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An Interbacterial NAD(P)(+) Glycohydrolase Toxin Requires Elongation Factor Tu for Delivery to Target Cells

机译:细菌间NAD(P)(+)乙醇水解酶毒素需要传递给靶细胞的延伸因子Tu

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摘要

Type VI secretion (T6S) influences the composition of microbial communities by catalyzing the delivery of toxins between adjacent bacterial cells. Here, we demonstrate that a T6S integral membrane toxin from Pseudomonas aeruginosa, Tse6, acts on target cells by degrading the universally essential dinucleotides NAD(+) and NADP(+). Structural analyses of Tse6 show that it resembles mono-ADP-ribosyltransferase proteins, such as diphtheria toxin, with the exception of a unique loop that both excludes proteinaceous ADP-ribose acceptors and contributes to hydrolysis. We find that entry of Tse6 into target cells requires its binding to an essential housekeeping protein, translation elongation factor Tu (EF-Tu). These proteins participate in a larger assembly that additionally directs toxin export and provides chaperone activity. Visualization of this complex by electron microscopy defines the architecture of a toxin-loaded T6S apparatus and provides mechanistic insight into intercellular membrane protein delivery between bacteria.
机译:VI型分泌(T6S)通过催化相邻细菌细胞之间的毒素传递来影响微生物群落的组成。在这里,我们证明铜绿假单胞菌Tse6的T6S整体膜毒素通过降解普遍必需的二核苷酸NAD(+)和NADP(+)作用于靶细胞。 Tse6的结构分析表明,它类似于单ADP-核糖基转移酶蛋白(例如白喉毒素),唯一的环除外,该环既排除了蛋白质的ADP-核糖受体,又有助于水解。我们发现,Tse6进入靶细胞需要结合至必需的管家蛋白翻译延伸因子Tu(EF-Tu)。这些蛋白质参与更大的装配,该装配另外指导毒素输出并提供伴侣活性。通过电子显微镜对该复合物的可视化定义了载有毒素的T6S仪器的体系结构,并提供了对细菌之间细胞间膜蛋白递送的机理的了解。

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