The amino-terminal functions of the simian virus 40 large T antigen are required to overcome wild-type p53-mediated growth arrest of cells.

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J Virol. 1994 March; 68(3): 1334-1341

The amino-terminal functions of the simian virus 40 large T antigen are required to overcome wild-type p53-mediated growth arrest of cells.

R S Quartin, C N Cole, J M Pipas and A J Levine

Department of Molecular Biology, Princeton University, New Jersey 08544-1014.

ABSTRACT

High levels of the p53 tumor suppressor protein can block progressionthrough the cell cycle. A model system for the study of themechanism of action of wild-type p53 is a cell line (T64-7B)derived from rat embryo fibroblasts transformed by activatedras and a temperature-sensitive murine p53 gene. At 37 to 39degrees C, the murine p53 protein is in a mutant conformationand the cells actively divide, whereas at 32 degrees C, theprotein has a wild-type conformation and the cells arrest inthe G1 phase of the cell cycle. Wild-type simian virus 40 largeT antigen and a variety of T-antigen mutants were assayed forthe ability to bypass the cell cycle block effected by the wild-typep53 protein to induce colony formation at 32 degrees C. Theresults indicate that two functions within the amino terminusof T antigen are essential to induce cell growth: (i) the abilityto bind to the retinoblastoma protein, Rb, and (ii) the presenceof a domain in the first exon that appears to interact withthe cellular protein, p300. Thus, the cell cycle arrest triggeredby wild-type p53 may be overcome by formation of a T-antigencomplex with Rb, p300, or both that could then function to eitherremove p53-mediated negative growth regulatory signals or promotea positive cell growth signal. Surprisingly, T antigen-p53 complexesare not required to overcome the temperature-sensitive p53 blockto the cell cycle in these cells. These data suggest that simianvirus 40 T antigen associated with Rb, p300, or both proteinscan communicate in a cell with the functions of the wild-typep53 protein.

J Virol. 1994 March; 68(3): 1334-1341

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