Role of pseudorabies virus glycoprotein gI in virus release from infected cells.

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J Virol. 1987 September; 61(9): 2764-2769

Role of pseudorabies virus glycoprotein gI in virus release from infected cells.

T C Mettenleiter, C Schreurs, F Zuckermann and T Ben-Porat

ABSTRACT

The Bartha vaccine strain of pseudorabies virus has a deletionin the short unique (Us) region of its genome which includesthe genes that code for glycoproteins gI and gp63 (E. Petrovskis,J. G. Timmins, T. M. Gierman, and L. E. Post, J. Virol. 60:1166-1169,1986). Restoration of an intact Us to the Bartha strain enhancesits ability to be released from infected rabbit kidney cellsand increases the size of the plaques formed on these cells(T. Ben-Porat, J. M. DeMarchi, J. Pendrys, R. A. Veach, andA. S. Kaplan, J. Virol. 57:191-196, 1986). To determine whichgene function plays a role in virus release from rabbit kidneycells, deletions were introduced into the genomes of both wild-typevirus and the "rescued" Bartha strain (Bartha strain to whichan intact Us had been restored) that abolish the expressionof either the gI gene alone or both gI and gp63 genes. The effectof these deletions on the phenotype of the viruses was studied.Deletion mutants of wild-type virus defective in either gI orgI and gp63 behave like wild-type virus with respect to virusrelease and plaque size on rabbit kidney cells. Deletion ofgI from the rescued Bartha strain, however, strongly affectsvirus release and causes a decrease in plaque size. We concludethat gI affects virus release but that at least one other viralfunction also affects this process. This function is defectivein the Bartha strain but not in wild-type virus; in its absencegI is essential to efficient release of the virus from rabbitkidney cells.

J Virol. 1987 September; 61(9): 2764-2769

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