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确定锥虫前核糖体复合物中的RNA-蛋白质相互作用。

Defining the RNA-protein interactions in the trypanosome preribosomal complex.

作者信息

Wang Lei, Ciganda Martin, Williams Noreen

机构信息

Department of Microbiology and Immunology and Witebsky Center for Microbial Pathogenesis and Immunology, University at Buffalo, Buffalo, New York, USA.

出版信息

Eukaryot Cell. 2013 Apr;12(4):559-66. doi: 10.1128/EC.00004-13. Epub 2013 Feb 8.

Abstract

In eukaryotes, 5S rRNA is transcribed in the nucleoplasm and requires the ribosomal protein L5 to deliver it to the nucleolus for ribosomal assembly. The trypanosome-specific proteins P34 and P37 form a novel preribosomal complex with the eukaryotic conserved L5-5S rRNA complex in the nucleoplasm. Previous results suggested that P34 acts together with L5 to bridge the interaction with 5S rRNA and thus to stabilize 5S rRNA, an important role in the early steps of ribosomal biogenesis. Here, we have delineated the domains of the two protein components, L5 and P34, and regions of the RNA partner, 5S rRNA, that are critical for protein-RNA interactions within the complex. We found that the L18 domain of L5 and the N terminus and RNA recognition motif of P34 bind 5S rRNA. We showed that Trypanosoma brucei L5 binds the β arm of 5S rRNA, while P34 binds loop A/stem V of 5S rRNA. We demonstrated that 5S rRNA is able to enhance the association between the protein components of the complex, L5 and P34. Both loop A/stem V and the β arm of 5S rRNA can separately enhance the protein-protein association, but their effects are neither additive nor synergistic. Domains in the two proteins for protein-protein and protein-RNA interactions overlap or are close to each other. This suggests that 5S rRNA binding might cause conformational changes in L5 and P34 and might also bridge the interactions, thus enhancing binding between the protein partners of this novel complex.

摘要

在真核生物中,5S核糖体RNA在核质中被转录,并且需要核糖体蛋白L5将其转运到核仁中进行核糖体组装。锥虫特异性蛋白P34和P37在核质中与真核生物保守的L5-5S核糖体RNA复合物形成一种新型的前核糖体复合物。先前的结果表明,P34与L5共同作用,以桥接与5S核糖体RNA的相互作用,从而稳定5S核糖体RNA,这在核糖体生物发生的早期步骤中起着重要作用。在这里,我们已经描绘了两种蛋白质成分L5和P34的结构域,以及RNA伴侣5S核糖体RNA的区域,这些对于复合物中的蛋白质-RNA相互作用至关重要。我们发现L5的L18结构域以及P34的N末端和RNA识别基序与5S核糖体RNA结合。我们表明,布氏锥虫L5与5S核糖体RNA的β臂结合,而P34与5S核糖体RNA的环A/茎V结合。我们证明5S核糖体RNA能够增强复合物的蛋白质成分L5和P34之间的结合。5S核糖体RNA的环A/茎V和β臂都可以分别增强蛋白质-蛋白质结合,但它们的作用既不是相加的也不是协同的。两种蛋白质中用于蛋白质-蛋白质和蛋白质-RNA相互作用的结构域相互重叠或彼此靠近。这表明5S核糖体RNA结合可能会导致L5和P34的构象变化,也可能桥接相互作用,从而增强这种新型复合物的蛋白质伴侣之间的结合。

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本文引用的文献

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