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S.R. Milligan, A.V. Balasubramanian, and J.C. Kalita

Physiology, Biomedical Sciences Division, King's College, London, United Kingdom

Abstract

The in vivo effects of xenoestrogens are of interest in relation to their potential health risks and/or beneficial effects on humans and animals. However, the apparent in vivo potency of the examined response can be confounded by a short half-life, and the metabolism of estrogens is very dependent on the nature of conversion and/or inactivation. To minimize such variables, we examined the estrogenic potency of a range of xenoestrogens in an acute in vivo assay--the stimulation of increased uterine vascular permeability in ovariectomized mice 4 hr after subcutaneous administration. While estradiol (E ₂ ) and estriol (E ₃ ; a relatively weak natural estrogen) readily induced vascular responses [median effective dose (ED ₅₀ ) <10 ^-9 mol], much higher amounts of xenoestrogens were required. Bisphenol A was about 10,000-fold less potent than E ₂ and E ₃ , and octylphenol and nonylphenol were about 100,000-fold less potent ; dioctyl phthalate, benzyl butyl phthalate, dibutyl phthalate, and trichlorinated biphenol produced no effect. Coumestrol was the most active phytoestrogen, with an ED ₅₀ between 10 ^-6 and 10 ^-7 mol ; genistein was about 10-fold less potent than coumestrol, and neither daidzein nor formononetin produced any marked effect, even at doses up to 10 ^-5 mol. All increases in vascular permeability could be blocked by the pure antiestrogen ICI 182,780. There was no evidence that any of the compounds could act as an antiestrogen in this assay or that they could exert synergistic effects in combination. These results indicate that even short-term exposure to most of the xenobiotic estrogens can induce typical estrogenic effects in vivo , but their estrogenic potency is very weak even when assessed in an acute response. Key words : environmental estrogens, phytoestrogens, uterus, vascular permeability, xenobiotic.

Environ Health Perspect 106:23-26 (1998) . [Online 2 January 1998]
http://ehpnet1.niehs.nih.gov/docs/1998/106p23-26milligan/ abstract.html

Address correspondence to S.R. Milligan, Physiology, Biomedical Sciences Division, King's College, Strand, London, WC2R 2LS, United Kingdom.

We are grateful to the Medical Research Council for support. J.C.K., a Commonwealth scholar from India, was supported by the British Council.

Received 10 June 1997 ; accepted 11 September 1997.