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Journal of Virology, October 2000, p. 9347-9352, Vol. 74, No. 20
Department of Veterinary Sciences and
Microbiology, University of Arizona, Tucson, Arizona 85721
Received 18 April 2000/Accepted 27 July 2000
Viral assembly is an ideal system in which to investigate the
transient recognition and interplay between proteins. During morphogenesis, scaffolding proteins temporarily associate with structural proteins, stimulating conformational changes that promote assembly and inhibit off-pathway reactions. Microviridae
morphogenesis is dependent on two scaffolding proteins, an internal and
an external species. The external scaffolding protein is the most
conserved protein within the Microviridae, whose canonical
members are
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Foreign and Chimeric External Scaffolding Proteins
as Inhibitors of Microviridae Morphogenesis
X174, G4, and 
3. However, despite 70% homology on
the amino acid level, overexpression of a foreign
Microviridae external scaffolding protein is a potent
cross-species inhibitor of morphogenesis. Mutants that are resistant to
the expression of a foreign scaffolding protein cannot be obtained via
one mutational step. To define the requirements for and constraints on
scaffolding protein interactions, chimeric external scaffolding
proteins have been constructed and analyzed for effects on in vivo
assembly. The results of these experiments suggest that at least two
cross-species inhibitory domains exist within these proteins; one
domain most likely blocks procapsid formation, and the other allows
procapsid assembly but blocks DNA packaging. A mutation conferring
resistance to the expression of a chimeric protein (chiDr)
that inhibits DNA packaging was isolated. The mutation maps to gene A,
which encodes a protein essential for packaging. The chiDr mutation confers resistance only to a
chimeric D protein; the mutant is still inhibited by the expression of
foreign D proteins. The results presented here demonstrate how closely
related proteins could be developed into antiviral agents that
specifically target virion morphogenesis.
*
Corresponding author. Mailing address: Department of
Veterinary Sciences and Microbiology, University of Arizona, Tucson, AZ
85721. Phone: (520) 626-6634. Fax: (520) 621-6366. E-mail: bfane{at}u.arizona.edu.
Journal of Virology, October 2000, p. 9347-9352, Vol. 74, No. 20
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
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