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Integrative structural analysis of the UTPB complex, an early assembly factor for eukaryotic small ribosomal subunits

机译:UTPB复合物的整合结构分析,这是真核小核糖体亚基的早期组装因子

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Ribosome assembly is an essential and conserved cellular process in eukaryotes that requires numerous assembly factors. The six-subunit UTPB complex is an essential component of the 90S precursor of the small ribosomal subunit. Here, we analyzed the molecular architecture of UTPB using an integrative structural biology approach. We mapped the major interactions that associate each of six UTPB proteins. Crystallographic studies showed that Utp1, Utp21, Utp12 and Utp13 are evolutionarily related and form a dimer of dimers (Utp1-Utp21, Utp12-Utp13) through their homologous helical C-terminal domains. Molecular docking with crosslinking restraints showed that the WD domains of Utp12 and Utp13 are associated, as are the WD domains of Utp1, Utp21 and Utp18. Electron microscopy images of the entire UTPB complex revealed that it predominantly adopts elongated conformations and possesses internal flexibility. We also determined crystal structures of the WD domain of Utp18 and the HAT and deviant HAT domains of Utp6. A structural model of UTPB was derived based on these data.
机译:核糖体组装是真核生物中必需且保守的细胞过程,需要大量的组装因子。六亚基UTPB复合物是小核糖体亚基90S前体的重要组成部分。在这里,我们使用整合结构生物学方法分析了UTPB的分子结构。我们绘制了与六个UTPB蛋白相关的主要相互作用。晶体学研究表明,Utp1,Utp21,Utp12和Utp13具有进化相关性,并通过其同源的螺旋C末端结构域形成二聚体的二聚体(Utp1-Utp21,Utp12-Utp13)。具有交联限制的分子对接表明,Utp12和Utp13的WD域是相关的,Utp1,Utp21和Utp18的WD域也是如此。整个UTPB复合物的电子显微镜图像显示,它主要采用细长的构象并具有内部柔韧性。我们还确定了Utp18的WD结构域以及Utp6的HAT和异常HAT结构域的晶体结构。基于这些数据,得出了UTPB的结构模型。

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