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Understanding ribosome assembly: the structure of in vivo assembled immature 30S subunits revealed by cryo-electron microscopy.

机译:了解核糖体组装:通过冷冻电子显微镜揭示的体内组装的不成熟30S亚基的结构。

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Four decades after early in vitro assembly studies demonstrated that ribosome assembly is a controlled process, our understanding of ribosome assembly is still incomplete. Just as structure determination has been so important to understanding ribosome function, so too will it be critical to sorting out the assembly process. Here, we used a viable deletion in the yjeQ gene, a recognized ribosome assembly factor, to isolate and structurally characterize immature 30S subunits assembled in vivo. These small ribosome subunits contained unprocessed 17S rRNA and lacked some late ribosomal proteins. Cryo-electron microscopy reconstructions revealed that the presence of precursor sequences in the rRNA induces a severe distortion in the 3' minor domain of the subunit involved in the decoding of mRNA and interaction with the large ribosome subunit. These findings suggest that rRNA processing events induce key local conformational changes directing the structure toward the mature assembly. We concluded that rRNA processing, folding, and the entry of tertiary r-proteins are interdependent events in the late stages of 30S subunit assembly. In addition, we demonstrate how studies of emerging assembly factors in ribosome biogenesis can help to elucidate the path of subunit assembly in vivo.
机译:在早期的体外组装研究表明核糖体组装是一个受控过程的四十年后,我们对核糖体组装的了解仍然不完整。正如结构确定对于理解核糖体功能非常重要一样,对整理组装过程也至关重要。在这里,我们使用了公认的核糖体装配因子yjeQ基因中的可行缺失,以分离并在结构上表征体内装配的未成熟30S亚基。这些小的核糖体亚基包含未加工的17S rRNA,并且缺少一些晚期核糖体蛋白。低温电子显微镜重建表明,rRNA中前体序列的存在会导致亚单位的3'微小结构域的严重畸变,而该亚单位涉及mRNA的解码以及与大核糖体亚单位的相互作用。这些发现表明,rRNA加工事件诱导了关键的局部构象变化,从而将结构导向成熟的装配体。我们得出的结论是,rRNA加工,折叠和三级r蛋白的进入是30S亚基组装后期的相互依赖事件。另外,我们证明了核糖体生物发生中新兴装配因子的研究如何有助于阐明体内亚基装配的途径。

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