Sexually dimorphic gene expression that overlaps maturation of type II pneumonocytes in fetal mouse lungs

doi:10.1186/1477-7827-4-25

Reproductive Biology and Endocrinology

Volume 4

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Sexually dimorphic gene expression that overlaps maturation of type II pneumonocytes in fetal mouse lungs

Marc Simard¹^,3 , Pierre R Provost¹^,2^,3 and Yves Tremblay¹^,2^,3

¹Laboratory of Ontogeny and Reproduction, CHUQ, PCHUL, Faculty of Medicine, Laval University, Québec City, Québec, Canada

²Ob/Gyn Department, Faculty of Medicine, Laval University, Québec City, Québec, Canada

³Centre de Recherche en Biologie de la Reproduction (CRBR), Laval University, Québec City, Québec, Canada

author email corresponding author email

Reproductive Biology and Endocrinology 2006, 4:25doi:10.1186/1477-7827-4-25


Published:	4 May 2006

Abstract

Background

In human, respiratory distress of the neonates, which occurs in prematurity, is prevalent in male. Late in gestation, maturation of type II pneumonocytes, and consequently the surge of surfactant synthesis are delayed in male fetuses compared with female fetuses. Although the presence of higher levels of androgens in male fetuses is thought to explain this sex difference, the identity of genes involved in lung maturation that are differentially modulated according to fetal sex is unknown. We have studied the sex difference in developing mouse lung by gene profiling during a three-day gestational window preceding and including the emergence of mature PTII cells (the surge of surfactant synthesis in the mouse occurs on GD 17.5).

Methods

Total RNA was extracted from lungs of male and female fetal mice (gestation days 15.5, 16.5, and 17.5), converted to cRNA, labeled with biotin, and hybridized to oligonucleotide microarrays (Affymetrix MOE430A). Analysis of data was performed using MAS5.0, LFCM and Genesis softwares.

Results

Many genes involved in lung maturation were expressed with no sex difference. Of the approximative 14 000 transcripts covered by the arrays, only 83 genes presented a sex difference at one or more time points between GDs 15.5 and 17.5. They include genes involved in hormone metabolism and regulation (i.e. steroidogenesis pathways), apoptosis, signal transduction, transcriptional regulation, and lipid metabolism with four apolipoprotein genes. Genes involved in immune functions and other metabolisms also displayed a sex difference.

Conclusion

Among these sexually dimorphic genes, some may be candidates for a role in lung maturation. Indeed, on GD 17.5, the sex difference in surfactant lipids correlates with the sex difference in pulmonary expression of apolipoprotein genes, which are involved in lipid transport. This suggests a role for these genes in the surge of surfactant synthesis. Our results would help to identify novel genes involved in the physiopathology of the respiratory distress of the neonates.