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. 1993 Apr 15;53(8):1739-42.

A structural role for metal ions in the "wild-type" conformation of the tumor suppressor protein p53

Affiliations
  • PMID: 8467489

A structural role for metal ions in the "wild-type" conformation of the tumor suppressor protein p53

P Hainaut et al. Cancer Res. .

Abstract

In human tumors, many different point mutations of the p53 gene knock out suppressor function and induce the p53 polypeptide to adopt an immunologically distinct, "mutant" conformation. Here we show that exposure to the metal chelator 1,10-phenanthroline induces wild-type p53 to adopt the mutant conformation and that this process is reversible. Conversion to mutant phenotype also occurs after exposure to (a) an organic mercurial reagent targeting cysteinyl residues and (b) low concentrations of mercury or cadmium. We propose that binding of metal ions, most probably zinc, to conserved cysteinyl residues stabilizes the tertiary structure of wild-type p53.

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