首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Conserved GTPase LepA (Elongation Factor 4) functions in biogenesis of the 30S subunit of the 70S ribosome
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Conserved GTPase LepA (Elongation Factor 4) functions in biogenesis of the 30S subunit of the 70S ribosome

机译:保守的GTPase LepA(延伸因子4)在70S核糖体30S亚基的生物发生中起作用

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摘要

The physiological role of LepA, a paralog of EF-G found in all bacteria, has been a mystery for decades. Here, we show that LepA functions in ribosome biogenesis. In cells lacking LepA, immature 30S particles accumulate. Four proteins are specifically underrepresented in these particles—S3, S10, S14, and S21—all of which bind late in the assembly process and contribute to the folding of the 3′ domain of 16S rRNA. Processing of 16S rRNA is also delayed in the mutant strain, as indicated by increased levels of precursor 17S rRNA in assembly intermediates. Mutation ΔlepA confers a synthetic growth phenotype in absence of RsgA, another GTPase, well known to act in 30S subunit assembly. Analysis of the ΔrsgA strain reveals accumulation of intermediates that resemble those seen in the absence of LepA. These data suggest that RsgA and LepA play partially redundant roles to ensure efficient 30S assembly.
机译:数十年来,在所有细菌中发现的EF-G旁系同源物LepA的生理作用一直是个谜。在这里,我们显示LepA在核糖体生物发生中起作用。在缺乏LepA的细胞中,未成熟的30S颗粒会积聚。在这些颗粒中,S3,S10,S14和S21这四个蛋白的表达特别不足,它们全部在组装过程后期结合,并有助于16S rRNA 3'结构域的折叠。突变菌株中16S rRNA的加工也被延迟,如装配中间体中前体17S rRNA水平的提高所表明的。突变ΔlepA在不存在另一种GTP酶RsgA的情况下赋予了合成的生长表型,众所周知,RsgA在30S亚基装配中起作用。 ΔrsgA菌株的分析表明,中间体的积累类似于在没有LepA的情况下所见的中间体。这些数据表明,RsgA和LepA发挥了部分冗余作用,以确保有效的30S组装。

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