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Rescue of the prototypic Arenavirus LCMV entirely from plasmid

机译:完全从质粒拯救原型竞技场病毒LCMV

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We document a helper-independent reverse genetics system for rescuing infectious arenaviruses from cloned cDNAs. We constructed plasmids containing full-length cDNAs of the antigenomic (ag) L and S segments of the Armstrong (ARM) strain of the prototypic Arenavirus lymphocytic choriomeningitis virus (LCMV) flanked at their 5 '- and 3 '-termini by the T7 RNA polymerase (T7RP) promoter and ribozyme sequences, respectively. These plasmids directed intracellular synthesis of viral L and S ag RNA species in cells expressing plasmid-supplied T7Rp. Co-expression of plasmid-supplied LCMV trans-acting factors, nucleoprotein (NP) and polymerase (L), resulted in replication and expression of L and S ag and genome RNA species, and generation of LCMV infectious progeny termed rT7/LCMV. The recombinant rT7/LCMV was unequivocally identified based on a genetic tag introduced in the recombinant S segment. In addition, rT7/LCMV exhibited growth and biological properties predicted for an ARM-like LCMV. To our knowledge, this is the first documented Arenavirus rescue, as well as of an ambisense negative strand (NS) RNA virus, entirely from cloned cDNAs. Our results extend the use of reverse genetic approaches for DNA-mediated virus rescue to all known virus families with NS RNA genome. (c) 2006 Elsevier Inc. All rights reserved.
机译:我们记录了从克隆的cDNA拯救传染性arenaviruses的独立于助手的反向遗传学系统。我们构建了质粒,该质粒包含原型球状病毒淋巴膜脑膜炎病毒(LCMV)的阿姆斯特朗(ARM)株的反基因组(ag)L和S区段的全长cDNA,T7 RNA位于其5'-和3'-末端聚合酶(T7RP)启动子和核酶序列。这些质粒指导表达质粒提供的T7Rp的细胞中病毒L和S ag RNA种类的细胞内合成。质粒提供的LCMV反作用因子,核蛋白(NP)和聚合酶(L)的共表达导致L和Sag和基因组RNA物种的复制和表达,并产生称为rT7 / LCMV的LCMV传染性子代。基于在重组S区段中引入的遗传标签明确鉴定了重组rT7 / LCMV。另外,rT7 / LCMV表现出可预测的ARM类LCMV生长和生物学特性。据我们所知,这是首次记载完全从克隆的cDNA中拯救出的Arenavirus以及歧义负链(NS)RNA病毒。我们的研究结果将反向遗传方法用于DNA介导的病毒抢救扩展到了所有已知的带有NS RNA基因组的病毒家族。 (c)2006 Elsevier Inc.保留所有权利。

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