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Crystal Structures of the uL3 Mutant Ribosome: Illustration of the Importance of Ribosomal Proteins for Translation Efficiency

机译:uL3突变核糖体的晶体结构:核糖体蛋白对翻译效率的重要性的例证

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摘要

The ribosome has been described as a ribozyme in which ribosomal RNA is responsible for peptidyl-transferase reaction catalysis. The W255C mutation of the universally conserved ribosomal protein uL3 has diverse effects on ribosome function (e.g., increased affinities for transfer RNAs, decreased rates of peptidyl-transfer), and cells harboring this mutation are resistant to peptidyl-transferase inhibitors (e.g., anisomycin). These observations beg the question of how a single amino acid mutation may have such wide ranging consequences. Here, we report the structure of the vacant yeast uL3 W255C mutant ribosome by X-ray crystallography, showing a disruption of the A-site side of the peptidyl-transferase center (PTC). An additional X-ray crystallographic structure of the anisomycin-containing mutant ribosome shows that high concentrations of this inhibitor restore a “WT-like” configuration to this region of the PTC, providing insight into the resistance mechanism of the mutant. Globally, our data demonstrate that ribosomal protein uL3 is structurally essential to ensure an optimal and catalytically efficient organization of the PTC, highlighting the importance of proteins in the RNA-centered ribosome.
机译:核糖体已被描述为一种核酶,其中核糖体RNA负责肽基转移酶反应的催化作用。普遍保守的核糖体蛋白uL3的W255C突变对核糖体功能有多种影响(例如,对转移RNA的亲和力增加,肽基转移率降低),具有该突变的细胞对肽基转移酶抑制剂(如茴香霉素)具有抵抗力。这些观察提出了一个问题,即单个氨基酸突变可能产生如此广泛的影响。在这里,我们通过X射线晶体学报告空酵母uL3 W255C突变核糖体的结构,显示了肽基转移酶中心(PTC)的A位侧的破坏。含有茴香霉素的突变核糖体的其他X射线晶体学结构表明,高浓度的该抑制剂可在PTC的该区域恢复“ WT样”构型,从而深入了解突变体的耐药机制。在全球范围内,我们的数据表明核糖体蛋白uL3在结构上对于确保PTC的最佳和催化高效组织至关重要,突出了蛋白质在以RNA为中心的核糖体中的重要性。

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