一个氨基酸的单点突变导致病毒融合蛋白中 eGFP 的荧光丧失,从而使重组水疱性口炎病毒获得适应性和生长优势。
A single amino acid change resulting in loss of fluorescence of eGFP in a viral fusion protein confers fitness and growth advantage to the recombinant vesicular stomatitis virus.
机构信息
School of Veterinary Medicine and Biomedical Sciences, University of Nebraska-Lincoln, Lincoln, Nebraska 68583-0900, USA.
出版信息
Virology. 2012 Oct 25;432(2):460-9. doi: 10.1016/j.virol.2012.07.004. Epub 2012 Jul 24.
Abstract
Using a recombinant vesicular stomatitis virus encoding eGFP fused in-frame with an essential viral replication protein, the phosphoprotein P, we show that during passage in culture, the virus mutates the nucleotide C289 within eGFP of the fusion protein PeGFP to A or T, resulting in R97S/C amino acid substitution and loss of fluorescence. The resultant non-fluorescent virus exhibits increased fitness and growth advantage over its fluorescent counterpart. The growth advantage of the non-fluorescent virus appears to be due to increased transcription and replication activities of the PeGFP protein carrying the R97S/C substitution. Further, our results show that the R97S/C mutation occurs prior to accumulation of mutations that can result in loss of expression of the gene inserted at the G-L gene junction. These results suggest that fitness gain is more important for the recombinant virus than elimination of expression of the heterologous gene.
摘要
我们使用一种重组水疱性口炎病毒,该病毒将 eGFP 与一个必需的病毒复制蛋白——磷蛋白 P 融合,以框架内的方式进行编码。我们发现,在培养过程中,病毒会将融合蛋白 PeGFP 中的 eGFP 内的核苷酸 C289 突变为 A 或 T,导致 R97S/C 氨基酸取代和荧光丧失。由此产生的非荧光病毒表现出比其荧光对应物更高的适应性和生长优势。非荧光病毒的生长优势似乎归因于 PeGFP 蛋白的转录和复制活性增加,该蛋白携带 R97S/C 取代。此外,我们的结果表明,R97S/C 突变发生在可导致插入到 G-L 基因连接处的基因表达丧失的突变积累之前。这些结果表明,适应性增益对重组病毒比消除异源基因的表达更为重要。
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