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单分子研究揭示 DEAD 盒蛋白 DDX1 促进 HIV-1 Rev 在 Rev 反应元件上的寡聚化。

Single-molecule studies reveal that DEAD box protein DDX1 promotes oligomerization of HIV-1 Rev on the Rev response element.

机构信息

Department of Molecular Biology, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, CA 92037, USA.

出版信息

J Mol Biol. 2011 Jul 29;410(5):959-71. doi: 10.1016/j.jmb.2011.04.026.

Abstract

Oligomeric assembly of Rev on the Rev response element (RRE) is essential for the nuclear export of unspliced and singly spliced human immunodeficiency virus type 1 viral mRNA transcripts. Several host factors, including the human DEAD box protein DDX1, are also known to be required for efficient Rev function. In this study, spontaneous assembly and dissociation of individual Rev-RRE complexes in the presence or absence of DDX1 were observed in real time via single-molecule total internal reflection fluorescence microscopy. Binding of up to eight fluorescently labeled Rev monomers to a single RRE molecule was visualized, and the event frequencies and corresponding binding and dissociation rates for the different Rev-RRE stoichiometries were determined. The presence of DDX1 eliminated a second kinetic phase present during the initial Rev binding step, attributed to nonproductive nucleation events, resulting in increased occurrence of higher-order Rev-RRE stoichiometries. This effect was further enhanced upon the addition of a non-hydrolyzable ATP analog (adenylyl-imidophosphate), whereas ADP had no effect beyond that of DDX1 alone. Notably, the first three Rev monomer binding events were accelerated in the presence of DDX1 and adenylyl-imidophosphate, while the dissociation rates remained unchanged. Measurements performed across a range of DDX1 concentrations suggest that DDX1 targets Rev rather than the RRE to promote oligomeric assembly. Moreover, DDX1 is able to restore the oligomerization activity of a Rev mutant that is otherwise unable to assemble on the RRE beyond a monomeric complex. Taken together, these results suggest that DDX1 acts as a cellular cofactor by promoting oligomerization of Rev on the RRE.

摘要

寡聚体装配的 Rev 反应元件(RRE)是必不可少的核出口未剪接和单剪接人类免疫缺陷病毒 1 型病毒 mRNA 转录本。几个宿主因子,包括人类 DEAD 盒蛋白 DDX1,也被认为是有效的 Rev 功能所必需的。在这项研究中,通过单分子全内反射荧光显微镜实时观察到在存在或不存在 DDX1 的情况下,单个 Rev-RRE 复合物的自发组装和解离。多达 8 个荧光标记的 Rev 单体结合到单个 RRE 分子上,并且确定了不同 Rev-RRE 化学计量的事件频率以及相应的结合和解离速率。DDX1 的存在消除了在初始 Rev 结合步骤中存在的第二个动力学相,归因于非生产性成核事件,导致更高阶的 Rev-RRE 化学计量的发生增加。在添加非水解的 ATP 类似物(腺苷酰亚胺磷酸)时,这种效果进一步增强,而 ADP 除了 DDX1 之外没有任何影响。值得注意的是,在 DDX1 和腺苷酰亚胺磷酸存在的情况下,前三个 Rev 单体结合事件被加速,而解离速率保持不变。在一系列 DDX1 浓度下进行的测量表明,DDX1 靶向 Rev 而不是 RRE 以促进寡聚体装配。此外,DDX1 能够恢复否则无法在 RRE 上组装超过单体复合物的 Rev 突变体的寡聚化活性。总之,这些结果表明,DDX1 作为一种细胞辅助因子,通过促进 Rev 在 RRE 上的寡聚化来发挥作用。

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