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Triple Gene Block Protein Interactions Involved in Movement of Barley Stripe Mosaic Virus

机译:大麦条纹花叶病毒运动涉及的三重基因块蛋白相互作用。

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摘要

Barley stripe mosaic virus (BSMV) encodes three movement proteins in an overlapping triple gene block (TGB), but little is known about the physical interactions of these proteins. We have characterized a ribonucleoprotein (RNP) complex consisting of the TGB1 protein and plus-sense BSMV RNAs from infected barley plants and have identified TGB1 complexes in planta and in vitro. Homologous TGB1 binding was disrupted by site-specific mutations in each of the first two N-terminal helicase motifs but not by mutations in two C-terminal helicase motifs. The TGB2 and TGB3 proteins were not detected in the RNP, but affinity chromatography and yeast two-hybrid experiments demonstrated that TGB1 binds to TGB3 and that TGB2 and TGB3 form heterologous interactions. These interactions required the TGB2 glycine 40 and the TGB3 isoleucine 108 residues, and BSMV mutants containing these amino acid substitution were unable to move from cell to cell. Infectivity experiments indicated that TGB1 separated on a different genomic RNA from TGB2 and TGB3 could function in limited cell-to-cell movement but that the rates of movement depended on the levels of expression of the proteins and the contexts in which they are expressed. Moreover, elevated expression of the wild-type TGB3 protein interfered with cell-to-cell movement but movement was not affected by the similar expression of a TGB3 mutant that fails to interact with TGB2. These experiments suggest that BSMV movement requires physical interactions of TGB2 and TGB3 and that substantial deviation from the TGB protein ratios expressed by the wild-type virus compromises movement.
机译:大麦条纹花叶病毒(BSMV)在重叠的三重基因区块(TGB)中编码三种运动蛋白,但对这些蛋白的物理相互作用了解甚少。我们已经表征了由感染大麦植物中的TGB1蛋白和正向BSMV RNA组成的核糖核蛋白(RNP)复合物,并在植物体内和体外鉴定了TGB1复合物。同源的TGB1结合被前两个N末端解旋酶基序中的每一个的位点特异性突变破坏,但未被两个C末端解旋酶基序的突变破坏。在RNP中未检测到TGB2和TGB3蛋白,但是亲和色谱和酵母双杂交实验表明TGB1与TGB3结合,并且TGB2和TGB3形成异源相互作用。这些相互作用需要TGB2甘氨酸40和TGB3异亮氨酸108残基,并且包含这些氨基酸取代的BSMV突变体无法在细胞间移动。感染性实验表明,在与TGB2和TGB3不同的基因组RNA上分离的TGB1可以在有限的细胞间运动中发挥作用,但运动速率取决于蛋白质的表达水平和表达背景。此外,野生型TGB3蛋白的表达升高会干扰细胞间的运动,但运动不会受到无法与TGB2相互作用的TGB3突变体相似表达的影响。这些实验表明,BSMV运动需要TGB2和TGB3的物理相互作用,并且与野生型病毒表达的TGB蛋白比率的实质性偏差会损害运动。

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