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Cytoplasmic Granule Formation and Translational Inhibition of Nodaviral RNAs in the Absence of the Double-Stranded RNA Binding Protein B2

机译:在没有双链RNA结合蛋白B2的情况下Nodaviral RNA的细胞质颗粒形成和翻译抑制。

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摘要

Flock House virus (FHV) is a positive-sense RNA insect virus with a bipartite genome. RNA1 encodes the RNA-dependent RNA polymerase, and RNA2 encodes the capsid protein. A third protein, B2, is translated from a subgenomic RNA3 derived from the 3′ end of RNA1. B2 is a double-stranded RNA (dsRNA) binding protein that inhibits RNA silencing, a major antiviral defense pathway in insects. FHV is conveniently propagated in Drosophila melanogaster cells but can also be grown in mammalian cells. It was previously reported that B2 is dispensable for FHV RNA replication in BHK21 cells; therefore, we chose this cell line to generate a viral mutant that lacked the ability to produce B2. Consistent with published results, we found that RNA replication was indeed vigorous but the yield of progeny virus was negligible. Closer inspection revealed that infected cells contained very small amounts of coat protein despite an abundance of RNA2. B2 mutants that had reduced affinity for dsRNA produced analogous results, suggesting that the dsRNA binding capacity of B2 somehow played a role in coat protein synthesis. Using fluorescence in situ hybridization of FHV RNAs, we discovered that RNA2 is recruited into large cytoplasmic granules in the absence of B2, whereas the distribution of RNA1 remains largely unaffected. We conclude that B2, by binding to double-stranded regions in progeny RNA2, prevents recruitment of RNA2 into cellular structures, where it is translationally silenced. This represents a novel function of B2 that further contributes to successful completion of the nodaviral life cycle.
机译:鸡群病毒(FHV)是一种具有两部分基因组的正义RNA昆虫病毒。 RNA1编码RNA依赖性RNA聚合酶,RNA2编码衣壳蛋白。第三个蛋白质B2从源自RNA1 3'末端的亚基因组RNA3翻译而来。 B2是一种双链RNA(dsRNA)结合蛋白,可抑制RNA沉默,而沉默是昆虫的主要抗病毒防御途径。 FHV方便地在果蝇果蝇细胞中繁殖,但也可以在哺乳动物细胞中繁殖。以前有报道说B2对于BHK21细胞中的FHV RNA复制是必不可少的。因此,我们选择该细胞系来产生缺乏产生B2能力的病毒突变体。与已发表的结果一致,我们发现RNA复制确实有力,但后代病毒的产量可忽略不计。仔细检查发现,尽管存在大量的RNA2,但被感染的细胞仍含有少量的外壳蛋白。对dsRNA的亲和力降低的B2突变体产生了相似的结果,表明B2的dsRNA结合能力在外壳蛋白合成中起了一定作用。使用FHV RNA的荧光原位杂交,我们发现在没有B2的情况下RNA2被募集到大的细胞质颗粒中,而RNA1的分布在很大程度上不受影响。我们得出的结论是,B2通过与子代RNA2中的双链区域结合,阻止RNA2募集到细胞结构中,在那里翻译被沉默。这代表了B2的新功能,进一步有助于成功地完成了淋巴结生命周期。

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