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Detailed analysis of RNA-protein interactions within the bacterial ribosomal protein L5/5S rRNA complex.

机译:细菌核糖体蛋白L5 / 5S rRNA复合物中RNA-蛋白相互作用的详细分析。

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摘要

The crystal structure of ribosomal protein L5 from Thermus thermophilus complexed with a 34-nt fragment comprising helix III and loop C of Escherichia coli 5S rRNA has been determined at 2.5 A resolution. The protein specifically interacts with the bulged nucleotides at the top of loop C of 5S rRNA. The rRNA and protein contact surfaces are strongly stabilized by intramolecular interactions. Charged and polar atoms forming the network of conserved intermolecular hydrogen bonds are located in two narrow planar parallel layers belonging to the protein and rRNA, respectively. The regions, including these atoms conserved in Bacteria and Archaea, can be considered an RNA-protein recognition module. Comparison of the T. thermophilus L5 structure in the RNA-bound form with the isolated Bacillus stearothermophilus L5 structure shows that the RNA-recognition module on the protein surface does not undergo significant changes upon RNA binding. In the crystal of the complex, the protein interacts with another RNA molecule in the asymmetric unit through the beta-sheet concave surface. This protein/RNA interface simulates the interaction of L5 with 23S rRNA observed in the Haloarcula marismortui 50S ribosomal subunit.
机译:来自嗜热栖热菌的核糖体蛋白L5的晶体结构与包含大肠杆菌5S rRNA的螺旋III和环C的34 nt片段复合,已确定分辨率为2.5A。该蛋白质与5S rRNA环C顶部的突出核苷酸特异性相互作用。 rRNA和蛋白质接触表面通过分子内相互作用而得到高度稳定。形成保守的分子间氢键网络的带电原子和极性原子位于分别属于蛋白质和rRNA的两个狭窄的平面平行层中。该区域,包括细菌和古细菌中保守的这些原子,可以被认为是RNA蛋白质识别模块。 RNA结合形式的嗜热链球菌L5结构与分离的嗜热脂肪芽孢杆菌L5结构的比较表明,蛋白质表面上的RNA识别模块在RNA结合后不会发生显着变化。在复合物的晶体中,蛋白质通过β-折叠凹面与不对称单元中的另一个RNA分子相互作用。这种蛋白质/ RNA界面模拟了在Halolorcula marismortui 50S核糖体亚基中观察到的L5与23S rRNA的相互作用。

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