Replicase Complex Genes of Semliki Forest Virus Confer Lethal Neurovirulence

doi:10.1128/JVI.74.10.4579-4589.2000

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Journal of Virology, May 2000, p. 4579-4589, Vol. 74, No. 10
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Replicase Complex Genes of Semliki Forest Virus Confer Lethal Neurovirulence

Minna T. Tuittila,¹^,²^,^* Maria G. Santagati,³ Matias Röyttä,⁴ Jorma A. Määttä,¹^,² and Ari E. Hinkkanen¹^,²

Department of Biochemistry and Pharmacy, Åbo Akademi University,¹ Turku Immunology Centre,² and Department of Virology, MediCity Research Laboratory,³ and Department of Pathology,⁴ University of Turku, Turku, Finland

Received 21 April 1999/Accepted 10 February 2000

Semliki Forest virus (SFV) is a mosquito-transmitted pathogen of small rodents, and infection of adult mice with SFV4, a neurovirulentstrain of SFV, leads to lethal encephalitis in a few days, whereasmice infected with the avirulent A7(74) strain remain asymptomatic.In adult neurons, A7(74) is unable to form virions and hence doesnot reach a critical threshold of neuronal damage. To elucidatethe molecular mechanisms of neurovirulence, we have cloned andsequenced the entire 11,758-nucleotide genome of A7(74) and comparedit to the highly neurovirulent SFV4 virus. We found several sequencedifferences and sought to localize determinants conferring theneuropathogenicity by using a panel of chimeras between SFV4 anda cloned recombinant, rA774. We first localized virulence determinantsin the nonstructural region by showing that rA774 structural genescombined with the SFV4 nonstructural genome produced a highlyvirulent virus, while a reciprocal recombinant was asymptomatic.In addition to several amino acid mutations in the nonstructuralregion, the nsp3 gene of rA774 displayed an opal termination codonand an in-frame 21-nucleotide deletion close to the nsp4 junction.Replacement in rA774 of the entire nsp3 gene with that of SFV4reconstituted the virulent phenotype, whereas an arginine at theopal position significantly increased virulence, leading to clinicalsymptoms in mice. Completion of the nsp3 deletion in rA774 didnot increase virulence. We conclude that the opal codon and aminoacid mutations other than the deleted residues are mainly responsiblefor the attenuation of A7(74) and that the attenuating determinantsreside entirely in the nonstructuralregion.

^* Corresponding author. Mailing address: Department of Biochemistry and Pharmacy, Åbo Akademi University, FIN-20520 Turku, Finland.Phone: 358-2-2154141. Fax: 358-2-2154745. E-mail: minna.tuittila{at}ra.abo.fi.

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