Mol Cell Biol. 1994 February; 14(2): 1171-1178
Physical and functional interaction between wild-type p53 and mdm2 proteins.
D S Haines,
J E Landers,
L J Engle and
D L George
Department of Genetics, University of Pennsylvania School of Medicine, Philadelphia 19104.
ABSTRACT
The mdm2 oncogene, which is often amplified in mammalian tumors, produces a number of transcripts that encode distinct protein forms. Previous studies demonstrating that overexpression of the mdm2 gene can activate its transforming potential, and can inhibit the transcriptional activation function of p53, prompted us to begin to explore possible functional differences among the various mdm2 products. Utilizing a transient transfection assay, we have evaluated four naturally occurring murine mdm2 forms for their ability to inhibit p53-mediated transcriptional activation of reporter genes regulated by p53 response elements. Three of these mdm2 forms were found to physically associate with the wild-type p53 protein and to possess the ability to inhibit its transactivation function. A fourth form failed to exhibit either of these functions. This last mdm2 form lacks the N-terminal protein domain that is present in the other three splice forms examined, pointing to this region as one that is critical for complex formation with the p53 protein. Identifying such differences among mdm2 proteins provides important clues for dissecting their functional domains, and emphasizes that defining the individual properties of these products will be critical in elucidating the overall growth control function of the mdm2 gene.
Mol Cell Biol. 1994 February; 14(2): 1171-1178
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Copyright © 1994 by the American Society for Microbiology. All rights reserved.