Genetic evidence for two distinct transactivation functions of the herpes simplex virus alpha protein ICP27.

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J Virol. 1990 April; 64(4): 1704-1715

Genetic evidence for two distinct transactivation functions of the herpes simplex virus alpha protein ICP27.

S A Rice and D M Knipe

Department of Microbiology and Molecular Genetics, Harvard Medical School, Boston, Massachusetts 02115.

ABSTRACT

Infected-cell protein 27 (ICP27) is a herpes simplex virus type1 alpha, or immediate-early, protein involved in the regulationof viral gene expression. To better understand the function(s)of ICP27 in infected cells, we have isolated and characterizedviral recombinants containing defined alterations in the ICP27gene. The mutant virus d27-1 contains a 1.6-kilobase deletionwhich removes the ICP27 gene promoter and most of the codingsequences, while n59R, n263R, n406R, and n504R are mutants containingnonsense mutations which encode ICP27 molecules truncated attheir carboxyl termini. All five mutants were defective forlytic replication in Vero cells. Analysis of the mutant phenotypessuggests that ICP27 has the following regulatory effects duringthe viral infection: (i) stimulation of expression of gamma-1genes, (ii) induction of expression of gamma-2 genes, (iii)down regulation of expression of alpha and beta genes late ininfection, and (iv) stimulation of viral DNA replication. Cellsinfected with the mutant n504R expressed wild-type levels ofgamma-1 proteins but appeared to be unable to efficiently expressgamma-2 mRNAs or proteins. This result suggests that ICP27 mediatestwo distinct transactivation functions, one which stimulatesgamma-1 gene expression and a second one required for gamma-2gene induction. Analysis of the mutant n406R suggested thata truncated ICP27 polypeptide can interfere with the expressionof many viral beta genes. Our results demonstrate that ICP27has a variety of positive and negative effects on the expressionof viral genes during infection.

J Virol. 1990 April; 64(4): 1704-1715

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