Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.

Gonad differentiation is a crucial step conditioning the future fertility of individuals and most of the master genes involved in this process have been investigated in detail. However, transcriptomic analyses of developing gonads from different animal models have revealed that hundreds of genes pre...

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Main Authors: Clara Gobé, Maëva Elzaiat, Nicolas Meunier, Marjolaine André, Eli Sellem, Patrice Congar, Luc Jouneau, Aurélie Allais-Bonnet, Ikrame Naciri, Bruno Passet, Eric Pailhoux, Maëlle Pannetier
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-02-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC6383954?pdf=render
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spelling doaj-7820e91da47545cda8dade438dda053d2020-11-25T02:31:41ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042019-02-01152e100790910.1371/journal.pgen.1007909Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.Clara GobéMaëva ElzaiatNicolas MeunierMarjolaine AndréEli SellemPatrice CongarLuc JouneauAurélie Allais-BonnetIkrame NaciriBruno PassetEric PailhouxMaëlle PannetierGonad differentiation is a crucial step conditioning the future fertility of individuals and most of the master genes involved in this process have been investigated in detail. However, transcriptomic analyses of developing gonads from different animal models have revealed that hundreds of genes present sexually dimorphic expression patterns. DMXL2 was one of these genes and its function in mammalian gonads was unknown. We therefore investigated the phenotypes of total and gonad-specific Dmxl2 knockout mouse lines. The total loss-of-function of Dmxl2 was lethal in neonates, with death occurring within 12 hours of birth. Dmxl2-knockout neonates were weak and did not feed. They also presented defects of olfactory information transmission and severe hypoglycemia, suggesting that their premature death might be due to global neuronal and/or metabolic deficiencies. Dmxl2 expression in the gonads increased after birth, during follicle formation in females and spermatogenesis in males. DMXL2 was detected in both the supporting and germinal cells of both sexes. As Dmxl2 loss-of-function was lethal, only limited investigations of the gonads of Dmxl2 KO pups were possible. They revealed no major defects at birth. The gonadal function of Dmxl2 was then assessed by conditional deletions of the gene in gonadal supporting cells, germinal cells, or both. Conditional Dmxl2 ablation in the gonads did not impair fertility in males or females. By contrast, male mice with Dmxl2 deletions, either throughout the testes or exclusively in germ cells, presented a subtle testicular phenotype during the first wave of spermatogenesis that was clearly detectable at puberty. Indeed, Dmxl2 loss-of-function throughout the testes or in germ cells only, led to sperm counts more than 60% lower than normal and defective seminiferous tubule architecture. Transcriptomic and immunohistochemichal analyses on these abnormal testes revealed a deregulation of Sertoli cell phagocytic activity related to germ cell apoptosis augmentation. In conclusion, we show that Dmxl2 exerts its principal function in the testes at the onset of puberty, although its absence does not compromise male fertility in mice.http://europepmc.org/articles/PMC6383954?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Clara Gobé
Maëva Elzaiat
Nicolas Meunier
Marjolaine André
Eli Sellem
Patrice Congar
Luc Jouneau
Aurélie Allais-Bonnet
Ikrame Naciri
Bruno Passet
Eric Pailhoux
Maëlle Pannetier
spellingShingle Clara Gobé
Maëva Elzaiat
Nicolas Meunier
Marjolaine André
Eli Sellem
Patrice Congar
Luc Jouneau
Aurélie Allais-Bonnet
Ikrame Naciri
Bruno Passet
Eric Pailhoux
Maëlle Pannetier
Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.
PLoS Genetics
author_facet Clara Gobé
Maëva Elzaiat
Nicolas Meunier
Marjolaine André
Eli Sellem
Patrice Congar
Luc Jouneau
Aurélie Allais-Bonnet
Ikrame Naciri
Bruno Passet
Eric Pailhoux
Maëlle Pannetier
author_sort Clara Gobé
title Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.
title_short Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.
title_full Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.
title_fullStr Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.
title_full_unstemmed Dual role of DMXL2 in olfactory information transmission and the first wave of spermatogenesis.
title_sort dual role of dmxl2 in olfactory information transmission and the first wave of spermatogenesis.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2019-02-01
description Gonad differentiation is a crucial step conditioning the future fertility of individuals and most of the master genes involved in this process have been investigated in detail. However, transcriptomic analyses of developing gonads from different animal models have revealed that hundreds of genes present sexually dimorphic expression patterns. DMXL2 was one of these genes and its function in mammalian gonads was unknown. We therefore investigated the phenotypes of total and gonad-specific Dmxl2 knockout mouse lines. The total loss-of-function of Dmxl2 was lethal in neonates, with death occurring within 12 hours of birth. Dmxl2-knockout neonates were weak and did not feed. They also presented defects of olfactory information transmission and severe hypoglycemia, suggesting that their premature death might be due to global neuronal and/or metabolic deficiencies. Dmxl2 expression in the gonads increased after birth, during follicle formation in females and spermatogenesis in males. DMXL2 was detected in both the supporting and germinal cells of both sexes. As Dmxl2 loss-of-function was lethal, only limited investigations of the gonads of Dmxl2 KO pups were possible. They revealed no major defects at birth. The gonadal function of Dmxl2 was then assessed by conditional deletions of the gene in gonadal supporting cells, germinal cells, or both. Conditional Dmxl2 ablation in the gonads did not impair fertility in males or females. By contrast, male mice with Dmxl2 deletions, either throughout the testes or exclusively in germ cells, presented a subtle testicular phenotype during the first wave of spermatogenesis that was clearly detectable at puberty. Indeed, Dmxl2 loss-of-function throughout the testes or in germ cells only, led to sperm counts more than 60% lower than normal and defective seminiferous tubule architecture. Transcriptomic and immunohistochemichal analyses on these abnormal testes revealed a deregulation of Sertoli cell phagocytic activity related to germ cell apoptosis augmentation. In conclusion, we show that Dmxl2 exerts its principal function in the testes at the onset of puberty, although its absence does not compromise male fertility in mice.
url http://europepmc.org/articles/PMC6383954?pdf=render
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