Literature DB >> 31403346

In-depth characterization of the placental imprintome reveals novel differentially methylated regions across birth weight categories.

Maya A Deyssenroth1, Carmen J Marsit2, Jia Chen1,3,4,5,6, Luca Lambertini1,5.   

Abstract

Imprinted genes play a pivotal role in placental processes underlying fetal development, and much interest centers on discerning whether these loci, via changes in DNA methylation and/or gene expression, inform disruptions in appropriate fetal growth. In this study, we comprehensively profiled DNA methylation across the placental imprintome and assessed the relationship with gene expression levels and aberrant fetal growth.Placental DNA methylation across 153 imprinted loci, including imprint control regions (ICR) and surrounding non-ICR regions, was surveyed using the Nimblegen TruSeq bisulfite sequencing platform among participants enrolled in the Rhode Island Child Health Study (RICHS, n = 163). Methylation and gene expression associations were assessed using eQTM analysis. Differential methylation analysis contrasting small (SGA) and large for gestational age (LGA) infants against appropriate for gestational age (AGA) infants was assessed using the DMRcate R package.We identified 34 SGA-related differentially methylated regions (DMRs) and 9 LGA-related DMRs (FDR<0.05), and these BW-DMRs predominated in promoter and intronic regions. We observed overall hypomethylation among SGA-DMRs overlapping maternally expressed (paternally imprinted) genes while no parent-of-origin effect was observed among LGA DMRs. Three BW-DMRs, mapping to GABRG3, IGF1R and MEST, were common to SGA and LGA placenta. We did not observe significant correlations between BW-DMR-associated CpG methylation and gene expression levels.We report the first in-depth characterization of the placental imprintome in a population-wide setting. Our findings reveal growth-related differences in methylation without concomitant expression differences in regions that extend beyond typically interrogated imprinted loci, highlighting potentially novel placental biomarkers of growth and development.

Entities:  

Keywords:  Birth Weight; Methylation; imprinting; placenta

Mesh:

Substances:

Year:  2019        PMID: 31403346      PMCID: PMC6961688          DOI: 10.1080/15592294.2019.1647945

Source DB:  PubMed          Journal:  Epigenetics        ISSN: 1559-2294            Impact factor:   4.528


  38 in total

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3.  Differential expression of imprinted genes in normal and IUGR human placentas.

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Journal:  Epigenetics       Date:  2009-05-14       Impact factor: 4.528

4.  Detection of global DNA methylation and paternally imprinted H19 gene methylation in preeclamptic placentas.

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Journal:  Hypertens Res       Date:  2011-02-17       Impact factor: 3.872

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10.  Conserved role of intragenic DNA methylation in regulating alternative promoters.

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Journal:  Nature       Date:  2010-07-08       Impact factor: 49.962

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Journal:  Epigenomics       Date:  2021-08-02       Impact factor: 4.357

2.  Being Born Large for Gestational Age is Associated with Increased Global Placental DNA Methylation.

Authors:  S E Dwi Putra; C Reichetzeder; A A Hasan; T Slowinski; C Chu; B K Krämer; B Kleuser; B Hocher
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3.  Differences in Placental Imprinted Gene Expression across Preeclamptic and Non-Preeclamptic Pregnancies.

Authors:  Maya A Deyssenroth; Qian Li; Carlos Escudero; Leslie Myatt; Jia Chen; James M Roberts
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