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Functional Maps of Protein Complexes from Quantitative Genetic Interaction Data

机译:来自定量遗传相互作用数据的蛋白质复合物功能图

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摘要

Recently, a number of advanced screening technologies have allowed for the comprehensive quantification of aggravating and alleviating genetic interactions among gene pairs. In parallel, TAP-MS studies (tandem affinity purification followed by mass spectroscopy) have been successful at identifying physical protein interactions that can indicate proteins participating in the same molecular complex. Here, we propose a method for the joint learning of protein complexes and their functional relationships by integration of quantitative genetic interactions and TAP-MS data. Using 3 independent benchmark datasets, we demonstrate that this method is >50% more accurate at identifying functionally related protein pairs than previous approaches. Application to genes involved in yeast chromosome organization identifies a functional map of 91 multimeric complexes, a number of which are novel or have been substantially expanded by addition of new subunits. Interestingly, we find that complexes that are enriched for aggravating genetic interactions (i.e., synthetic lethality) are more likely to contain essential genes, linking each of these interactions to an underlying mechanism. These results demonstrate the importance of both large-scale genetic and physical interaction data in mapping pathway architecture and function.
机译:近来,许多先进的筛选技术已经允许对加重和减轻基因对之间的遗传相互作用进行全面定量。同时,TAP-MS研究(先进行串联亲和纯化,然后进行质谱分析)已成功鉴定出物理蛋白质相互作用,该相互作用可表明蛋白质参与同一分子复合物。在这里,我们提出了一种通过定量遗传相互作用和TAP-MS数据的整合来联合学习蛋白质复合物及其功能关系的方法。使用3个独立的基准数据集,我们证明了该方法比以前的方法在识别功能相关蛋白对方面的准确性高出50%。对涉及酵母染色体组织的基因的应用鉴定了91个多聚体复合物的功能图谱,其中许多是新颖的或已通过添加新的亚基而得到实质性扩展。有趣的是,我们发现为加剧遗传相互作用(即合成致死性)而富集的复合物更有可能包含必不可少的基因,并将这些相互作用中的每一个与潜在机制联系起来。这些结果证明了大规模遗传和物理相互作用数据在作图途径结构和功能中的重要性。

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