首页> 外文期刊>Journal of Molecular Biology >Distinct regions of human eIF3 are sufficient for binding to the HCV IRES and the 40S ribosomal subunit.
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Distinct regions of human eIF3 are sufficient for binding to the HCV IRES and the 40S ribosomal subunit.

机译:人eIF3的不同区域足以结合HCV IRES和40S核糖体亚基。

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摘要

Translation of the hepatitis C virus (HCV) genomic RNA initiates from an internal ribosome entry site (IRES) in its 5' untranslated region and requires a minimal subset of translation initiation factors to occur, namely eukaryotic initiation factor (eIF) 2 and eIF3. Low-resolution structural information has revealed how the HCV IRES RNA binds human eIF3 and the 40S ribosomal subunit and positions the start codon for initiation. However, the exact nature of the interactions between the HCV IRES RNA and the translational machinery remains unknown. Using limited proteolysis and mass spectrometry, we show that distinct regions of human eIF3 are sufficient for binding to the HCV IRES RNA and the 40S subunit. Notably, the eIF3 subunit eIF3b is protected by HCV IRES RNA binding, yet is exposed in the complex when compared to subunits eIF3e, eIF3f, eIF3h, and eIF3l. Limited proteolysis reveals that eIF3 binding to the 40S ribosomal subunit occurs through many redundant interactions that can compensate for each other. These data suggest how the HCV IRES binds to specific regions of eIF3 to target the translational machinery to the viral genomic RNA and provide a framework for modeling the architecture of intact human eIF3.
机译:丙型肝炎病毒(HCV)基因组RNA的翻译从其5'非翻译区内的内部核糖体进入位点(IRES)开始,并且需要翻译启动因子(即真核启动因子(eIF)2和eIF3)的最小子集出现。低分辨率的结构信息表明,HCV IRES RNA如何结合人eIF3和40S核糖体亚基并定位起始密码子以进行起始。但是,HCV IRES RNA与翻译机制之间相互作用的确切性质仍然未知。使用有限的蛋白水解和质谱,我们显示出人类eIF3的不同区域足以结合HCV IRES RNA和40S亚基。值得注意的是,与亚基eIF3e,eIF3f,eIF3h和eIF31相比,eIF3亚基eIF3b受HCV IRES RNA结合保护,但暴露于复合物中。有限的蛋白水解揭示eIF3与40S核糖体亚基的结合是通过许多可以相互补偿的冗余相互作用发生的。这些数据表明,HCV IRES如何与eIF3的特定区域结合,以将翻译机制靶向病毒基因组RNA,并为建模完整的人类eIF3的体系结构提供了框架。

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