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Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation

The mechanisms and the mediators relaying Fsh action on testicular functions are poorly understood. Unlike in mammals, in fish both gonadotropins (Fsh and Lh) are able to efficiently stimulate steroidogenesis, likely through a direct interaction with their cognate receptors present on the Leydig cel...

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Autores principales: Sambroni, Elisabeth, Lareyre, Jean-Jacques, Le Gac, Florence
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3806798/
https://www.ncbi.nlm.nih.gov/pubmed/24194844
http://dx.doi.org/10.1371/journal.pone.0076684
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author Sambroni, Elisabeth
Lareyre, Jean-Jacques
Le Gac, Florence
author_facet Sambroni, Elisabeth
Lareyre, Jean-Jacques
Le Gac, Florence
author_sort Sambroni, Elisabeth
collection PubMed
description The mechanisms and the mediators relaying Fsh action on testicular functions are poorly understood. Unlike in mammals, in fish both gonadotropins (Fsh and Lh) are able to efficiently stimulate steroidogenesis, likely through a direct interaction with their cognate receptors present on the Leydig cells. In this context, it is crucial to understand if Fsh effects are mediated through the production of steroids. To address this issue we performed transcriptome studies after in vitro incubations of rainbow trout testis explants in the presence of Fsh alone or in combination with trilostane, an inhibitor of Δ4- steroidogenesis. Trilostane significantly reduced or suppressed the response of many genes to Fsh (like wisp1, testis gapdhs, cldn11, inha, vt1 or dmrt1) showing that, in fish, important aspects of Fsh action follow indirect pathways and require the production of Δ4-steroids. What is more, most of the genes regulated by Fsh through steroid mediation were similarly regulated by Lh (and/or androgens). In contrast, the response to Fsh of other genes was not suppressed in the presence of trilostane. These latter included genes encoding for anti-mullerian hormone, midkine a (pleiotrophin related), angiopoietine-related protein, cyclins E1 and G1, hepatocyte growth factor activator, insulin-like growth factor 1b/3. A majority of those genes were preferentially regulated by Fsh, when compared to Lh, suggesting that specific regulatory effects of Fsh did not depend on steroid production. Finally, antagonistic effects between Fsh and steroids were found, in particular for genes encoding key factors of steroidogenesis (star, hsd3b1, cyp11b2-2) or for genes of the Igf system (igf1b/3). Our study provides the first clear evidence that, in fish, Fsh exerts Δ4-steroid-independent regulatory functions on many genes which are highly relevant for the onset of spermatogenesis.
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spelling pubmed-38067982013-11-05 Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation Sambroni, Elisabeth Lareyre, Jean-Jacques Le Gac, Florence PLoS One Research Article The mechanisms and the mediators relaying Fsh action on testicular functions are poorly understood. Unlike in mammals, in fish both gonadotropins (Fsh and Lh) are able to efficiently stimulate steroidogenesis, likely through a direct interaction with their cognate receptors present on the Leydig cells. In this context, it is crucial to understand if Fsh effects are mediated through the production of steroids. To address this issue we performed transcriptome studies after in vitro incubations of rainbow trout testis explants in the presence of Fsh alone or in combination with trilostane, an inhibitor of Δ4- steroidogenesis. Trilostane significantly reduced or suppressed the response of many genes to Fsh (like wisp1, testis gapdhs, cldn11, inha, vt1 or dmrt1) showing that, in fish, important aspects of Fsh action follow indirect pathways and require the production of Δ4-steroids. What is more, most of the genes regulated by Fsh through steroid mediation were similarly regulated by Lh (and/or androgens). In contrast, the response to Fsh of other genes was not suppressed in the presence of trilostane. These latter included genes encoding for anti-mullerian hormone, midkine a (pleiotrophin related), angiopoietine-related protein, cyclins E1 and G1, hepatocyte growth factor activator, insulin-like growth factor 1b/3. A majority of those genes were preferentially regulated by Fsh, when compared to Lh, suggesting that specific regulatory effects of Fsh did not depend on steroid production. Finally, antagonistic effects between Fsh and steroids were found, in particular for genes encoding key factors of steroidogenesis (star, hsd3b1, cyp11b2-2) or for genes of the Igf system (igf1b/3). Our study provides the first clear evidence that, in fish, Fsh exerts Δ4-steroid-independent regulatory functions on many genes which are highly relevant for the onset of spermatogenesis. Public Library of Science 2013-10-23 /pmc/articles/PMC3806798/ /pubmed/24194844 http://dx.doi.org/10.1371/journal.pone.0076684 Text en © 2013 Sambroni 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
Sambroni, Elisabeth
Lareyre, Jean-Jacques
Le Gac, Florence
Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation
title Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation
title_full Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation
title_fullStr Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation
title_full_unstemmed Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation
title_short Fsh Controls Gene Expression in Fish both Independently of and through Steroid Mediation
title_sort fsh controls gene expression in fish both independently of and through steroid mediation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3806798/
https://www.ncbi.nlm.nih.gov/pubmed/24194844
http://dx.doi.org/10.1371/journal.pone.0076684
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