首页> 美国卫生研究院文献>Journal of Virology >Construction and characterization of an infectious DNA clone and of mutants of simian immunodeficiency virus isolated from the African green monkey.
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Construction and characterization of an infectious DNA clone and of mutants of simian immunodeficiency virus isolated from the African green monkey.

机译:从非洲绿猴分离的感染性DNA克隆和猿猴免疫缺陷病毒突变体的构建和表征。

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摘要

We constructed a full-length molecular clone of simian immunodeficiency virus from an African green monkey. Upon transfection, this clone directed the production of virus particles cytopathic and infectious to human CD4+ leukemia cell lines. Mutations were introduced by recombinant DNA techniques into eight open reading frames of simian immunodeficiency virus from the African green monkey thus far identified. The phenotypes of mutant viruses, i.e., infectivity, cytopathogenicity, transactivation of gene expression controlled by a long terminal repeat, and viral RNA and protein syntheses, were examined by transfection and infection experiments. Three structural (gag, pol, and env) and two regulatory (tat and rev) gene mutants were not infectious, whereas vif, vpx, and nef were dispensable for infectivity and mutant viruses were highly cytopathic. In transient transfection assays, a rev mutant produced mainly small mRNA species and no detectable virus protein and particles. The transactivation potential of a tat mutant was about 10-fold less than that of wild-type DNA, generating small amounts of virus.
机译:我们从非洲绿猴构建了猿猴免疫缺陷病毒的全长分子克隆。转染后,该克隆指导细胞病变并感染人CD4 +白血病细胞系的病毒颗粒的产生。通过重组DNA技术将突变引入迄今已鉴定的来自非洲绿猴的猿猴免疫缺陷病毒的八个开放阅读框中。通过转染和感染实验检查了突变病毒的表型,即感染性,细胞致病性,由长末端重复序列控制的基因表达的反式激活以及病毒RNA和蛋白质的合成。三个结构性(gag,pol和env)和两个调节性(tat和rev)基因突变体无感染性,而vif,vpx和nef对感染性不可或缺,而突变病毒则具有高度的细胞病变性。在瞬时转染测定中,rev突变体主要产生较小的mRNA种类,而未检测到病毒蛋白和颗粒。 tat突变体的反式激活潜能比野生型DNA低约10倍,从而产生少量病毒。

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