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HIV-1 Rev protein assembles on viral RNA one molecule at a time

机译:HIV-1 Rev蛋白一次在一个分子上组装在病毒RNA上

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摘要

Oligomerization of the HIV-1 protein Rev on the Rev Response Element (RRE) regulates nuclear export of genomic viral RNA and partially spliced viral mRNAs encoding for structural proteins. Single-molecule fluorescence spectroscopy has been used to dissect the multistep assembly pathway of this essential ribonucleoprotein, revealing dynamic intermediates and the mechanism of assembly. Assembly is initiated by binding of Rev to a high-affinity site in stem-loop IIB of the RRE and proceeds rapidly by addition of single Rev monomers, facilitated by cooperative Rev-Rev interactions on the RRE. Dwell-time analysis of fluorescence trajectories recorded during individual Rev-RRE assembly reactions has revealed the microscopic rate constants for several of the Rev monomer binding and dissociation steps. The high-affinity binding of multiple Rev monomers to the RRE is achieved on a much faster timescale than reported in previous bulk kinetic studies of Rev-RRE association, indicating that oligomerization is an early step in complex assembly.
机译:HIV-1蛋白Rev在Rev反应元件(RRE)上的寡聚化调节基因组病毒RNA和编码结构蛋白的部分剪接病毒mRNA的核输出。单分子荧光光谱法已被用来解剖这种基本核糖核蛋白的多步组装途径,揭示了动态中间体和组装机制。通过将Rev结合到RRE的茎环IIB中的高亲和力位点来启动组装,并通过添加单个Rev单体迅速进行,并通过RRE上的协作Rev-Rev相互作用促进组装。在各个Rev-RRE组装反应过程中记录的荧光轨迹的停留时间分析揭示了几个Rev单体结合和解离步骤的微观速率常数。与以前的Rev-RRE缔合动力学研究中报道的结果相比,多种Rev单体与RRE的高亲和力结合要快得多,这表明低聚是复杂组装的早期步骤。

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