Optimization of targeted RNA recombination and mapping of a novel nucleocapsid gene mutation in the coronavirus mouse hepatitis virus.

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J Virol. 1994 January; 68(1): 328-337

Optimization of targeted RNA recombination and mapping of a novel nucleocapsid gene mutation in the coronavirus mouse hepatitis virus.

P S Masters, C A Koetzner, C A Kerr and Y Heo

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

ABSTRACT

We have recently described a method of introducing site-specificmutations into the genome of the coronavirus mouse hepatitisvirus (MHV) by RNA recombination between cotransfected genomicRNA and a synthetic subgenomic mRNA (C. A. Koetzner, M. M. Parker,C. S. Ricard, L. S. Sturman, and P. S. Masters, J. Virol. 66:1841-1848,1992). By using a thermolabile N protein mutant of MHV (Alb4)as the recipient virus and synthetic RNA7 (the mRNA for thenucleocapsid protein N) as the donor, we selected engineeredrecombinant viruses as heat-stable progeny resulting from cotransfection.We have now been able to greatly increase the efficiency oftargeted recombination in this process by using a syntheticdefective interfering (DI) RNA in place of RNA7. The frequencyof recombination is sufficiently high that, with Alb4 as therecipient, recombinants can be directly identified without usingthermal selection. The synthetic DI RNA has been used to demonstratethat the lesion in another temperature-sensitive and thermolabileMHV mutant, Alb1, maps to the N gene. Sequencing of the Alb1N gene revealed two closely linked point mutations that fallin a region of the N molecule previously noted as being themost highly conserved region among all of the coronavirus Nproteins. Analysis of revertants of the Alb1 mutant revealedthat one of the two mutations is critical for the temperature-sensitivephenotype; the second mutation is phenotypically silent.

J Virol. 1994 January; 68(1): 328-337

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