Potent inhibition of estrogen sulfotransferase by hydroxylated PCB metabolites: a novel pathway explaining the estrogenic activity of PCBs.

Monique H A Kester,Walter Meinl,Michael W H Coughtrie,Theo J Visser,Stephen H Safe,Charles N Falany,Abraham Brouwer,A Gerlienke Schuur,Dick Tibboel,Hansruedi Glatt,Sema Bulduk,George G J M Kuiper,Ake Bergman

doi:10.1210/endo.141.5.7530

Potent inhibition of estrogen sulfotransferase by hydroxylated PCB metabolites: a novel pathway explaining the estrogenic activity of PCBs.

Monique H A Kester, Walter Meinl + Show 11 more

Open Access

https://doi.org/10.1210/endo.141.5.7530

Copy DOI

Journal: EndocrinologyJN	Publication Date: Jan 1, 2000
Citations: 352

Affiliation: German Institute of Human Nutrition, University of Dundee, Texas A&M University, University of Alabama, Stockholm University, Erasmus University Rotterdam

#Hydroxylated Polychlorinated Biphenyls Metabolites #Polychlorinated Biphenyls + Show 8 more

Abstract
Full-Text PDF
Similar Papers

Abstract

Polychlorinated biphenyls (PCBs) are persistent environmental pollutants which exert a variety of toxic effects in animals, including disturbances of sexual development and reproductive function. The estrogenic effects of PCBs may be mediated in part by hydroxylated PCB metabolites (PCB-OHs), but the mechanisms by which they are brought about are not understood. PCBs as well as PCB-Hs show low affinities for both alpha and beta estrogen receptor isoforms. In the present study we demonstrate that various environmentally relevant PCB-OHs are extremely potent inhibitors of human estrogen sulfotransferase, strongly suggesting that they indirectly induce estrogenic activity by increasing estradiol bioavailability in target tissues.

Full Text