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Crystal structure of the transfer-RNA domain of transfer-messenger RNA in complex with SmpB

机译:与SmpB复合的传递信使RNA的transfer-RNA结构域的晶体结构

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Accurate translation of genetic information into protein sequence depends on complete messenger RNA molecules. Truncated mRNAs cause synthesis of defective proteins, and arrest ribosomes at the end of their incomplete message. In bacteria, a hybrid RNA molecule that combines the functions of both transfer and messenger RNAs (called tmRNA) rescues stalled ribosomes, and targets aberrant, partially synthesized, proteins for proteolytic degradation. Here we report the 3.2-A-resol-ution structure of the tRNA-like domain of tmRNA (tmRNA_Δ) in complex with small protein B (SmpB), a protein essential for biological functions of tmRNA. We find that the flexible RNA molecule adopts an open L-shaped conformation and SmpB binds to its elbow region, stabilizing the single-stranded D-loop in an extended conformation. The most striking feature of the structure of tmRNA_Δ is a 90° rotation of the TΨC-arm around the helical axis. Owing to this unusual conformation, the SmpB-tmRNA_Δ complex positioned into the A-site of the ribosome orients SmpB towards the small ribosomal subunit, and directs tmRNA towards the elongation-factor binding region of the ribosome. On the basis of this structure, we propose a model for the binding of tmRNA on the ribosome.
机译:将遗传信息准确翻译成蛋白质序列取决于完整的信使RNA分子。截短的mRNA会导致缺陷蛋白的合成,并在不完整信息的末尾阻止核糖体。在细菌中,结合了转移RNA和信使RNA(称为tmRNA)功能的杂合RNA分子可以拯救失速的核糖体,并靶向部分合成的异常蛋白进行蛋白水解降解。在这里,我们报告了与小蛋白B(SmpB)结合的tmRNA的tRNA样结构域(tmRNA_Δ)的3.2-A-拆分结构,该蛋白对tmRNA的生物学功能至关重要。我们发现,柔性RNA分子采用开放的L形构象,SmpB结合到其肘部区域,稳定了扩展构象中的单链D环。 tmRNA_Δ结构的最显着特征是TΨC臂绕螺旋轴旋转90°。由于这种不寻常的构象,位于核糖体A位点的SmpB-tmRNA_Δ复合物使SmpB朝向小的核糖体亚基,并将tmRNA引向核糖体的延伸因子结合区。在此结构的基础上,我们提出了tmRNA与核糖体结合的模型。

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