首页> 美国卫生研究院文献>Journal of Virology >Chemical Mutagenesis of Dengue Virus Type 4 Yields Mutant Viruses Which Are Temperature Sensitive in Vero Cells or Human Liver Cells and Attenuated in Mice
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Chemical Mutagenesis of Dengue Virus Type 4 Yields Mutant Viruses Which Are Temperature Sensitive in Vero Cells or Human Liver Cells and Attenuated in Mice

机译:登革热病毒4型的化学诱变产生突变病毒它们在Vero细胞或人肝细胞中具有温度敏感性并且在小鼠中具有减毒作用

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摘要

A recombinant live attenuated dengue virus type 4 (DEN4) vaccine candidate, 2AΔ30, was found previously to be generally well tolerated in humans, but a rash and an elevation of liver enzymes in the serum occurred in some vaccinees. 2AΔ30, a non-temperature-sensitive (non-ts) virus, contains a 30-nucleotide deletion (Δ30) in the 3′ untranslated region (UTR) of the viral genome. In the present study, chemical mutagenesis of DEN4 was utilized to generate attenuating mutations which may be useful in further attenuation of the 2AΔ30 candidate vaccine. Wild-type DEN4 2A virus was grown in Vero cells in the presence of 5-fluorouracil, and a panel of 1,248 clones were isolated. Twenty ts mutant viruses were identified that were ts in both simian Vero and human liver HuH-7 cells (n = 13) or only in HuH-7 cells (n = 7). Each of the 20 ts mutant viruses possessed an attenuation phenotype, as indicated by restricted replication in the brains of 7-day-old mice. The complete nucleotide sequence of the 20 ts mutant viruses identified nucleotide substitutions in structural and nonstructural genes as well as in the 5′ and 3′ UTRs, with more than one change occurring, in general, per mutant virus. A ts mutation in the NS3 protein (nucleotide position 4995) was introduced into a recombinant DEN4 virus possessing the Δ30 deletion, thereby creating rDEN4Δ30-4995, a recombinant virus which is ts and more attenuated than rDEN4Δ30 virus in the brains of mice. We are assembling a menu of attenuating mutations that should be useful in generating satisfactorily attenuated recombinant dengue vaccine viruses and in increasing our understanding of the pathogenesis of dengue virus.
机译:先前发现重组重组活减毒4型登革热病毒4型(DEN4)候选疫苗在人类中通常具有良好的耐受性,但某些疫苗中出现皮疹和血清中肝酶升高。非温度敏感性(非ts)病毒2AΔ30在病毒基因组的3'非翻译区(UTR)中包含一个30个核苷酸的缺失(Δ30)。在本研究中,DEN4的化学诱变被用于产生减毒突变,这可能对进一步减毒2AΔ30候选疫苗有用。野生型DEN4 2A病毒在5-氟尿嘧啶存在下在Vero细胞中生长,并分离出一组1,248个克隆。在猿猴Vero和人肝HuH-7细胞(n = 13)或仅在HuH-7细胞(n = 7)中鉴定出20种ts突变病毒。 20 ts突变病毒中的每一种都具有减毒表型,如在7日龄小鼠的大脑中复制受限所表明的那样。 20 ts突变病毒的完整核苷酸序列确定了结构和非结构基因以及5'和3'UTR中的核苷酸取代,通常每个突变病毒发生一个以上的变化。将NS3蛋白中的ts突变(核苷酸4995位)引入具有Δ30缺失的重组DEN4病毒中,从而产生rDEN4Δ30-4995,这是一种重组病毒,在小鼠的脑中是ts且比rDEN4Δ30病毒更弱。我们正在组装一系列减毒突变,这些突变应可用于产生令人满意的减毒重组登革热疫苗病毒,并有助于增进我们对登革热病毒发病机理的了解。

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