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ABCF ATPases Involved in Protein Synthesis Ribosome Assembly and Antibiotic Resistance: Structural and Functional Diversification across the Tree of Life

机译:ABCF ATPase参与蛋白质合成核糖体组装和抗生素抗性:生命之树上的结构和功能多样化

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摘要

Within the larger ABC superfamily of ATPases, ABCF family members eEF3 in Saccharomyces cerevisiae and EttA in Escherichia coli have been found to function as ribosomal translation factors. Several other ABCFs including biochemically characterized VgaA, LsaA and MsrE confer resistance to antibiotics that target the peptidyl transferase center and exit tunnel of the ribosome. However, the diversity of ABCF subfamilies, the relationships among subfamilies and the evolution of antibiotic resistance (ARE) factors from other ABCFs have not been explored. To address this, we analyzed the presence of ABCFs and their domain architectures in 4505 genomes across the tree of life. We find 45 distinct subfamilies of ABCFs that are widespread across bacterial and eukaryotic phyla, suggesting that they were present in the last common ancestor of both. Surprisingly, currently known ARE ABCFs are not confined to a distinct lineage of the ABCF family tree, suggesting that ARE can readily evolve from other ABCF functions. Our data suggest that there are a number of previously unidentified ARE ABCFs in antibiotic producers and important human pathogens. We also find that ATPase-deficient mutants of all four E. coli ABCFs (EttA, YbiT, YheS and Uup) inhibit protein synthesis, indicative of their ribosomal function, and demonstrate a genetic interaction of ABCFs Uup and YheS with translational GTPase BipA involved in assembly of the 50S ribosome subunit. Finally, we show that the ribosome-binding resistance factor VmlR from Bacillus subtilis is localized to the cytoplasm, ruling out a role in antibiotic efflux.
机译:在较大的ABC ATP酶超家族中,酿酒酵母中的ABCF家族成员eEF3和大肠杆菌中的EttA被用作核糖体翻译因子。包括生化表征的VgaA,LsaA和MsrE在内的其他几种ABCF赋予了针对以肽基转移酶中心和核糖体出口通道为目标的抗生素的抗药性。然而,尚未探索ABCF亚家族的多样性,亚家族之间的关系以及其他ABCF的抗生素抗性(ARE)因子的演变。为了解决这个问题,我们分析了生命之树中4505个基因组中ABCF的存在及其域结构。我们发现ABCFs的45个不同的亚家族遍布细菌和真核生物门,表明它们存在于两者的最后共同祖先中。出人意料的是,当前已知的ARE ABCF并不局限于ABCF家族树的独特谱系,这表明ARE可以很容易地从其他ABCF功能演变而来。我们的数据表明,在抗生素生产商和重要的人类病原体中,存在许多以前未被确认的ARE ABCF。我们还发现所有四个大肠杆​​菌ABCF(EttA,YbiT,YheS和Uup)的ATPase缺陷型突变体均抑制蛋白质合成,表明其核糖体功能,并证明ABCF Uup和YheS与参与翻译的GTPase BipA的遗传相互作用50S核糖体亚基的组装。最后,我们显示了来自枯草芽孢杆菌的核糖体结合抗性因子VmlR定位于细胞质,排除了抗生素外排的作用。

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