Catechol estrogen metabolites and conjugates in mammary tumors and hyperplastic tissue from estrogen receptor-{alpha} knock-out (ERKO)/Wnt-1 mice: implications for initiation of mammary tumors

doi:10.1093/carcin/22.9.1573

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Carcinogenesis, Vol. 22, No. 9, 1573-1576, September 2001
© 2001 Oxford University Press

SHORT COMMUNICATION

Catechol estrogen metabolites and conjugates in mammary tumors and hyperplastic tissue from estrogen receptor- ${alpha}$ knock-out (ERKO)/Wnt-1 mice: implications for initiation of mammary tumors

Prabu Devanesan¹, Richard J. Santen², Wayne P. Bocchinfuso³, Kenneth S. Korach³, Eleanor G. Rogan¹ and Ercole Cavalieri¹^,4

¹ Eppley Institute for Research in Cancer and Allied Diseases, University of Nebraska Medical Center, Omaha, NE 68198-6085,
² Division of Hematology, Oncology and Endocrinology, Cancer Center, University of Virginia Health Science Center, Charlottesville, VA 22908 and
³ Receptor Biology Section, Laboratory of Reproductive and Developmental Toxicology, National Institute of Environmental Health Sciences, NIH, Research Triangle Park, NC 27709, USA

A novel model of breast cancer was established by crossing micecarrying the Wnt-1 transgene (100% of adult females developspontaneous mammary tumors) with the ERKO mouse line, in whichmammary tumors develop despite a lack of functional estrogenreceptor- ${alpha}$ . To begin investigating whether metabolite-mediatedgenotoxicity of estrogens may play an important role in theinitiation of mammary tumors, the pattern of estrogen metabolitesand conjugates was examined in ERKO/Wnt-1 mice. Extracts ofhyperplastic mammary tissue and mammary tumors were analyzedby HPLC with identification and quantification of compoundsby multichannel electrochemical detection. Picomole amountsof the 4-catechol estrogens (CE) were detected, but their methoxyconjugates, as well as the 2-CE and their methoxy conjugates,were not. 4-CE conjugates with glutathione or its hydrolyticproducts (cysteine and N-acetylcysteine) were detected in picomoleamounts in both tumors and hyperplastic mammary tissue, demonstratingthe formation of CE-3,4-quinones. These preliminary findingsshow that the estrogen metabolite profile in the mammary tissueis unbalanced, in that the normally minor 4-CE metabolites weredetected in the mammary tissue and not the normally predominant2-CE. These results are consistent with the hypothesis thatthe mammary tumor development is primarily initiated by metabolismof estrogens to 4-CE and, then, to CE-3,4-quinones, which mayreact with DNA to induce oncogenic mutations.

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Carcinogenesis

SHORT COMMUNICATION

Catechol estrogen metabolites and conjugates in mammary tumors and hyperplastic tissue from estrogen receptor- knock-out (ERKO)/Wnt-1 mice: implications for initiation of mammary tumors

Catechol estrogen metabolites and conjugates in mammary tumors and hyperplastic tissue from estrogen receptor- ${alpha}$ knock-out (ERKO)/Wnt-1 mice: implications for initiation of mammary tumors