Genistein Stimulates Growth of Human Breast Cancer Cells in a Novel, Postmenopausal Animal Model, with Low Plasma Estradiol Concentrations

Overview

Journal Carcinogenesis

Specialty Oncology

Date 2006 Mar 16

PMID 16537557

Citations 32

Authors

Young H Ju

Kimberly F Allred

Clinton D Allred

William G Helferich

Affiliations

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Abstract

We have demonstrated that genistein (GEN) stimulates growth of estrogen-dependent breast tumors in vivo. In this study, we evaluated whether dietary GEN can act in an additive manner with low circulating levels of 17beta-estradiol (E2). We developed an E2 delivery system using silastic implants that yield low circulating plasma E2 levels similar to those observed in postmenopausal women. We inserted various concentrations of E2 silastic implants (1:127, 1:63, 1:31, 1:15 and 1:7 = E2:cholesterol) and injected estrogen-dependent human breast cancer (MCF-7) cells into ovariectomized athymic mice. The E2 implants tested (1:127-1:7) generated 30.1-101.6 pM E2 in plasma, which is comparable to the E2 levels observed in postmenopausal women. The E2 implants stimulated MCF-7 tumor growth in a dose-dependent manner. We selected the 1:31 ratio of E2 implant to evaluate if dietary GEN acts in an additive manner with low E2 levels to influence the growth of MCF-7 tumors. Ovariectomized mice were divided into four groups: MCF-7 control, 500 ppm GEN, 1:31 E2, and 1:31 E2 + 500 ppm GEN. At week 17, the average tumor sizes were 7.6, 32.1, 67.4 and 106.8 mm2 for these groups, respectively (P < 0.05), demonstrating that 500 ppm GEN additively stimulated MCF-7 tumor growth in the presence of low levels of E2. In summary, we established a preclinical mouse model that results in E2 blood concentrations similar to those found in postmenopausal women. Further, we observed that these concentrations regulate the growth rate of MCF-7 breast tumors. Using this model, we demonstrated that dietary GEN in the presence of low levels of circulating E2 act in an additive manner to stimulate estrogen-dependent tumor growth in vivo. Results from this study suggest that consumption of products containing GEN may not be safe for postmenopausal women with estrogen-dependent breast cancer.

Citing Articles

Inflammation Factors and Genistein Supplementation in Cancer-Preliminary Research.

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PMID: 38534756 PMC: 10968949. DOI: 10.3390/cimb46030140.

Can genistein be a potential agent against skin side effects associated with the treatment of breast cancer?.

Pawlicka M, Filip A Postepy Dermatol Alergol. 2022; 39(1):7-12.

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Role of dietary fat on obesity-related postmenopausal breast cancer: insights from mouse models and methodological considerations.

Tan P, Teng K Breast Cancer. 2021; 28(3):556-571.

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Proteins from with selective apoptotic cytotoxicity towards MCF7 cell line and suppresses MCF7-xenograft tumor growth.

Kong B, Teoh K, Tan N, Tan C, Ng S, Fung S PeerJ. 2020; 8:e9650.

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Beyond the Antioxidant Activity of Dietary Polyphenols in Cancer: the Modulation of Estrogen Receptors (ERs) Signaling.

Cipolletti M, Solar Fernandez V, Montalesi E, Marino M, Fiocchetti M Int J Mol Sci. 2018; 19(9).

PMID: 30189583 PMC: 6165334. DOI: 10.3390/ijms19092624.