Identification of the p53 protein domain involved in formation of the simian virus 40 large T-antigen-p53 protein complex.

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J Virol. 1986 September; 59(3): 574-583

Identification of the p53 protein domain involved in formation of the simian virus 40 large T-antigen-p53 protein complex.

T H Tan, J Wallis and A J Levine

ABSTRACT

An expression vector utilizing the enhancer and promoter regionof the simian virus 40 (SV40) DNA regulating a murine p53 cDNAclone was constructed. The vector produced murine p53 proteinin monkey cells identified by five different monoclonal antibodies,three of which were specific for the murine form of p53. Themurine p53 produced in monkey cells formed an oligomeric proteincomplex with the SV40 large tumor antigen. A large number ofdeletion mutations, in-frame linker insertion mutations, andlinker insertion mutations resulting in a frameshift mutationwere constructed in the cDNA coding portion of the p53 proteinexpression vector. The wild-type and mutant p53 cDNA vectorswere expressed in monkey cells producing the SV40 large T antigen.The conformation and levels of p53 protein and its ability toform protein complexes with the SV40 T antigen were determinedby using five different monoclonal antibodies with quite distinctepitope recognition sites. Insertion mutations between aminoacid residues 123 and 215 (of a total of 390 amino acids) eliminatedthe ability of murine p53 to bind to the SV40 large T antigen.Deletion (at amino acids 11 through 33) and insertion mutations(amino acids 222 through 344) located on either side of thisT-antigen-binding protein domain produced a murine p53 proteinthat bound to the SV40 large T antigen. The same five insertionmutations that failed to bind with the SV40 large T antigenalso failed to react with a specific monoclonal antibody, PAb246.In contrast, six additional deletion and insertion mutationsthat produced p53 protein that did bind with T antigen wereeach recognized by PAb246. The proposed epitope for PAb246 hasbeen mapped adjacent (amino acids 88 through 109) to the T-antigen-bindingdomain (amino acids 123 through 215) localized by the mutationsmapped in this study. Finally, some insertion mutations thatproduced a protein that failed to bind to the SV40 T antigenappeared to have an enhanced ability to complex with a 68-kilodaltoncellular protein in monkey cells.

J Virol. 1986 September; 59(3): 574-583

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