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Rapid killing of urothelial carcinoma-cells by wild-type p53
Authors:Makri D  Schulz W  Grimm M  Schmitzdrager B
Affiliation:UNIV DUSSELDORF,INST PHYSIOL CHEM 1,D-40001 DUSSELDORF,GERMANY. UNIV DUSSELDORF,UROL KLIN,D-40001 DUSSELDORF,GERMANY.
Abstract:The effect of the tumor suppressor p53 on urothelial carcinoma cells was studied by transfecting six cell lines containing different mutations in the p53 gene with an expression construct for the wild-type protein. In all cell lines, the number of cell clones resistant to a neomycin analogue was strongly diminished when pCMVhup53 was cotransfected with the resistance plasmid pRSVneo as compared to cotransfection with either a plasmid vector, a p53 deletion and a mutant p53 expression vector. Cytochemical analysis showed that cells cotransfected with pCMVhup53 and an expression plasmid for beta-galactosidase disappeared during the second day after transfection. Thus, reexpression of wildtype p53 efficiently and rapidly kills urothelial carcinoma cells, independent of the different mutations in p53 they contain.
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