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Changing patterns of localization of the tobacco mosaic virus movement protein and replicase to the endoplasmic reticulum and microtubules during infection.

机译:感染期间烟草花叶病毒运动蛋白和复制酶定位到内质网和微管的定位模式改变。

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摘要

Tobacco mosaic virus (TMV) derivatives that encode movement protein (MP) as a fusion to the green fluorescent protein (MP:GFP) were used in combination with antibody staining to identify host cell components to which MP and replicase accumulate in cells of infected Nicotiana benthamiana leaves and in infected BY-2 protoplasts. MP:GFP and replicase colocalized to the endoplasmic reticulum (ER; especially the cortical ER) and were present in large, irregularly shaped, ER-derived structures that may represent "viral factories." The ER-derived structures required an intact cytoskeleton, and microtubules appeared to redistribute MP:GFP from these sites during late stages of infection. In leaves, MP:GFP accumulated in plasmodesmata, whereas in protoplasts, the MP:GFP was targeted to distinct, punctate sites near the plasma membrane. Treating protoplasts with cytochalasin D and brefeldin A at the time of inoculation prevented the accumulation of MP:GFP at these sites. It is proposed that the punctate sites anchor the cortical ER to plasma membrane and are related to sites at which plasmodesmata form in walled cells. Hairlike structures containing MP:GFP appeared on the surface of some of the infected protoplasts and are reminiscent of similar structures induced by other plant viruses. We present a model that postulates the role of the ER and cytoskeleton in targeting the MP and viral ribonucleoprotein from sites of virus synthesis to the plasmodesmata through which infection is spread.
机译:编码与绿色荧光蛋白(MP:GFP)融合的运动蛋白(MP)的烟草花叶病毒(TMV)衍生物与抗体染色结合使用,以鉴定感染了烟草的细胞中积累有MP和复制的宿主细胞成分本生叶和感染的BY-2原生质体中。 MP:GFP和复制酶共定位于内质网(ER;尤其是皮质ER),并以大的,不规则形状的,ER衍生的结构存在,可能代表“病毒工厂”。 ER衍生的结构需要完整的细胞骨架,在感染后期,微管似乎会从这些位点重新分布MP:GFP。在叶片中,MP:GFP累积在胞浆中,而在原生质体中,MP:GFP靶向质膜附近不同的点状部位。接种时用细胞松弛素D和布雷菲德菌素A处理原生质体可防止MP:GFP在这些位点积聚。提出的点状部位将皮质内质网锚定在质膜上,并与壁细胞中的胞浆菌形成的部位有关。含有MP:GFP的毛状结构出现在一些被感染的原生质体表面,让人联想到其他植物病毒诱导的相似结构。我们提出了一个模型,该模型推测了ER和细胞骨架在从病毒合成部位到通过感染传播的疟原虫的目标MP和病毒核糖核蛋白中的作用。

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