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Function Architecture and Biogenesis of Reovirus Replication Neoorganelles

机译:呼肠孤病毒复制新细胞的功能结构和生物发生。

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摘要

Most viruses that replicate in the cytoplasm of host cells form neoorganelles that serve as sites of viral genome replication and particle assembly. These highly specialized structures concentrate viral proteins and nucleic acids, prevent the activation of cell-intrinsic defenses, and coordinate the release of progeny particles. Reoviruses are common pathogens of mammals that have been linked to celiac disease and show promise for oncolytic applications. These viruses form nonenveloped, double-shelled virions that contain ten segments of double-stranded RNA. Replication organelles in reovirus-infected cells are nucleated by viral nonstructural proteins µNS and σNS. Both proteins partition the endoplasmic reticulum to form the matrix of these structures. The resultant membranous webs likely serve to anchor viral RNA–protein complexes for the replication of the reovirus genome and the assembly of progeny virions. Ongoing studies of reovirus replication organelles will advance our knowledge about the strategies used by viruses to commandeer host biosynthetic pathways and may expose new targets for therapeutic intervention against diverse families of pathogenic viruses.
机译:在宿主细胞的细胞质中复制的大多数病毒会形成新细胞器,作为病毒基因组复制和颗粒装配的位点。这些高度专业化的结构可浓缩病毒蛋白和核酸,阻止细胞内在防御的激活,并协调子代颗粒的释放。呼肠孤病毒是哺乳动物的常见病原体,已与乳糜泻相关,并显示出溶瘤的应用前景。这些病毒形成无包膜的双壳病毒粒子,其中包含十段双链RNA。呼肠孤病毒感染细胞中的复制细胞器被病毒非结构蛋白µNS和σNS形核。两种蛋白质都将内质网分开,以形成这些结构的基质。由此产生的膜状网可能会锚定病毒RNA-蛋白质复合物,用于呼肠孤病毒基因组的复制和子代病毒体的组装。正在进行的呼肠孤病毒复制细胞器的研究将提高我们对病毒用于控制宿主生物合成途径的策略的了解,并可能为针对多种病原性病毒的治疗干预提供新的靶点。

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