Abstract

The objective of the research is to continue to use the estrogen-induced carcinomas in hamster kidney and liver as experimental models to elucidate the mechanisms whereby estrogens, both natural and synthetic, ellicit tumorigenesis in the hamster. We have concluded that in addition to their hormonal properties, estrogen possess carcinogenic properties which can be partially dissociated from the former. To elucidate more precisely the role estrogens play in causing these carcinomas, the following studies are proposed. 1) At present, the most plausible reactive intermediates which might be involved in neoplastic changes in hamster kidney are the arene oxides and o-quinones of the catechol pathway. To test this hypothesis, 2- and 4- hydroxyestrogens will be synthesized and their carcinogenic activities assessed in the hamster kidney. U-0521, an inhibitor of COMT will be used concomitantly with DES or 17Beta-estradiol in an effort to potentiate the carcinogenic effects of these estrogens and to discern the significance of the proposed catechol pathway in estrogen carcinogenesis. Modified steroidal estrogens (deoxoestrone, 11Beta-methoxy, 11Beta-methy and 11Beta-ethyl) will be prepared to further elucidate the significance of the catechol pathway in renal tumorigenesis. 2) We propose to attempt to indirectly identify the presence of arene oxide formation by observing an NIH-shift with the aid of epoxide hydrolase inhibitor, TCPO, and employing the estrogen hydroxylase assay. 3) We will continue our assessment of estrogen-2/-4 hydroxylase activity and formation of catechol estrogens, particularly in regard to 2 hydroxyestrogen formation using HPLC analyses. COMT and demethylase activities will also be assessed and their substrate specificity determined. These latter enzymes will provide more precise information regarding the in-vivo concentration of catechol estrogens in these tissues. 4) Prevention of estrogen-induced renal tumorigenesis in the hamster by androgens, progestins, or antiestrogens may be mediated in part by nonhormonal mechanisms by inhibiting catechol estrogen formation and hence arene oxide and oquinone amounts. This hypothesis will be tested employing estrogen hydroxylase assay with hormonally treated microsomes. 5) The P-450 MMM will be examined in detail in the untreated kidney and liver, and nonhormonal probes (Beta-NF, AlphaNF and 3-MC) will be used to perturb the P-450 MMM activities to determine alterations which may occur in estrogen metabolism. 6) The nature of the induction of liver tumors with Alpha-NF/estrogen treatment will be studied to rigorously identity the metabolites formed by [14C]-17Beta-E2 and DES in hamster liver and kidney.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA022008-14
Application #
3165693
Study Section
Chemical Pathology Study Section (CPA)
Project Start
1977-09-01
Project End
1992-11-30
Budget Start
1990-12-06
Budget End
1991-11-30
Support Year
14
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Washington State University
Department
Type
Schools of Pharmacy
DUNS #
041485301
City
Pullman
State
WA
Country
United States
Zip Code
99164

  Publications

Liao, D Z; Hou, X; Bai, S et al. (2000) Unusual deregulation of cell cycle components in early and frank estrogen-induced renal neoplasias in the Syrian hamster. Carcinogenesis 21:2167-73
Hou, X; Li, J J; Chen, W et al. (1996) Estrogen-induced proto-oncogene and suppressor gene expression in the hamster kidney: significance for estrogen carcinogenesis. Cancer Res 56:2616-20
Li, J J; Li, S A; Oberley, T D et al. (1995) Carcinogenic activities of various steroidal and nonsteroidal estrogens in the hamster kidney: relation to hormonal activity and cell proliferation. Cancer Res 55:4347-51
Gonzalez, A; Oberley, T D; Schultz, J L et al. (1993) In vitro characterization of estrogen induced Syrian hamster renal tumors: comparison with an immortalized cell line derived from diethylstilbestrol-treated adult hamster kidney. In Vitro Cell Dev Biol Anim 29A:562-73
Oberley, T D; Gonzalez, A; Lauchner, L J et al. (1991) Characterization of early kidney lesions in estrogen-induced tumors in the Syrian hamster. Cancer Res 51:1922-9
Oberley, T D; Allen, R G; Schultz, J L et al. (1991) Antioxidant enzymes and steroid-induced proliferation of kidney tubular cells. Free Radic Biol Med 10:79-83
Li, J J; Li, S A (1990) Estrogen carcinogenesis in hamster tissues: a critical review. Endocr Rev 11:524-31
Li, S A; Purdy, R H; Li, J J (1989) Variations in catechol O-methyltransferase activity in rodent tissues: possible role in estrogen carcinogenicity. Carcinogenesis 10:63-7
Tse, J; Goldfarb, S; Pugh, T D (1989) Autoradiographic evidence of estrogen binding sites in nuclei of diethylstilbesterol induced hamster renal carcinomas. Carcinogenesis 10:957-9
Gonzalez, A; Oberley, T D; Li, J J (1989) Morphological and immunohistochemical studies of the estrogen-induced Syrian hamster renal tumor: probable cell of origin. Cancer Res 49:1020-8

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