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A census of human soluble protein complexes

机译:人类可溶性蛋白复合物普查

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Cellular processes often depend on stable physical associations between proteins. Despite recent progress, knowledge of the composition of human protein complexes remains limited. To close this gap, we applied an integrative global proteomic profiling approach, based on chromatographic separation of cultured human cell extracts into more than one thousand biochemical fractions that were subsequently analyzed by quantitative tandem mass spectrometry, to systematically identify a network of 13,993 high-confidence physical interactions among 3,006 stably associated soluble human proteins. Most of the 622 putative protein complexes we report are linked to core biological processes and encompass both candidate disease genes and unannotated proteins to inform on mechanism. Strikingly, whereas larger multiprotein assemblies tend to be more extensively annotated and evolutionarily conserved, human protein complexes with five or fewer subunits are far more likely to be functionally unannotated or restricted to vertebrates, suggesting more recent functional innovations.
机译:细胞过程通常取决于蛋白质之间的稳定物理联系。尽管有最近的进展,但是关于人类蛋白质复合物的组成的知识仍然有限。为了弥合这一差距,我们采用了集成的全局蛋白质组学分析方法,该方法基于将培养的人细胞提取物进行色谱分离,分离成一千多个生化部分,然后通过定量串联质谱法进行分析,以系统性地识别出13,993个高可信度网络3,006种稳定相关的可溶性人类蛋白质之间的物理相互作用。我们报告的622种推定的蛋白质复合物中的大多数与核心生物学过程相关,并且涵盖候选疾病基因和未注释的蛋白质,以告知机制。令人惊讶的是,虽然较大的多蛋白装配体往往被更广泛地注释和进化上保守,但是具有五个或更少亚基的人蛋白质复合物却在功能上没有注释或仅限于脊椎动物,这表明了更多的近期功能创新。

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