The long-term goals of this research are to understand how the herpes simplex virus major DNA-binding protein, ICP8, moves into and within the cell nucleus, interacts with cellular and viral proteins and assembles into macromolecular structures to promote viral DNA replication and regulate viral gene expression.
The specific aims are: (1) To define the mechanisms of intranuclear assembly of HSV DNA replication proteins by co-immunoprecipitation analysis of wt and mutant forms of ICP8 and other HSV DNA replication proteins to define the requirements for interactions of ICP8 with other viral proteins in infected cells and in vitro, by isolation of viruses expressing mutant ICP8 molecules to define the role of specific protein-protein interactions during assembly of prereplicative sites in infected cells, and by preparation and use of antibodies specific for individual portions of the ICP8 molecule to examine the accessibility of specific portions of ICP8 as replication structures assemble. (2) To determine the mechanism of the induction of the conformational change in ICP8 that occurs coincident with localization to prereplicative sites in the nucleus by defining the relationship between the conformational epitope and the DNA-binding function of ICP8, by providing biochemical evidence for a conformational change, by defining the minimal macromolecular requirements for the conformational change, by identification of host proteins that bind to specific forms of ICP8, and by mapping the conformational epitope recognized by the 39S monoclonal antibody. (3) To determine the role of ICP8 in the effects of HSV on the cell cycle by defining the function of the interaction between ICP8 and Rb by defining the sequences of ICP8 required for interaction with Rb, and isolation and characterization of a mutant virus defective for interaction of ICP8 with Rb, and by defining how HSV infection increases the level of p53 in infected cells. (4) To define the roles of ICP8 and other DNA replication proteins in regulation of viral gene expression by determining their effects on HSV gene expression from parental viral DNA templates. The integration of the results from these studies on protein assembly and regulation of gene expression should allow the formulation of a model of the mechanisms by which intranuclear localization and assembly of viral proteins and DNA affect the utilization of a DNA molecule for transcription and DNA replication. In addition, these studies should provide new understanding of nuclear replication events that could serve as targets for antiviral agents against the herpesviruses.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA026345-18
Application #
2414092
Study Section
Virology Study Section (VR)
Project Start
1979-07-01
Project End
2001-04-30
Budget Start
1997-05-01
Budget End
1998-04-30
Support Year
18
Fiscal Year
1997
Total Cost
Indirect Cost
Name
Harvard University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115
Uprichard, Susan L; Knipe, David M (2003) Conformational changes in the herpes simplex virus ICP8 DNA-binding protein coincident with assembly in viral replication structures. J Virol 77:7467-76
Taylor, Travis J; McNamee, Elizabeth E; Day, Cheryl et al. (2003) Herpes simplex virus replication compartments can form by coalescence of smaller compartments. Virology 309:232-47
Taylor, Travis J; Knipe, David M (2003) C-terminal region of herpes simplex virus ICP8 protein needed for intranuclear localization. Virology 309:219-31
Brockman, Mark A; Knipe, David M (2002) Herpes simplex virus vectors elicit durable immune responses in the presence of preexisting host immunity. J Virol 76:3678-87
Zhou, Changhong; Knipe, David M (2002) Association of herpes simplex virus type 1 ICP8 and ICP27 proteins with cellular RNA polymerase II holoenzyme. J Virol 76:5893-904
Da Costa, X J; Morrison, L A; Knipe, D M (2001) Comparison of different forms of herpes simplex replication-defective mutant viruses as vaccines in a mouse model of HSV-2 genital infection. Virology 288:256-63
McNamee, E E; Taylor, T J; Knipe, D M (2000) A dominant-negative herpesvirus protein inhibits intranuclear targeting of viral proteins: effects on DNA replication and late gene expression. J Virol 74:10122-31
Da Costa, X; Kramer, M F; Zhu, J et al. (2000) Construction, phenotypic analysis, and immunogenicity of a UL5/UL29 double deletion mutant of herpes simplex virus 2. J Virol 74:7963-71
de Bruyn Kops, A; Uprichard, S L; Chen, M et al. (1998) Comparison of the intranuclear distributions of herpes simplex virus proteins involved in various viral functions. Virology 252:162-78
Uprichard, S L; Knipe, D M (1997) Assembly of herpes simplex virus replication proteins at two distinct intranuclear sites. Virology 229:113-25

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