Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts

In rodents, in utero exposure to exogenous estrogens including diethylstilboestrol (DES) results in major suppression of steroidogenesis in fetal testes. Whether similar effects occur in the human fetal testis is equivocal. Based on the results of the rodent studies, we hypothesised that exposure of...

Descripción completa

Detalles Bibliográficos
Autores principales: Mitchell, Rod T., Sharpe, Richard M., Anderson, Richard A., McKinnell, Chris, Macpherson, Sheila, Smith, Lee B., Wallace, W. Hamish B., Kelnar, Christopher J. H., van den Driesche, Sander
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3631175/
https://www.ncbi.nlm.nih.gov/pubmed/23620786
http://dx.doi.org/10.1371/journal.pone.0061726
_version_ 1782266759539064832
author Mitchell, Rod T.
Sharpe, Richard M.
Anderson, Richard A.
McKinnell, Chris
Macpherson, Sheila
Smith, Lee B.
Wallace, W. Hamish B.
Kelnar, Christopher J. H.
van den Driesche, Sander
author_facet Mitchell, Rod T.
Sharpe, Richard M.
Anderson, Richard A.
McKinnell, Chris
Macpherson, Sheila
Smith, Lee B.
Wallace, W. Hamish B.
Kelnar, Christopher J. H.
van den Driesche, Sander
author_sort Mitchell, Rod T.
collection PubMed
description In rodents, in utero exposure to exogenous estrogens including diethylstilboestrol (DES) results in major suppression of steroidogenesis in fetal testes. Whether similar effects occur in the human fetal testis is equivocal. Based on the results of the rodent studies, we hypothesised that exposure of human fetal testes to DES would result in a reduction in testosterone production. We show, using a xenograft approach, that testosterone production is not reduced in human fetal testis following DES exposure. Human fetal testes (15–19 weeks’ gestation, n = 6) were xenografted into castrate male nude mice which were then treated for 35 days with vehicle or 100 µg/kg DES three times a week. For comparison, similar treatment was applied to pregnant rats from e13.5–e20.5 and effects on fetal testes evaluated at e21.5. Xenograft testosterone production was assessed by measuring host seminal vesicle (SV) weights as an indirect measure over the entire grafting period, and single measurement of serum testosterone at termination. Human fetal testis xenografts showed similar survival in DES and vehicle-exposed hosts. SV weight (44.3 v 26.6 mg, p = 0.01) was significantly increased in DES compared to vehicle-exposed hosts, respectively, indicating an overall increase in xenograft testosterone production over the grafting period, whilst serum testosterone at termination was unchanged. In contrast intra-testicular testosterone levels were reduced by 89%, in fetal rats exposed to DES. In rats, DES effects are mediated via Estrogen Receptor α (ESR1). We determined ESR1 protein and mRNA expression in human and rat fetal testis. ESR1 was expressed in rat, but not in human, fetal Leydig cells. We conclude that human fetal testis exposure to DES does not impair testosterone production as it does in rats, probably because ESR1 is not expressed in human fetal Leydig cells. This indicates that DES exposure is likely to pose minimal risk to masculinization of the human fetus.
format Online
Article
Text
id pubmed-3631175
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-36311752013-04-25 Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts Mitchell, Rod T. Sharpe, Richard M. Anderson, Richard A. McKinnell, Chris Macpherson, Sheila Smith, Lee B. Wallace, W. Hamish B. Kelnar, Christopher J. H. van den Driesche, Sander PLoS One Research Article In rodents, in utero exposure to exogenous estrogens including diethylstilboestrol (DES) results in major suppression of steroidogenesis in fetal testes. Whether similar effects occur in the human fetal testis is equivocal. Based on the results of the rodent studies, we hypothesised that exposure of human fetal testes to DES would result in a reduction in testosterone production. We show, using a xenograft approach, that testosterone production is not reduced in human fetal testis following DES exposure. Human fetal testes (15–19 weeks’ gestation, n = 6) were xenografted into castrate male nude mice which were then treated for 35 days with vehicle or 100 µg/kg DES three times a week. For comparison, similar treatment was applied to pregnant rats from e13.5–e20.5 and effects on fetal testes evaluated at e21.5. Xenograft testosterone production was assessed by measuring host seminal vesicle (SV) weights as an indirect measure over the entire grafting period, and single measurement of serum testosterone at termination. Human fetal testis xenografts showed similar survival in DES and vehicle-exposed hosts. SV weight (44.3 v 26.6 mg, p = 0.01) was significantly increased in DES compared to vehicle-exposed hosts, respectively, indicating an overall increase in xenograft testosterone production over the grafting period, whilst serum testosterone at termination was unchanged. In contrast intra-testicular testosterone levels were reduced by 89%, in fetal rats exposed to DES. In rats, DES effects are mediated via Estrogen Receptor α (ESR1). We determined ESR1 protein and mRNA expression in human and rat fetal testis. ESR1 was expressed in rat, but not in human, fetal Leydig cells. We conclude that human fetal testis exposure to DES does not impair testosterone production as it does in rats, probably because ESR1 is not expressed in human fetal Leydig cells. This indicates that DES exposure is likely to pose minimal risk to masculinization of the human fetus. Public Library of Science 2013-04-19 /pmc/articles/PMC3631175/ /pubmed/23620786 http://dx.doi.org/10.1371/journal.pone.0061726 Text en © 2013 Mitchell et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Mitchell, Rod T.
Sharpe, Richard M.
Anderson, Richard A.
McKinnell, Chris
Macpherson, Sheila
Smith, Lee B.
Wallace, W. Hamish B.
Kelnar, Christopher J. H.
van den Driesche, Sander
Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts
title Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts
title_full Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts
title_fullStr Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts
title_full_unstemmed Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts
title_short Diethylstilboestrol Exposure Does Not Reduce Testosterone Production in Human Fetal Testis Xenografts
title_sort diethylstilboestrol exposure does not reduce testosterone production in human fetal testis xenografts
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3631175/
https://www.ncbi.nlm.nih.gov/pubmed/23620786
http://dx.doi.org/10.1371/journal.pone.0061726
work_keys_str_mv AT mitchellrodt diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT sharperichardm diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT andersonricharda diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT mckinnellchris diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT macphersonsheila diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT smithleeb diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT wallacewhamishb diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT kelnarchristopherjh diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts
AT vandendrieschesander diethylstilboestrolexposuredoesnotreducetestosteroneproductioninhumanfetaltestisxenografts

Ejemplares similares