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Phenotypic Consequence of Rearranging the N Gene of RABV HEP-Flury

机译:RABV HEP-Flury N基因重排的表型后果

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摘要

Nucleoprotein (N) is a key element in rabies virus (RABV) replication. To further investigate the effect of N on RABV, we manipulated an infectious cDNA clone of the RABV HEP-Flury to rearrange the N gene from its wild-type position of 1 (N-P-M-G-L) to 2 (P-N-M-G-L), 3 (P-M-N-G-L), or 4 (P-M-G-N-L), using an approach that left the viral nucleotide sequence unaltered. Subsequently, viable viruses were recovered from each of the rearranged cDNA and examined for their gene expression levels, growth kinetics in cell culture, pathogenicity in suckling mice and protection in mice. The results showed that gene rearrangement decreased N mRNA transcription and vRNA replication. As a result, all viruses with rearranged genomes showed worse replication than that of rHEP-Flury in NA cells at a MOI of 0.01, but equivalent or slightly better replication levels at a MOI of 3. Consequently, the lethality in suckling mice infected with N4 was clearly attenuated compared with rHEP-Flury. However, the protection to mice was not enhanced. This study not only gives us insight into the understanding of the phenotype of RABV N gene rearrangement, but also helps with rabies vaccine candidate construction.
机译:核蛋白(N)是狂犬病毒(RABV)复制的关键要素。为了进一步研究N对RABV的影响,我们操作了RABV HEP-Flury的感染性cDNA克隆,将N基因从其野生型位置1(NPMGL)重置为2(PNMGL),3(PMNGL)或4(PMGNL),使用不改变病毒核苷酸序列的方法。随后,从每个重排的cDNA中回收活病毒,并检查其基因表达水平,细胞培养中的生长动力学,哺乳小鼠的致病性和小鼠的保护作用。结果表明基因重排减少了N mRNA转录和vRNA复制。结果,在MOI为0.01的情况下,所有具有重排基因组的病毒在NA细胞中的复制均比rHEP-Flury差,但在MOI为3时,复制水平却相当或略高。因此,感染了N4的乳鼠的致死性与rHEP-Flury相比,其明显减弱。但是,对小鼠的保护作用没有增强。这项研究不仅使我们深入了解了RABV N基因重排的表型,而且还帮助构建了狂犬病疫苗候选物。

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