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通过反向遗传学系统拯救传染性轮状病毒重组体受到 VP4 受体结合区的限制。

Rescue of Infectious Rotavirus Reassortants by a Reverse Genetics System Is Restricted by the Receptor-Binding Region of VP4.

机构信息

Department of Biological Safety, German Federal Institute for Risk Assessment, 10589 Berlin, Germany.

Human Metabolomics, Faculty of Natural and Agricultural Sciences, North-West University, 2531 Potchefstroom, South Africa.

出版信息

Viruses. 2021 Feb 25;13(3):363. doi: 10.3390/v13030363.

Abstract

The rotavirus species A (RVA) capsid contains the spike protein VP4, which interacts with VP6 and VP7 and is involved in cellular receptor binding. The capsid encloses the genome consisting of eleven dsRNA segments. Reassortment events can result in novel strains with changed properties. Using a plasmid-based reverse genetics system based on simian RVA strain SA11, we previously showed that the rescue of viable reassortants containing a heterologous VP4-encoding genome segment was strain-dependent. In order to unravel the reasons for the reassortment restrictions, we designed here a series of plasmids encoding chimeric VP4s. Exchange of the VP4 domains interacting with VP6 and VP7 was not sufficient for rescue of viable viruses. In contrast, the exchange of fragments encoding the receptor-binding region of VP4 resulted in virus rescue. All parent strains and the rescued reassortants replicated efficiently in MA-104 cells used for virus propagation. In contrast, replication in BSR T7/5 cells used for plasmid transfection was only efficient for the SA11 strain, whereas the rescued reassortants replicated slowly, and the parent strains failing to produce reassortants did not replicate. While future research in this area is necessary, replication in BSR T7/5 cells may be one factor that affects the rescue of RVAs.

摘要

轮状病毒 A 种(RVA)衣壳包含与 VP6 和 VP7 相互作用并参与细胞受体结合的刺突蛋白 VP4。衣壳包含由 11 个 dsRNA 片段组成的基因组。重组事件可导致具有改变特性的新菌株。使用基于猿猴 RVA 株 SA11 的基于质粒的反向遗传学系统,我们之前表明,含有异源 VP4 编码基因组片段的有活力的重组体的拯救是依赖于株的。为了解开重组限制的原因,我们在这里设计了一系列编码嵌合 VP4 的质粒。与 VP6 和 VP7 相互作用的 VP4 结构域的交换不足以拯救有活力的病毒。相比之下,交换编码 VP4 受体结合区的片段导致病毒拯救。用于病毒繁殖的 MA-104 细胞中,所有亲本株和拯救的重组体都有效地复制。相比之下,用于质粒转染的 BSR T7/5 细胞中的复制仅对 SA11 株有效,而拯救的重组体复制缓慢,不能产生重组体的亲本株则不复制。虽然未来在这一领域的研究是必要的,但 BSR T7/5 细胞中的复制可能是影响 RVA 拯救的一个因素。

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