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Reverse genetics with a full-length infectious cDNA of severe acute respiratory syndrome coronavirus

机译:严重急性呼吸系统综合症冠状病毒全长传染性cDNA的反向遗传学

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摘要

A previously undescribed coronavirus (CoV) is the etiologic agent responsible for severe acute respiratory syndrome (SARS). Using a panel of contiguous cDNAs that span the entire genome, we have assembled a full-length cDNA of the SARS-CoV Urbani strain, and have rescued molecularly cloned SARS viruses (infectious clone SARS-CoV) that contained the expected marker mutations inserted into the component clones. Recombinant viruses replicated as efficiently as WT virus and both were inhibited by treatment with the cysteine proteinase inhibitor (2S,3S)-transepoxysuccinyl-L-leucylamido-3-methylbutane ethyl ester. In addition, subgenomic transcripts were initiated from the consensus sequence ACGAAC in both the WT and infectious clone SARS-CoV. Availability of a SARS-CoV full-length cDNA provides a template for manipulation of the viral genome, allowing for the rapid and rational development and testing of candidate vaccines and therapeutics against this important human pathogen.
机译:先前未描述的冠状病毒(CoV)是导致严重急性呼吸系统综合症(SARS)的病原体。使用跨越整个基因组的一组连续cDNA,我们组装了SARS-CoV Urbani株的全长cDNA,并拯救了分子克隆的SARS病毒(传染性克隆SARS-CoV),其中包含预期的标记突变,组件克隆。重组病毒的复制效率与WT病毒相同,并且都通过半胱氨酸蛋白酶抑制剂(2S,3S)-反式环氧琥珀酰-L-亮氨酰胺基-3-甲基丁烷乙酯的处理而被抑制。另外,WT和感染性克隆SARS-CoV中的共有序列ACGAAC都启动了亚基因组转录物。 SARS-CoV全长cDNA的提供为操纵病毒基因组提供了模板,从而可以快速合理地开发和测试针对这种重要人类病原体的候选疫苗和治疗剂。

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