferential interactions within supramolecular protein complexes: the proteasome case

机译:破译超分子蛋白复合物中的优先相互作用:蛋白酶体情况

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摘要

In eukaryotic cells, intracellular protein breakdown is mainly performed by the ubiquitin–proteasome system. Proteasomes are supramolecular protein complexes formed by the association of multiple sub-complexes and interacting proteins. Therefore, they exhibit a very high heterogeneity whose function is still not well understood. Here, using a newly developed method based on the combination of affinity purification and protein correlation profiling associated with high-resolution mass spectrometry, we comprehensively characterized proteasome heterogeneity and identified previously unknown preferential associations within proteasome sub-complexes. In particular, we showed for the first time that the two main proteasome subtypes, standard proteasome and immunoproteasome, interact with a different subset of important regulators. This trend was observed in very diverse human cell types and was confirmed by changing the relative proportions of both 20S proteasome forms using interferon-γ. The new method developed here constitutes an innovative and powerful strategy that could be broadly applied for unraveling the dynamic and heterogeneous nature of other biologically relevant supramolecular protein complexes.
机译:在真核细胞中,细胞内蛋白质的分解主要由泛素-蛋白酶体系统完成。蛋白酶体是由多个亚复合物和相互作用的蛋白质结合形成的超分子蛋白质复合物。因此,它们表现出非常高的异质性,其功能仍未被很好地理解。在这里,我们使用一种基于亲和力纯化和与高分辨率质谱相关的蛋白质相关分析相结合的新开发方法,对蛋白酶体的异质性进行了全面表征,并确定了蛋白酶体亚复合物中以前未知的优先关联。特别是,我们首次展示了两种主要的蛋白酶体亚型,即标准蛋白酶体和免疫蛋白酶体,与重要调节剂的不同子集相互作用。在非常多种多样的人类细胞类型中观察到了这种趋势,并通过使用干扰素-γ改变了两种20S蛋白酶体形式的相对比例得到了证实。这里开发的新方法构成了一种创新而强大的策略,可以广泛地用于揭示其他生物学相关的超分子蛋白质复合物的动态和异质性质。

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