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首页> 外文期刊>Virology >Plasmodesmal targeting and intercellular movement of potato mop-top pomovirus is mediated by a membrane anchored tyrosine-based motif on the lumenal side of the endoplasmic reticulum and the C-terminal transmembrane domain in the TGB3 movement protein.
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Plasmodesmal targeting and intercellular movement of potato mop-top pomovirus is mediated by a membrane anchored tyrosine-based motif on the lumenal side of the endoplasmic reticulum and the C-terminal transmembrane domain in the TGB3 movement protein.

机译:马铃薯拖把细小波状病毒的等离子靶向和细胞间运动是由内质网腔侧的膜锚定酪氨酸基序和TGB3运动蛋白的C端跨膜结构域介导的。

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摘要

Live-cell fluorescence microscopy was used to investigate the third triple gene block protein (TGB3) of potato mop-top pomovirus and its role in assisted targeting of TGB2 to plasmodesmata (PD). Wild-type and mutant TGB3 proteins were expressed under the control of the 35S promoter or from a virus reporter clone. Assisted targeting of TGB2 to PD was optimal when the proteins were expressed from a bicistronic plasmid in the relative ratios expected in a virus infection, suggesting that excess TGB3 inhibited PD localisation. Contrary to the generally accepted view, bimolecular fluorescence complementation showed that the TGB3 N terminus is located in the cytosol. Mutational analysis to dissect TGB3 sub domain functions showed that PD targeting was mediated by a composite signal comprising an ER-lumenal tyrosine-based motif and the C-terminal transmembrane domain. Mutation of either of these domains also abolished cell-to-cell movement of the virus. The results are discussed in the context of TGB3 membrane topology.
机译:活细胞荧光显微镜技术用于研究马铃薯拖把顶部痘病毒的第三个三联基因阻滞蛋白(TGB3)及其在辅助TGB2靶向浆膜瘤(PD)中的作用。野生型和突变型TGB3蛋白在35S启动子的控制下或从病毒报告基因克隆中表达。当从双顺反子质粒以病毒感染中预期的相对比率表达蛋白质时,将TGB2辅助靶向至PD最佳,这表明过量的TGB3抑制了PD定位。与普遍接受的观点相反,双分子荧光互补显示TGB3 N末端位于细胞质中。解剖TGB3子域功能的突变分析表明,PD靶向作用是由复合信号介导的,该复合信号包含基于ER腔酪氨酸的基序和C端跨膜结构域。这些结构域中任何一个的突变也消除了病毒的细胞间移动。在TGB3膜拓扑中讨论了结果。

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