PhIP carcinogenicity in breast cancer: Computational and experimental evidence for competitive interactions with human estrogen receptor

Brian J. Bennion, Monique Cosman, Felice C Lightstone, Mark G. Knize, Jennifer L. Montgomery, L. Michelle Bennett, James S. Felton, Kristen S. Kulp

Research output: Contribution to journalArticle

26 Scopus citations

Abstract

Many carcinogens have been shown to cause tissue specific tumors in animal models. The mechanism for this specificity has not been fully elucidated and is usually attributed to differences in organ metabolism. For heterocyclic amines, potent carcinogens that are formed in well-done meat, the ability to either bind to the estrogen receptor and activate or inhibit an estrogenic response will have a major impact on carcinogenicity. Here, we describe our work with the human estrogen receptor alpha (ERa), the mutagenic/carcinogenic heterocyclic amines PhIP, MeIQx, and IFP, and the hydroxylated metabolite of PhIP, N 2-hydroxy-PhIP. We demonstrate both by computational docking and NMR analysis that PhIP binds with the ligand binding domain (LBD). This binding competes with estradiol (E2) in the native E2 binding cavity of the receptor. In vitro assays show that PhIP, in contrast to the other heterocyclic amines, increases cell proliferation in MCF-7 human breast cancer cells and activates the ERα receptor. We also find that other heterocyclic amines and N 2-hydroxy-PhIP inhibit ERα activation. We propose that the mechanism for the tissue-specific carcinogenicity seen in the rat breast tumors and the presumptive human breast cancer associated with the consumption of well-done meat maybe mediated by this receptor activation.

Original languageEnglish (US)
Pages (from-to)1528-1536
Number of pages9
JournalChemical Research in Toxicology
Volume18
Issue number10
DOIs
StatePublished - Oct 2005
Externally publishedYes

ASJC Scopus subject areas

  • Drug Discovery
  • Organic Chemistry
  • Chemistry(all)
  • Toxicology
  • Health, Toxicology and Mutagenesis

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