Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein

BACKGROUND: Embryo implantation relies on precise hormonal regulation, associated gene expression changes, and appropriate female reproductive tract tissue architecture. Female mice exposed neonatally to the phytoestrogen genistein (GEN) at doses similar to those in infants consuming soy-based infan...

Descripción completa

Detalles Bibliográficos
Autores principales: Jefferson, Wendy N., Padilla-Banks, Elizabeth, Suen, Alisa A., Royer, Lindsey J., Zeldin, Sharon M., Arora, Ripla, Williams, Carmen J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Environmental Health Perspectives 2020
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7138129/
https://www.ncbi.nlm.nih.gov/pubmed/32186404
http://dx.doi.org/10.1289/EHP6336
_version_ 1783518536855977984
author Jefferson, Wendy N.
Padilla-Banks, Elizabeth
Suen, Alisa A.
Royer, Lindsey J.
Zeldin, Sharon M.
Arora, Ripla
Williams, Carmen J.
author_facet Jefferson, Wendy N.
Padilla-Banks, Elizabeth
Suen, Alisa A.
Royer, Lindsey J.
Zeldin, Sharon M.
Arora, Ripla
Williams, Carmen J.
author_sort Jefferson, Wendy N.
collection PubMed
description BACKGROUND: Embryo implantation relies on precise hormonal regulation, associated gene expression changes, and appropriate female reproductive tract tissue architecture. Female mice exposed neonatally to the phytoestrogen genistein (GEN) at doses similar to those in infants consuming soy-based infant formulas are infertile due in part to uterine implantation defects. OBJECTIVES: Our goal was to determine the mechanisms by which neonatal GEN exposure causes implantation defects. METHODS: Female mice were exposed to GEN on postnatal days (PND)1–5 and uterine tissues collected on PND5, PND22–26, and during pregnancy. Analysis of tissue weights, morphology, and gene expression was performed using standard histology, confocal imaging with three-dimensional analysis, real-time reverse transcription polymerase chain reaction (real-time RT-PCR), and microarrays. The response of ovariectomized adults to [Formula: see text] (E2) and artificial decidualization were measured. Leukemia inhibitory factor (LIF) injections were given intraperitoneally and implantation sites visualized. Gene expression patterns were compared with curated data sets to identify upstream regulators. RESULTS: GEN-exposed mice exhibited reduced uterine weight gain in response to E2 treatment or artificial decidualization compared with controls; however, expression of select hormone responsive genes remained similar between the two groups. Uteri from pregnant GEN-exposed mice were posteriorized and had reduced glandular epithelium. Implantation failure was not rescued by LIF administration. Microarray analysis of GEN-exposed uteri during early pregnancy revealed significant overlap with several conditional uterine knockout mouse models, including Foxa2, Wnt4, and Sox17. These models exhibit reduced endometrial glands, features of posteriorization and implantation failure. Expression of Foxa2, Wnt4, and Sox17, as well as genes important for neonatal uterine differentiation (Wnt7a, Hoxa10, and Msx2), were severely disrupted on PND5 in GEN-exposed mice. DISCUSSION: Our findings suggest that neonatal GEN exposure in mice disrupts expression of genes important for uterine development, causing posteriorization and diminished gland function during pregnancy that contribute to implantation failure. These findings could have implications for women who consumed soy-based formulas as infants. https://doi.org/10.1289/EHP6336
format Online
Article
Text
id pubmed-7138129
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Environmental Health Perspectives
record_format MEDLINE/PubMed
spelling pubmed-71381292020-04-09 Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein Jefferson, Wendy N. Padilla-Banks, Elizabeth Suen, Alisa A. Royer, Lindsey J. Zeldin, Sharon M. Arora, Ripla Williams, Carmen J. Environ Health Perspect Research BACKGROUND: Embryo implantation relies on precise hormonal regulation, associated gene expression changes, and appropriate female reproductive tract tissue architecture. Female mice exposed neonatally to the phytoestrogen genistein (GEN) at doses similar to those in infants consuming soy-based infant formulas are infertile due in part to uterine implantation defects. OBJECTIVES: Our goal was to determine the mechanisms by which neonatal GEN exposure causes implantation defects. METHODS: Female mice were exposed to GEN on postnatal days (PND)1–5 and uterine tissues collected on PND5, PND22–26, and during pregnancy. Analysis of tissue weights, morphology, and gene expression was performed using standard histology, confocal imaging with three-dimensional analysis, real-time reverse transcription polymerase chain reaction (real-time RT-PCR), and microarrays. The response of ovariectomized adults to [Formula: see text] (E2) and artificial decidualization were measured. Leukemia inhibitory factor (LIF) injections were given intraperitoneally and implantation sites visualized. Gene expression patterns were compared with curated data sets to identify upstream regulators. RESULTS: GEN-exposed mice exhibited reduced uterine weight gain in response to E2 treatment or artificial decidualization compared with controls; however, expression of select hormone responsive genes remained similar between the two groups. Uteri from pregnant GEN-exposed mice were posteriorized and had reduced glandular epithelium. Implantation failure was not rescued by LIF administration. Microarray analysis of GEN-exposed uteri during early pregnancy revealed significant overlap with several conditional uterine knockout mouse models, including Foxa2, Wnt4, and Sox17. These models exhibit reduced endometrial glands, features of posteriorization and implantation failure. Expression of Foxa2, Wnt4, and Sox17, as well as genes important for neonatal uterine differentiation (Wnt7a, Hoxa10, and Msx2), were severely disrupted on PND5 in GEN-exposed mice. DISCUSSION: Our findings suggest that neonatal GEN exposure in mice disrupts expression of genes important for uterine development, causing posteriorization and diminished gland function during pregnancy that contribute to implantation failure. These findings could have implications for women who consumed soy-based formulas as infants. https://doi.org/10.1289/EHP6336 Environmental Health Perspectives 2020-03-18 /pmc/articles/PMC7138129/ /pubmed/32186404 http://dx.doi.org/10.1289/EHP6336 Text en https://ehp.niehs.nih.gov/about-ehp/license EHP is an open-access journal published with support from the National Institute of Environmental Health Sciences, National Institutes of Health. All content is public domain unless otherwise noted.
spellingShingle Research
Jefferson, Wendy N.
Padilla-Banks, Elizabeth
Suen, Alisa A.
Royer, Lindsey J.
Zeldin, Sharon M.
Arora, Ripla
Williams, Carmen J.
Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein
title Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein
title_full Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein
title_fullStr Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein
title_full_unstemmed Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein
title_short Uterine Patterning, Endometrial Gland Development, and Implantation Failure in Mice Exposed Neonatally to Genistein
title_sort uterine patterning, endometrial gland development, and implantation failure in mice exposed neonatally to genistein
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7138129/
https://www.ncbi.nlm.nih.gov/pubmed/32186404
http://dx.doi.org/10.1289/EHP6336
work_keys_str_mv AT jeffersonwendyn uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein
AT padillabankselizabeth uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein
AT suenalisaa uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein
AT royerlindseyj uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein
AT zeldinsharonm uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein
AT aroraripla uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein
AT williamscarmenj uterinepatterningendometrialglanddevelopmentandimplantationfailureinmiceexposedneonatallytogenistein

Ejemplares similares