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Identification of a Hydrophobic Domain of HA2 Essential to Morphogenesis of Helicoverpa armigera Nucleopolyhedrovirus▿

机译:棉铃虫核型多角体病毒的形态发生必不可少的HA2疏水域的鉴定▿

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摘要

The HA2 protein of the Helicoverpa armigera single-nucleocapsid nucleopolyhedrovirus (HearNPV) is a WASP homology protein capable of nucleating branched actin filaments in the presence of the Arp2/3 complex in vitro. To determine the role of ha2 in the HearNPV life cycle, ha2 knockout and ha2 repair bacmids were constructed. Transfection and infection analysis demonstrated that the ha2 null bacmid was unable to produce infectious budded virus (BV), while the repair bacmid rescued the defect. In vitro analysis demonstrated that the WCA domain of HA2 accelerates Arp2/3-mediated actin assembly and is indispensable to the function of HA2. However, analysis of the repaired recombinant with a series of truncated ha2 mutants demonstrated that the WCA domain was essential but not enough to yield infectious virions, and a hydrophobic domain (H domain) consisting of amino acids (aa) 167 to 193 played a pivotal role in the production of BV. Subcellular localization analysis with enhanced green fluorescent protein fusions showed that the H domain functioned as a nuclear localization signal. In addition, deletion of the C terminus of the ha2 product, a phosphatidylinositol 4-kinase homolog, dramatically decreased the viral titer, while deletion of 128 aa from the N terminus did not affect HA2 function.
机译:棉铃虫单核衣壳核多角体病毒(HearNPV)的HA2蛋白是一种WASP同源蛋白,能够在体外存在Arp2 / 3复合物的情况下使分支的肌动蛋白细丝成核。为了确定ha2在HearNPV生命周期中的作用,构建了ha2敲除和ha2修复杆粒。转染和感染分析表明,ha2无效杆状病毒不能产生传染性芽生病毒(BV),而修复杆状病毒可以挽救该缺陷。体外分析表明,HA2的WCA结构域可加速Arp2 / 3介导的肌动蛋白组装,并且对HA2的功能必不可少。但是,用一系列截短的ha2突变体对修复的重组体进行的分析表明,WCA结构域是必不可少的,但不足以产生感染性病毒体,而由氨基酸(aa)167至193组成的疏水结构域(H结构域)发挥了关键作用在BV生产中的作用。用增强的绿色荧光蛋白融合物进行的亚细胞定位分析表明,H结构域起着核定位信号的作用。此外,删除ha2产物的C末端(磷脂酰肌醇4激酶同源物)可显着降低病毒滴度,而从N末端删除128个氨基酸不会影响HA2的功能。

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