Role for nsP2 Proteins in the Cessation of Alphavirus Minus-Strand Synthesis by Host Cells

doi:10.1128/JVI.80.1.360-371.2006

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Journal of Virology, January 2006, p. 360-371, Vol. 80, No. 1
0022-538X/06/$08.00+0 doi:10.1128/JVI.80.1.360-371.2006
Copyright © 2006, American Society for Microbiology. All Rights Reserved.

Role for nsP2 Proteins in the Cessation of Alphavirus Minus-Strand Synthesis by Host Cells

Dorothea L. Sawicki,¹^* Silvia Perri,² John M. Polo,² and Stanley G. Sawicki¹

Microbiology and Immunology Department, Medical University of Ohio, Toledo, Ohio 43614,¹ Chiron Corporation, Emeryville, California²

Received 29 March 2005/ Accepted 22 September 2005

In order to establish nonlytic persistent infections (PI) ofBHK cells, replicons derived from Sindbis (SIN) and SemlikiForest (SFV) viruses have mutations in nsP2. Five differentnsP2 PI replicons were compared to wild-type (wt) SIN, SFV,and wt nsPs SIN replicons. Replicon PI BHK21 cells had viralRNA synthesis rates that were less than 5% of those of the wtvirus and $~$ 10% or less of those of SIN wt replicon-infected cells,and, in contrast to wt virus and replicons containing wt nsP2,all showed a phenotype of continuous minus-strand synthesisand of unstable, mature replication/transcription complexes(RC+) that are active in plus-strand synthesis. Minus-strandsynthesis and incorporation of [³H]uridine into replicativeintermediates differed among PI replicons, depending on thelocation of the mutation in nsP2. Minus-strand synthesis byPI cells appeared normal; it was dependent on continuous P123and P1234 polyprotein synthesis and ceased when protein synthesiswas inhibited. The failure by the PI replicons to shut off minus-strandsynthesis was not due to some defect in the PI cells but ratherwas due to the loss of some function in the mutated nsP2. Thiswas demonstrated by showing that superinfection of PI cellswith wt SFV triggered the shutdown of minus-strand synthesis,which we believe is a host response to infection with alphaviruses.Together, the results indicate alphavirus nsP2 functions toengage the host response to infection and activate a switchfrom the early-to-late phase. The loss of this function leadsto continuous viral minus-strand synthesis and the productionof unstable RC+.

* Corresponding author. Mailing address: Medical University of Ohio, Department of Microbiology and Immunology, 3055 Arlington Avenue, Toledo, OH 43614. Phone: (419) 383-4337. Fax: (419) 383-3002. E-mail: dsawicki{at}meduohio.edu.

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