Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad

The development of mammalian fetal germ cells along oogenic or spermatogenic fate trajectories is dictated by signals from the surrounding gonadal environment. Germ cells in the fetal testis enter mitotic arrest, whilst those in the fetal ovary undergo sex-specific entry into meiosis, the initiation...

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Autores principales: Childs, Andrew J., Cowan, Gillian, Kinnell, Hazel L., Anderson, Richard A., Saunders, Philippa T. K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3108594/
https://www.ncbi.nlm.nih.gov/pubmed/21674038
http://dx.doi.org/10.1371/journal.pone.0020249
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author Childs, Andrew J.
Cowan, Gillian
Kinnell, Hazel L.
Anderson, Richard A.
Saunders, Philippa T. K.
author_facet Childs, Andrew J.
Cowan, Gillian
Kinnell, Hazel L.
Anderson, Richard A.
Saunders, Philippa T. K.
author_sort Childs, Andrew J.
collection PubMed
description The development of mammalian fetal germ cells along oogenic or spermatogenic fate trajectories is dictated by signals from the surrounding gonadal environment. Germ cells in the fetal testis enter mitotic arrest, whilst those in the fetal ovary undergo sex-specific entry into meiosis, the initiation of which is thought to be mediated by selective exposure of fetal ovarian germ cells to mesonephros-derived retinoic acid (RA). Aspects of this model are hard to reconcile with the spatiotemporal pattern of germ cell differentiation in the human fetal ovary, however. We have therefore examined the expression of components of the RA synthesis, metabolism and signalling pathways, and their downstream effectors and inhibitors in germ cells around the time of the initiation of meiosis in the human fetal gonad. Expression of the three RA-synthesising enzymes, ALDH1A1, 2 and 3 in the fetal ovary and testis was equal to or greater than that in the mesonephros at 8–9 weeks gestation, indicating an intrinsic capacity within the gonad to synthesise RA. Using immunohistochemistry to detect RA receptors RARα, β and RXRα, we find germ cells to be the predominant target of RA signalling in the fetal human ovary, but also reveal widespread receptor nuclear localization indicative of signalling in the testis, suggesting that human fetal testicular germ cells are not efficiently shielded from RA by the action of the RA-metabolising enzyme CYP26B1. Consistent with this, expression of CYP26B1 was greater in the human fetal ovary than testis, although the sexually-dimorphic expression patterns of the germ cell-intrinsic regulators of meiotic initiation, STRA8 and NANOS2, appear conserved. Finally, we demonstrate that RA induces a two-fold increase in STRA8 expression in cultures of human fetal testis, but is not sufficient to cause widespread meiosis-associated gene expression. Together, these data indicate that while local production of RA within the fetal ovary may be important in regulating the onset of meiosis in the human fetal ovary, mechanisms other than CYP26B1-mediated metabolism of RA may exist to inhibit the entry of germ cells into meiosis in the human fetal testis.
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spelling pubmed-31085942011-06-13 Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad Childs, Andrew J. Cowan, Gillian Kinnell, Hazel L. Anderson, Richard A. Saunders, Philippa T. K. PLoS One Research Article The development of mammalian fetal germ cells along oogenic or spermatogenic fate trajectories is dictated by signals from the surrounding gonadal environment. Germ cells in the fetal testis enter mitotic arrest, whilst those in the fetal ovary undergo sex-specific entry into meiosis, the initiation of which is thought to be mediated by selective exposure of fetal ovarian germ cells to mesonephros-derived retinoic acid (RA). Aspects of this model are hard to reconcile with the spatiotemporal pattern of germ cell differentiation in the human fetal ovary, however. We have therefore examined the expression of components of the RA synthesis, metabolism and signalling pathways, and their downstream effectors and inhibitors in germ cells around the time of the initiation of meiosis in the human fetal gonad. Expression of the three RA-synthesising enzymes, ALDH1A1, 2 and 3 in the fetal ovary and testis was equal to or greater than that in the mesonephros at 8–9 weeks gestation, indicating an intrinsic capacity within the gonad to synthesise RA. Using immunohistochemistry to detect RA receptors RARα, β and RXRα, we find germ cells to be the predominant target of RA signalling in the fetal human ovary, but also reveal widespread receptor nuclear localization indicative of signalling in the testis, suggesting that human fetal testicular germ cells are not efficiently shielded from RA by the action of the RA-metabolising enzyme CYP26B1. Consistent with this, expression of CYP26B1 was greater in the human fetal ovary than testis, although the sexually-dimorphic expression patterns of the germ cell-intrinsic regulators of meiotic initiation, STRA8 and NANOS2, appear conserved. Finally, we demonstrate that RA induces a two-fold increase in STRA8 expression in cultures of human fetal testis, but is not sufficient to cause widespread meiosis-associated gene expression. Together, these data indicate that while local production of RA within the fetal ovary may be important in regulating the onset of meiosis in the human fetal ovary, mechanisms other than CYP26B1-mediated metabolism of RA may exist to inhibit the entry of germ cells into meiosis in the human fetal testis. Public Library of Science 2011-06-03 /pmc/articles/PMC3108594/ /pubmed/21674038 http://dx.doi.org/10.1371/journal.pone.0020249 Text en Childs 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
Childs, Andrew J.
Cowan, Gillian
Kinnell, Hazel L.
Anderson, Richard A.
Saunders, Philippa T. K.
Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad
title Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad
title_full Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad
title_fullStr Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad
title_full_unstemmed Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad
title_short Retinoic Acid Signalling and the Control of Meiotic Entry in the Human Fetal Gonad
title_sort retinoic acid signalling and the control of meiotic entry in the human fetal gonad
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3108594/
https://www.ncbi.nlm.nih.gov/pubmed/21674038
http://dx.doi.org/10.1371/journal.pone.0020249
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