Repair and mutagenesis of the genome of a deletion mutant of the coronavirus mouse hepatitis virus by targeted RNA recombination.

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J Virol. 1992 April; 66(4): 1841-1848

Repair and mutagenesis of the genome of a deletion mutant of the coronavirus mouse hepatitis virus by targeted RNA recombination.

C A Koetzner, M M Parker, C S Ricard, L S Sturman and P S Masters

Wadsworth Center for Laboratories and Research, New York State Department of Health, Albany 12201-0509.

ABSTRACT

The genetic characterization of a nucleocapsid (N) protein mutantof the coronavirus mouse hepatitis virus (MHV) is described.The mutant, Albany 4 (Alb4), is both temperature sensitive andthermolabile. Analysis of the progeny of a mixed infection showedthat the defective Alb4 allele is recessive to wild type, andits gene product is diffusible. The N protein of Alb4 was foundto be smaller than its wild-type counterpart, and sequence analysisof the Alb4 N gene revealed that it contains an internal deletionof 87 nucleotides, producing an in-frame deletion of 29 aminoacids. All of these properties of Alb4 made it ideal for useas a recipient in a targeted RNA recombination experiment inwhich the deletion in Alb4 was repaired by recombination withsynthetic RNA7, the smallest MHV subgenomic mRNA. Progeny froma cotransfection of Alb4 genomic RNA and synthetic RNA7 wereselected for thermal stability. Polymerase chain reaction analysisof candidate recombinants showed that they had regained thematerial that is deleted in the Alb4 mutant. They also had acquireda five-nucleotide insertion in the 3' untranslated region, whichhad been incorporated into the synthetic RNA7 as a moleculartag. The presence of the tag was directly verified, as well,by sequencing the genomic RNA of purified recombinant viruses.This provided a clear genetic proof that the Alb4 phenotypewas due to the observed deletion in the N gene. In addition,these results demonstrated that it is possible to obtain stable,independently replicating progeny from recombination betweencoronavirus genomic RNA and a tailored, synthetic RNA species.

J Virol. 1992 April; 66(4): 1841-1848

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