Abstract

Several countries have experienced rises in cryptorchidisms, hypospadias and testicular germ cell cancer. The reasons for these trends are largely unknown, but Skakkebaek has proposed that these disorders form a testicular dysgenesis syndrome and can be traced to androgen insufficiency in foetal life. This suggests that antiandrogenic chemicals might contribute to risks, but few chemicals have been linked to these diseases in epidemiological studies. In animal studies with p,p ′-dichlorodiphenyldichloroethylene, effects typical of disruptions of male sexual differentiation became apparent when the foetal levels of this androgen receptor (AR) antagonist approached values associated with responses in in vitro assays. This prompted us to analyse whether the 22 chemicals with AR antagonistic properties would produce mixture effects in an in vitro AR antagonism assay when combined at concentrations found in human serum. Other antiandrogenic modalities could not be considered. Two scenarios were investigated, one representative of average serum levels reported in European countries, the other in line with levels towards the high exposures. In both situations, the in vitro potency of the 22 selected AR antagonists was too low to produce combined AR antagonistic effects at the concentrations found in human serum, although the high exposure scenario came quite close to measurable effects. Nevertheless, our analysis exposes an explanation gap which can only be bridged by conjuring up as yet undiscovered high potency AR antagonists or, alternatively, high exposures to unknown agents of average potency.

Highlights

  • In recent years, several countries have experienced increases in the incidence of cryptorchisms (reviewed by Main et al (2010)) and hypospadias (Pierik et al 2002, Boisen et al 2005, Nelson et al 2005, Nassar et al 2007), the most frequent congenital malformations in young boys

  • We identified 22 chemicals for which both human tissue levels and concentration–response relationships for androgen receptor (AR) antagonism in vitro were available (Table 1) and assessed whether measurable combination effects are to be expected in the MDA-kb2 assay, when AR antagonists are combined at levels measured in human tissues

  • For the 22 chemicals listed in Table 1, we recorded concentration–response relationships for AR antagonism in the MDA-kb2 gene reporter assay (Fig. 2)

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Summary

Introduction

Several countries have experienced increases in the incidence of cryptorchisms (reviewed by Main et al (2010)) and hypospadias (Pierik et al 2002, Boisen et al 2005, Nelson et al 2005, Nassar et al 2007), the most frequent congenital malformations in young boys. The incidence of testicular germ cell cancers has risen steadily in Caucasian white men (Chia et al 2010) and is the most commonly. The meeting was supported by the Danish Ministry of the Environment – Environmental Protection Agency as an activity under the Danish Centre on Endocrine Disrupters. Publication of this special issue has been supported by the Society for Reproduction and Fertility. The opinions or views expressed in this special issue are those of the authors, and do not necessarily reflect the opinions or recommendations of the Danish Ministry of the Environment – Environmental Protection Agency or the Society for Reproduction and Fertility. The Guest Editors for this special issue were Anna-Maria Andersson, Hanne Frederiksen, Niels Erik Skakkebæk, Rigshospitalet, Denmark, Kenneth M Grigor, Western General Hospital, Edinburgh, UK and Jorma Toppari, University of Turku, Finland

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