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DNA methylation defects in spermatozoa of male partners from couples experiencing recurrent pregnancy loss.

Authors :
Khambata, Kushaan
Raut, Sanketa
Deshpande, Sharvari
Mohan, Sweta
Sonawane, Shobha
Gaonkar, Reshma
Ansari, Zakiya
Datar, Mamata
Bansal, Vandana
Patil, Anushree
Warke, Himangi
Balasinor, Nafisa H
Source :
Human Reproduction; Jan2021, Vol. 36 Issue 1, p48-60, 13p
Publication Year :
2021

Abstract

<bold>Study Question: </bold>What is the sperm DNA methylation status of imprinted genes in male partners from couples experiencing recurrent pregnancy loss (RPL)?<bold>Summary Answer: </bold>Aberrations in sperm DNA methylation status of several imprinted genes, such as insulin like growth factor-2-H19 differentially methylated region (IGF2-H19 DMR), intergenic differentially methylated region (IG-DMR), mesoderm specific transcript (MEST), zinc finger protein which regulates apoptosis and cell cycle arrest (ZAC), DMR in intron 10 of KCNQ1 gene (KvDMR), paternally expressed gene 3 (PEG3) and paternally expressed gene 10 (PEG10), as well as decreased sperm global 5-methylcytosine (5mC) levels, are associated with RPL.<bold>What Is Known Already: </bold>RPL is defined as loss of two or more pregnancies, affecting 1-2% of couples of reproductive age. Although there are several maternal and paternal aetiological factors contributing to RPL, nearly 50% of the cases remain idiopathic. Thus, there is a need to identify putative paternal factors that could be contributing towards pregnancy loss in cases of idiopathic RPL.<bold>Study Design, Size, Duration: </bold>In this case-control study, 112 couples undergoing RPL with no identifiable cause were recruited from September 2015 to May 2018. The control group comprised of 106 healthy proven fertile couples with no history of infertility or miscarriage.<bold>Participants/materials, Setting, Methods: </bold>In this study, we investigated the paternal genetic and epigenetic factors that could be associated with RPL. We studied DNA methylation, by pyrosequencing, of selected imprinted genes implicated in embryo development, such as IGF2-H19 DMR, IG-DMR, MEST, ZAC, KvDMR, PEG3, PEG10 and small nuclear ribonucleoprotein polypeptide N (SNRPN) in sperm of men whose partners present RPL. Global DNA methylation in sperm was evaluated by studying 5mC content and long interspersed nuclear element 1 (LINE1) promoter methylation. We also studied polymorphisms by pyrosequencing in the IGF2-H19 DMR as well in the IGF2 promoter in both groups.<bold>Main Results and the Role Of Chance: </bold>In the RPL group, we found a significant decrease in the global sperm 5mC levels and significant decrease in DNA methylation at three CpG sites in LINE1 promoter. For IGF2-H19 DMR and IG-DMR, a significant decrease in sperm DNA methylation at specific CpG sites was observed in RPL group. For maternally imprinted genes like MEST, ZAC, KvDMR, PEG3 and PEG10 hypermethylation was noted. Polymorphism studies for IGF2-H19 DMR and IGF2 revealed significant differences in the genotypic frequencies in males.<bold>Limitations, Reasons For Caution: </bold>In this study, we analysed the methylation levels of selected candidate imprinted genes implicated in embryo development. Detection of methylation changes occurring at the genome-wide level may reveal further candidate genes having a better distinction between the control and study groups.<bold>Wider Implications Of the Findings: </bold>Our study demonstrates that certain polymorphisms and aberrant sperm methylation status in imprinted genes are associated with RPL and could contribute to the aetiology of RPL. This study suggests that investigation of paternal genetic and epigenetic factors could be useful in identification of possible causes of idiopathic RPL.<bold>Study Funding/competing Interest(s): </bold>This study was funded by Department of Science and Technology-Science and Engineering Research Board (EMR/2014/000145) and National Institute for Research in Reproductive Health intramural funds (RA/872/01-2020). All authors declare no conflict of interest.<bold>Trial Registration Number: </bold>N/A. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
02681161
Volume :
36
Issue :
1
Database :
Complementary Index
Journal :
Human Reproduction
Publication Type :
Academic Journal
Accession number :
148188726
Full Text :
https://doi.org/10.1093/humrep/deaa278