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大肠杆菌GTP酶CgtAE参与大型核糖体组装的后期步骤。

The Escherichia coli GTPase CgtAE is involved in late steps of large ribosome assembly.

作者信息

Jiang Mengxi, Datta Kaustuv, Walker Angela, Strahler John, Bagamasbad Pia, Andrews Philip C, Maddock Janine R

机构信息

Department of Molecular, Cellular and Developmental Biology, University of Michigan, 830 North University, Ann Arbor, MI 48109-1048, USA.

出版信息

J Bacteriol. 2006 Oct;188(19):6757-70. doi: 10.1128/JB.00444-06.

Abstract

The bacterial ribosome is an extremely complicated macromolecular complex the in vivo biogenesis of which is poorly understood. Although several bona fide assembly factors have been identified, their precise functions and temporal relationships are not clearly defined. Here we describe the involvement of an Escherichia coli GTPase, CgtA(E), in late steps of large ribosomal subunit biogenesis. CgtA(E) belongs to the Obg/CgtA GTPase subfamily, whose highly conserved members are predominantly involved in ribosome function. Mutations in CgtA(E) cause both polysome and rRNA processing defects; small- and large-subunit precursor rRNAs accumulate in a cgtA(E) mutant. In this study we apply a new semiquantitative proteomic approach to show that CgtA(E) is required for optimal incorporation of certain late-assembly ribosomal proteins into the large ribosomal subunit. Moreover, we demonstrate the interaction with the 50S ribosomal subunits of specific nonribosomal proteins (including heretofore uncharacterized proteins) and define possible temporal relationships between these proteins and CgtA(E). We also show that purified CgtA(E) associates with purified ribosomal particles in the GTP-bound form. Finally, CgtA(E) cofractionates with the mature 50S but not with intermediate particles accumulated in other large ribosome assembly mutants.

摘要

细菌核糖体是一种极其复杂的大分子复合物,其在体内的生物发生过程目前还知之甚少。尽管已经鉴定出了几种真正的组装因子,但其精确功能和时间关系尚未明确界定。在此,我们描述了一种大肠杆菌GTP酶CgtA(E)在核糖体大亚基生物发生后期步骤中的作用。CgtA(E)属于Obg/CgtA GTP酶亚家族,该家族高度保守的成员主要参与核糖体功能。CgtA(E)的突变会导致多聚核糖体和rRNA加工缺陷;小亚基和大亚基前体rRNA在cgtA(E)突变体中积累。在本研究中,我们应用一种新的半定量蛋白质组学方法来表明,CgtA(E)是某些后期组装的核糖体蛋白最佳整合到大核糖体亚基中所必需的。此外,我们证明了特定非核糖体蛋白(包括迄今未鉴定的蛋白)与50S核糖体亚基之间的相互作用,并确定了这些蛋白与CgtA(E)之间可能的时间关系。我们还表明,纯化的CgtA(E)以GTP结合形式与纯化的核糖体颗粒结合。最后,CgtA(E)与成熟的50S核糖体共分离,但不与其他大核糖体组装突变体中积累的中间颗粒共分离。

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