Maturitas
Volume 56, Issue 2 , Pages 142-152, 20 February 2007

Differential effects of progestogens, by type and regimen, on estrogen-metabolizing enzymes in human breast cancer cells

Department of Obstetrics and Gynecology, Kyoto Prefectural University of Medicine, Graduate School of Medical Science, 465 Kajii-cho, Kamigyo-ku, Kyoto 602-8566, Japan

Received 15 March 2006; received in revised form 30 June 2006; accepted 5 July 2006. published online 10 August 2006.

Abstract 

Objectives

To investigate the in vitro effects of five progestogens commonly used in hormone replacement therapy (HRT) on estrogen-metabolizing enzymes in human breast cancer cells.

Methods

The human hormone-dependent breast cancer cell lines T47D, MCF-7, and MCF-7aro were cultured with estradiol (E2) and progestogens. The mRNA levels of estrogen-metabolizing enzymes were determined by RT-PCR or Northern blot, and enzyme activities by radiolabeled substrates. Cell proliferation was measured by bromodeoxyuridine incorporation. In vitro models for continuous combined regimen (CCR) and sequential combined regimen (SCR) were established to mimic the in vivo conditions of HRT.

Results

Medroxyprogesterone acetate (MPA) plus E2 (10−8M) stimulated the mRNA levels and activities of estrogen-activating enzymes aromatase (at 10−8M MPA), 17β-hydroxysteroid dehydrogenase type 1 (17βHSD1) (at 10−6M), and sulfatase (at 10−8 to 10−6M) compared to E2 only. Progesterone also stimulated enzyme activity, but to a lower magnitude. Levonorgestrel, norethindrone, and dienogest showed no enzyme stimulation. The estrogen-inactivating enzymes 17β-hydroxysteroid dehydrogenase type 2 and sulfotransferase were not affected by any of the progestogens tested. However, all the progestogens (at 10−8 to 10−6M) inhibited E2-stimulated cell proliferation. While increased aromatase and 17βHSD1 activities were observed in the CCR model, no significant enzyme stimulation was observed in the SCR model.

Conclusions

The present study suggested that progestogens exert different actions on estrogen-metabolizing enzymes in breast cancer cells dependent on the specific progestogen and regimen used. Further studies are needed to elucidate whether MPA, a progestogen currently used in HRT, leads to a higher risk of breast cancer development than other progestogens.

Keywords: Hormone replacement therapy, Breast cancer cells, Progestogen, Estrogen-metabolizing enzyme

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PII: S0378-5122(06)00272-6

doi:10.1016/j.maturitas.2006.07.003

Maturitas
Volume 56, Issue 2 , Pages 142-152, 20 February 2007

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