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包含大肠杆菌中保守且必需蛋白质复合物的相互作用网络。

Interaction network containing conserved and essential protein complexes in Escherichia coli.

作者信息

Butland Gareth, Peregrín-Alvarez José Manuel, Li Joyce, Yang Wehong, Yang Xiaochun, Canadien Veronica, Starostine Andrei, Richards Dawn, Beattie Bryan, Krogan Nevan, Davey Michael, Parkinson John, Greenblatt Jack, Emili Andrew

机构信息

Banting and Best Department of Medical Research, University of Toronto, 112 College Street, Toronto, Ontario M5G 1L6, Canada.

出版信息

Nature. 2005 Feb 3;433(7025):531-7. doi: 10.1038/nature03239.

Abstract

Proteins often function as components of multi-subunit complexes. Despite its long history as a model organism, no large-scale analysis of protein complexes in Escherichia coli has yet been reported. To this end, we have targeted DNA cassettes into the E. coli chromosome to create carboxy-terminal, affinity-tagged alleles of 1,000 open reading frames (approximately 23% of the genome). A total of 857 proteins, including 198 of the most highly conserved, soluble non-ribosomal proteins essential in at least one bacterial species, were tagged successfully, whereas 648 could be purified to homogeneity and their interacting protein partners identified by mass spectrometry. An interaction network of protein complexes involved in diverse biological processes was uncovered and validated by sequential rounds of tagging and purification. This network includes many new interactions as well as interactions predicted based solely on genomic inference or limited phenotypic data. This study provides insight into the function of previously uncharacterized bacterial proteins and the overall topology of a microbial interaction network, the core components of which are broadly conserved across Prokaryota.

摘要

蛋白质通常作为多亚基复合物的组成部分发挥功能。尽管大肠杆菌作为模式生物已有很长历史,但尚未有关于其蛋白质复合物的大规模分析报道。为此,我们将DNA盒靶向导入大肠杆菌染色体,以创建1000个开放阅读框(约占基因组的23%)的羧基末端、带有亲和标签的等位基因。总共成功标记了857种蛋白质,其中包括198种在至少一种细菌物种中必不可少的高度保守的可溶性非核糖体蛋白质,而648种蛋白质可纯化至均一状态,并通过质谱鉴定其相互作用的蛋白质伙伴。通过连续几轮的标记和纯化,揭示并验证了涉及多种生物过程的蛋白质复合物相互作用网络。该网络包括许多新的相互作用以及仅基于基因组推断或有限表型数据预测的相互作用。这项研究为先前未表征的细菌蛋白质的功能以及微生物相互作用网络的整体拓扑结构提供了见解,其核心成分在原核生物中广泛保守。

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