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Rewiring the severe acute respiratory syndrome coronavirus (SARS-CoV) transcription circuit: Engineering a recombination-resistant genome

机译:重布线严重急性呼吸系统综合症冠状病毒(SARS-CoV)转录回路:工程化重组抗性基因组

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Live virus vaccines provide significant protection against many detrimental human and animal diseases, but reversion to virulence by mutation and recombination has reduced appeal. Using severe acute respiratory syndrome coronavirus as a model, we engineered a different transcription regulatory circuit and isolated recombinant viruses. The transcription network allowed for efficient expression of the viral transcripts and proteins, and the recombinant viruses replicated to WT levels. Recombinant genomes were then constructed that contained mixtures of the WT and mutant regulatory circuits, reflecting recombinant viruses that might occur in nature. Although viable viruses could readily be isolated from WT and recombinant genomes containing homogeneous transcription circuits, chimeras that contained mixed regulatory networks were invariantly lethal, because viable chimeric viruses were not isolated. Mechanistically, mixed regulatory circuits promoted inefficient subgenomic transcription from inappropriate start sites, resulting in truncated ORFs and effectively minimize viral structural protein expression. Engineering regulatory transcription circuits of intercommunicating alleles successfully introduces genetic traps into a viral genome that are lethal in RNA recombinant progeny viruses.
机译:活病毒疫苗对许多有害的人类和动物疾病提供了重要的保护,但是通过突变和重组恢复为毒力已降低了吸引力。以严重急性呼吸系统综合症冠状病毒为模型,我们设计了一个不同的转录调控电路并分离了重组病毒。转录网络可有效表达病毒转录物和蛋白质,重组病毒可复制至WT水平。然后构建重组基因组,其中包含野生型和突变型调控电路的混合物,反映了自然界可能出现的重组病毒。尽管可以很容易地从野生型和含有同质转录回路的重组基因组中分离出活病毒,但是包含混合调控网络的嵌合体始终具有致死性,因为没有分离出嵌合病毒。从机制上讲,混合的调节电路会从不合适的起始位点促进低效率的亚基因组转录,导致ORF截短并有效地最小化病毒结构蛋白的表达。相互交流的等位基因的工程调控转录电路成功地将遗传陷阱引入到病毒基因组中,这种病毒陷阱在RNA重组子代病毒中具有致命性。

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