Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch

Male factor infertility is a problem in today’s society but many underlying causes are still unknown. The generation of a conditional Sertoli cell (SC)-specific connexin 43 (Cx43) knockout mouse line (SCCx43KO) has provided a translational model. Expression of the gap junction protein Cx43 between a...

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Autores principales: Hilbold, Erika, Distl, Ottmar, Hoedemaker, Martina, Wilkening, Sandra, Behr, Rüdiger, Rajkovic, Aleksandar, Langeheine, Marion, Rode, Kristina, Jung, Klaus, Metzger, Julia, Brehm, Ralph H. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7140672/
https://www.ncbi.nlm.nih.gov/pubmed/32164318
http://dx.doi.org/10.3390/cells9030676
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author Hilbold, Erika
Distl, Ottmar
Hoedemaker, Martina
Wilkening, Sandra
Behr, Rüdiger
Rajkovic, Aleksandar
Langeheine, Marion
Rode, Kristina
Jung, Klaus
Metzger, Julia
Brehm, Ralph H. J.
author_facet Hilbold, Erika
Distl, Ottmar
Hoedemaker, Martina
Wilkening, Sandra
Behr, Rüdiger
Rajkovic, Aleksandar
Langeheine, Marion
Rode, Kristina
Jung, Klaus
Metzger, Julia
Brehm, Ralph H. J.
author_sort Hilbold, Erika
collection PubMed
description Male factor infertility is a problem in today’s society but many underlying causes are still unknown. The generation of a conditional Sertoli cell (SC)-specific connexin 43 (Cx43) knockout mouse line (SCCx43KO) has provided a translational model. Expression of the gap junction protein Cx43 between adjacent SCs as well as between SCs and germ cells (GCs) is known to be essential for the initiation and maintenance of spermatogenesis in different species and men. Adult SCCx43KO males show altered spermatogenesis and are infertile. Thus, the present study aims to identify molecular mechanisms leading to testicular alterations in prepubertal SCCx43KO mice. Transcriptome analysis of 8-, 10- and 12-day-old mice was performed by next-generation sequencing (NGS). Additionally, candidate genes were examined by qRT-PCR and immunohistochemistry. NGS revealed many significantly differentially expressed genes in the SCCx43KO mice. For example, GC-specific genes were mostly downregulated and found to be involved in meiosis and spermatogonial differentiation (e.g., Dmrtb1, Sohlh1). In contrast, SC-specific genes implicated in SC maturation and proliferation were mostly upregulated (e.g., Amh, Fshr). In conclusion, Cx43 in SCs appears to be required for normal progression of the first wave of spermatogenesis, especially for the mitosis-meiosis switch, and also for the regulation of prepubertal SC maturation.
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spelling pubmed-71406722020-04-13 Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch Hilbold, Erika Distl, Ottmar Hoedemaker, Martina Wilkening, Sandra Behr, Rüdiger Rajkovic, Aleksandar Langeheine, Marion Rode, Kristina Jung, Klaus Metzger, Julia Brehm, Ralph H. J. Cells Article Male factor infertility is a problem in today’s society but many underlying causes are still unknown. The generation of a conditional Sertoli cell (SC)-specific connexin 43 (Cx43) knockout mouse line (SCCx43KO) has provided a translational model. Expression of the gap junction protein Cx43 between adjacent SCs as well as between SCs and germ cells (GCs) is known to be essential for the initiation and maintenance of spermatogenesis in different species and men. Adult SCCx43KO males show altered spermatogenesis and are infertile. Thus, the present study aims to identify molecular mechanisms leading to testicular alterations in prepubertal SCCx43KO mice. Transcriptome analysis of 8-, 10- and 12-day-old mice was performed by next-generation sequencing (NGS). Additionally, candidate genes were examined by qRT-PCR and immunohistochemistry. NGS revealed many significantly differentially expressed genes in the SCCx43KO mice. For example, GC-specific genes were mostly downregulated and found to be involved in meiosis and spermatogonial differentiation (e.g., Dmrtb1, Sohlh1). In contrast, SC-specific genes implicated in SC maturation and proliferation were mostly upregulated (e.g., Amh, Fshr). In conclusion, Cx43 in SCs appears to be required for normal progression of the first wave of spermatogenesis, especially for the mitosis-meiosis switch, and also for the regulation of prepubertal SC maturation. MDPI 2020-03-10 /pmc/articles/PMC7140672/ /pubmed/32164318 http://dx.doi.org/10.3390/cells9030676 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Hilbold, Erika
Distl, Ottmar
Hoedemaker, Martina
Wilkening, Sandra
Behr, Rüdiger
Rajkovic, Aleksandar
Langeheine, Marion
Rode, Kristina
Jung, Klaus
Metzger, Julia
Brehm, Ralph H. J.
Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch
title Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch
title_full Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch
title_fullStr Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch
title_full_unstemmed Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch
title_short Loss of Cx43 in Murine Sertoli Cells Leads to Altered Prepubertal Sertoli Cell Maturation and Impairment of the Mitosis-Meiosis Switch
title_sort loss of cx43 in murine sertoli cells leads to altered prepubertal sertoli cell maturation and impairment of the mitosis-meiosis switch
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7140672/
https://www.ncbi.nlm.nih.gov/pubmed/32164318
http://dx.doi.org/10.3390/cells9030676
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