A small region of the dengue virus-encoded RNA-dependent RNA polymerase, NS5, confers interaction with both the nuclear transport receptor importin-beta and the viral helicase, NS3.

Magnus Johansson, Andrew J. Brooks, D. A. Jans, Subhash G. Vasudevan
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引用次数: 173

Abstract

The dengue virus RNA-dependent RNA polymerase, NS5, and the protease/helicase, NS3, are multidomain proteins that have been shown to interact both in vivo and in vitro. A hyperphosphorylated form of NS5 that does not interact with NS3 has been detected in the nuclei of virus-infected cells, presumably as the result of the action of a functional nuclear localization sequence within the interdomain region of NS5 (residues 369-405). In this study, it is shown by using the yeast two-hybrid system that the C-terminal region of NS3 (residues 303-618) interacts with the N-terminal region of NS5 (residues 320-368). Further, it is shown that this same region of NS5 is also recognized by the cellular nuclear import receptor importin-beta. The interaction between NS5 and importin-beta and competition by NS3 with the latter for the same binding site on NS5 were confirmed by pull-down assays. The direct interaction of importin-beta with NS5 has implications for the mechanism by which this normally cytoplasmic protein may be targetted to the nucleus.
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登革热病毒编码的RNA依赖RNA聚合酶NS5的一个小区域可以与核转运受体importin- β和病毒解旋酶NS3相互作用。
登革病毒RNA依赖的RNA聚合酶NS5和蛋白酶/解旋酶NS3是多结构域蛋白,已被证明在体内和体外都能相互作用。在病毒感染细胞的细胞核中检测到NS5的一种不与NS3相互作用的过度磷酸化形式,可能是由于NS5结构域间区域内的功能性核定位序列的作用(残基369-405)。本研究利用酵母双杂交系统发现,NS3的c端区域(残基303-618)与NS5的n端区域(残基320-368)相互作用。此外,研究表明NS5的同一区域也被细胞核输入受体importin- β识别。下拉实验证实了NS5与importin-beta的相互作用以及NS3与后者竞争NS5上的相同结合位点。importin- β与NS5的直接相互作用暗示了这种通常的细胞质蛋白可能靶向细胞核的机制。
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