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Reconstitution of HIV-1 Rev nuclear export: Independent requirements for nuclear import and export

机译:重组HIV-1 Rev核出口:核进出口的独立要求

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摘要

The Rev protein of HIV-1 actively shuttles between nucleus and cytoplasm and mediates the export of unspliced retroviral RNAs. The localization of shuttling proteins such as Rev is controlled by the relative rates of nuclear import and export. To study nuclear export in isolation, we generated cell lines expressing a green fluorescent protein-labeled chimeric protein consisting of HIV-1 Rev and a hormone-inducible nuclear localization sequence. Steroid removal switches off import thus allowing direct visualization of the Rev export pathway in living cells. After digitonin permeabilization of these cells, we found that a functional nuclear export sequence (NES), ATP, and fractionated cytosol were sufficient for nuclear export in vitro. Nuclear pore-specific lectins and leptomycin B were potent export inhibitors. Nuclear export was not inhibited by antagonists of calcium metabolism that block nuclear import. These data further suggest that nuclear pores do not functionally close when luminal calcium stores are depleted. The distinct requirements for nuclear import and export argue that these competing processes may be regulated independently. This system should have wide applicability for the analysis of nuclear import and export.
机译:HIV-1的Rev蛋白在核和细胞质之间活跃穿梭,并介导未剪接的逆转录病毒RNA的输出。诸如Rev的穿梭蛋白的定位受核进出口的相对速率控制。为了单独研究核输出,我们生成了表达绿色荧光蛋白标记的嵌合蛋白的细胞系,该蛋白由HIV-1 Rev和激素诱导的核定位序列组成。去除类固醇会关闭导入,从而可以直接观察活细胞中的Rev导出途径。洋地黄皂苷透化这些细胞后,我们发现功能性核输出序列(NES),ATP和分离的细胞质足以在体外进行核输出。核孔特异性凝集素和瘦霉素B是有效的出口抑制剂。阻止核输入的钙代谢拮抗剂不会抑制核输出。这些数据进一步表明,当腔内钙存储减少时,核孔不会在功能上关闭。对核进出口的不同要求认为,这些相互竞争的过程可能受到独立监管。该系统应在核进出口分析中具有广泛的适用性。

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