首页> 美国卫生研究院文献>Journal of Virology >Note: Virus Reconstituted from Infectious Bacterial Artificial Chromosome (BAC)-Cloned Murine Gammaherpesvirus 68 Acquires Wild-Type Properties In Vivo Only after Excision of BAC Vector Sequences
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Note: Virus Reconstituted from Infectious Bacterial Artificial Chromosome (BAC)-Cloned Murine Gammaherpesvirus 68 Acquires Wild-Type Properties In Vivo Only after Excision of BAC Vector Sequences

机译:注意:从感染性细菌人工染色体(BAC)克隆的鼠γ疱疹病毒68重构的病毒仅在切除BAC载体序列后才能体内获得野生型特性

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摘要

We studied the in vivo biological properties of viruses reconstituted from the genome of murine gammaherpesvirus 68 (MHV-68) cloned as an infectious bacterial artificial chromosome (BAC). Recombinant virus RγHV68A98.01, containing BAC vector sequences, is attenuated in vivo as determined by (i) viral titers in the lungs during the acute phase of infection, (ii) the extent of splenomegaly, and (iii) the number of latently infected spleen cells reactivating virus in an ex vivo reactivation assay. Since the BAC vector sequences were flanked by loxP sites, passaging the virus in fibroblasts expressing Cre recombinase resulted in the generation of recombinant virus RγHV68A98.02, with biological properties comparable to those of wild-type MHV-68. On the basis of these data we conclude (i) that excision of BAC vector sequences from cloned MHV-68 genomes is critical for reconstitution of the wild-type phenotypic properties of this virus and (ii) that the BAC-cloned MHV-68 genome is suitable for the construction of mutants and mutant libraries whose phenotypes can be reliably assessed in vivo.
机译:我们研究了从克隆为感染性细菌人工染色体(BAC)的鼠γ疱疹病毒68(MHV-68)基因组中重组的病毒的体内生物学特性。包含BAC载体序列的重组病毒RγHV68A98.01在体内被减毒,具体取决于(i)感染急性期期间肺中的病毒滴度,(ii)脾肿大程度和(iii)潜在感染的数量在离体再激活测定中脾细胞再激活病毒。由于BAC载体序列位于loxP位点的两侧,因此在表达Cre重组酶的成纤维细胞中传代病毒导致了重组病毒RγHV68A98.02的产生,其生物学特性与野生型MHV-68相当。根据这些数据,我们得出以下结论:(i)从克隆的MHV-68基因组中切除BAC载体序列对于重组该病毒的野生型表型至关重要,并且(ii)BAC克隆的MHV-68基因组适于构建表型可以在体内可靠评估的突变体和突变体文库。

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