Abstract

The overall aims of these studies are to define the funcitons performed by Simian Virus 40 (SV40) large T antigen and to determine the domains of the polypeptide involved in different functions. During the next project period, studies will be focused on two major questions: 1. What is the nature of the host range/helper function (hr/hf) activity of T antigen? This function is provide by the C-terminal 35 amino acids of large T. Hr/hf mutants are most defective in CV-lP and grow best in Vero monkey kidney cells. Mutants lacking this function are positive for viral DNA replication but have defects in viral late gene expression. Translation of viral mRNAs is most affected, but other steps in the infection cycle are also affected. Mutants are also defective for adenovirus helper function. Proposed studies will investigate the possibility that the hr/hf defect affects an SV40 response to interferon or to activation of enogenous P1/eIF2-alpha kinase. Patterns of macromolecular synthesis in mutant-infected cells will be examined further, particularly the structures of mutant late mRNAs and the levels of phosphorylation of capsid protein VP1. Other studies will determine whether various adenovirus or polymavirus functions can compensate for the hr/hf defect and whether SV40 gene products other than the C-terminus of T can enhance adenovirus growth in CV-1P monkey cells. Second-site revertants of hr/hf mutants will be isolated and characterized. 2. What is the relationship between T antigen's ability to stimulate host DNA replication and other activities of T antigen? The ability of mutants of SV40 to induce host cell DNA replication will be determined by microinjection of mutant genome into quiescent primary cultures of rodent cells and established rodent cell lines. Initially, mutants with small deletions and linker insertions will be used. Subsequent studies will use point mutants. Additional studies will be performed to determine whether T antigen's ability to induce host DNA synthesis co-segregates with its activities in viral DNA replication, transactivation of gene expression from the SV40 late and RSV LTR promoters, immortalizaton of primary rodent cells, and malignant transformation of established cell lines.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA039259-08
Application #
3178104
Study Section
Virology Study Section (VR)
Project Start
1985-04-01
Project End
1993-03-31
Budget Start
1992-04-01
Budget End
1993-03-31
Support Year
8
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Dartmouth College
Department
Type
Schools of Medicine
DUNS #
041027822
City
Hanover
State
NH
Country
United States
Zip Code
03755

  Publications

Conzen, S D; Snay, C A; Cole, C N (1997) Identification of a novel antiapoptotic functional domain in simian virus 40 large T antigen. J Virol 71:4536-43
Anderson, M M; Chen, J; Cole, C N et al. (1996) Activation of the human thymidine kinase (TK) promoter by simian virus 40 large T antigen requires both the T antigen pRb family-binding domain and TK promoter sequences resembling E2F-binding sites. J Virol 70:6304-13
Del Sal, G; Ruaro, E M; Utrera, R et al. (1995) Gas1-induced growth suppression requires a transactivation-independent p53 function. Mol Cell Biol 15:7152-60
Conzen, S D; Cole, C N (1995) The three transforming regions of SV40 T antigen are required for immortalization of primary mouse embryo fibroblasts. Oncogene 11:2295-302
Rajan, P; Swaminathan, S; Zhu, J et al. (1995) A novel translational regulation function for the simian virus 40 large-T antigen gene. J Virol 69:785-95
Feldherr, C; Cole, C; Lanford, R E et al. (1994) The effects of SV40 large T antigen and p53 on nuclear transport capacity in BALB/c 3T3 cells. Exp Cell Res 213:164-71
Rice, P W; Cole, C N (1993) Efficient transcriptional activation of many simple modular promoters by simian virus 40 large T antigen. J Virol 67:6689-97
Zhu, J; Rice, P W; Gorsch, L et al. (1992) Transformation of a continuous rat embryo fibroblast cell line requires three separate domains of simian virus 40 large T antigen. J Virol 66:2780-91
Heath, C V; Fanning, E; Cole, C N (1992) Adenovirus helper function activity of simian virus 40 T antigen mutants. Virology 189:762-5
Zhu, J Y; Abate, M; Rice, P W et al. (1991) The ability of simian virus 40 large T antigen to immortalize primary mouse embryo fibroblasts cosegregates with its ability to bind to p53. J Virol 65:6872-80

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