Encapsidation of the Flavivirus Kunjin Replicon RNA by Using a Complementation System Providing Kunjin Virus Structural Proteins in trans

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J Virol, July 1998, p. 5967-5977, Vol. 72, No. 7
0022-538X/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

Encapsidation of the Flavivirus Kunjin Replicon RNA by Using a Complementation System Providing Kunjin Virus Structural Proteins in trans

Alexander A. Khromykh,^* Andrei N. Varnavski, and Edwin G. Westaway

Sir Albert Sakzewski Virus Research Centre, Royal Children's Hospital, Brisbane, Queensland 4029, Australia

Received 15 October 1997/Accepted 23 March 1998

Kunjin virus (KUN) replicon RNA was encapsidated by a procedure involving two consecutive electroporations of BHK-21 cells,first with KUN replicon RNA C20DXrep (with prME and most of Cdeleted) and about 24 h later with a recombinant Semliki Forestvirus (SFV) replicon RNA(s) expressing KUN structural proteins.The presence of KUN replicon RNA in encapsidated particles wasdemonstrated by its amplification and expression in newly infectedBHK-21 cells, detected by Northern blotting with a KUN-specificprobe and by immunofluorescence analysis with anti-NS3 antibodies.No infectious particles were produced when C20DXrep RNA and recombinantSFV RNAs were electroporated simultaneously. When the second electroporationwas performed with a single SFV replicon RNA expressing the KUNcontiguous prME genes and the KUN C gene together but under controlof two separate 26S subgenomic promoters (SFV-prME-C107), a 10-fold-highertiter of infectious particles was achieved than when two differentSFV replicon RNAs expressing the KUN C gene (SFV-C107) and prMEgenes (SFV-prME) separately were used. No SFV replicon RNAs expressingKUN structural proteins were encapsidated in secreted particles.Infectious particles pelleted by ultracentrifugation of the culturefluid from cells sequentially transfected with C20DXrep and SFV-prME-C107RNAs were neutralized by preincubation with monoclonal antibodiesto KUN E protein. Radioimmunoprecipitation analysis with anti-Eantibodies of the culture fluid of the doubly transfected cellsshowed the presence of C, prM/M, and E proteins in the immunoprecipitatedparticles. Reverse transcription-PCR analysis showed that theimmunoprecipitated particles also contained KUN-specific RNA.The encapsidated replicon particles sedimented more slowly thanKUN virions in a 5 to 25% sucrose density gradient and were uniformlyspherical, with an ~35-nm diameter, compared with ~50 nm for KUNvirions. The results of this study demonstrate for the first timepackaging of flavivirus RNA in trans, and they exclude a rolein packaging for virtually all of the structural region. Possibleapplications of the developed packaging system include the definitionof the packaging signal(s) in flavivirus RNA as well as the aminoacid motif(s) in the structural proteins involved in RNA encapsidation,virion assembly, and secretion. Furthermore, it could facilitatethe development of a noninfectious vaccine delivery system basedon encapsidation of a noncytopathic flavivirus replicon expressingheterologous genes.

^* Corresponding author. Mailing address: Sir Albert Sakzewski Virus Research Centre, Royal Children's Hospital, Herston Rd.,Brisbane, QLD 4029, Australia. Phone: (617) 3253-1568. Fax: (617)3253-1401. E-mail: A.Khromykh{at}mailbox.uq.edu.au.

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