2012
DOI: 10.1038/ejhg.2012.262
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Frequency and characterization of DNA methylation defects in children born SGA

Abstract: Various genes located at imprinted loci and regulated by epigenetic mechanisms are involved in the control of growth and differentiation. The broad phenotypic variability of imprinting disorders suggests that individuals with inborn errors of imprinting might remain undetected among patients born small for gestational age (SGA). We evaluated quantitative DNA methylation analysis at differentially methylated regions (DMRs) of 10 imprinted loci (PLAGL1, IGF2R DMR2, GRB10, H19 DMR, IGF2, MEG3, NDN, SNRPN, NESP, N… Show more

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Cited by 17 publications
(7 citation statements)
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“…No epimutations affecting ZDBF2 were identified Third, we studied a cohort of 52 SGA-born children (SGA cohort) enriched for patients with a phenotype at the severe end of the spectrum (i.e., lack of catchup growth and/or developmental delay) for aberrant DNA methylation at the ZDBF2 and FAM50B loci applying the Illumina Infinium HumanMethylation450 BeadChip. These patients were previously shown to be not affected by classical imprinting disorders [25]. None of these patients displayed aberrant DNA methylation values at the FAM50B locus (Supplementary Figure S4 & Supplementary Table S2E).…”
Section: Verification Of Array-based Mlidmentioning
confidence: 85%
“…No epimutations affecting ZDBF2 were identified Third, we studied a cohort of 52 SGA-born children (SGA cohort) enriched for patients with a phenotype at the severe end of the spectrum (i.e., lack of catchup growth and/or developmental delay) for aberrant DNA methylation at the ZDBF2 and FAM50B loci applying the Illumina Infinium HumanMethylation450 BeadChip. These patients were previously shown to be not affected by classical imprinting disorders [25]. None of these patients displayed aberrant DNA methylation values at the FAM50B locus (Supplementary Figure S4 & Supplementary Table S2E).…”
Section: Verification Of Array-based Mlidmentioning
confidence: 85%
“…As found in our previous smaller study, ART-conceived children were significantly over-represented among BWS ME + patients but more extensive methylation profiling using the CpG methylation array did not clearly differentiate between post-ART and naturally conceived BWS patients. Previously methylation profiling at imprinted loci in ART-conceived children without imprinting disorders has shown no generalised tendency to methylation changes [ 37 ]. We investigated a cohort with IC2 epimutations and though it could be argued that such cases might have been susceptible to ART-associated imprinting errors, only a minority had a ME + epigenotype.…”
Section: Discussionmentioning
confidence: 99%
“…Peripheral blood (PB) samples from 54 children born SGA, defined as birth length and/or birth weight -2SD below the mean for gestational age according to the reference data published by Niklasson et al [ 24 ], were included. The cohort has been recruited in the framework of the consortium “Diseases caused by imprinting defects: clinical spectrum and pathogenetic mechanisms” and partially overlaps with the previously described cohort of SGA born children studied for their DNA-methylation pattern at 10 imprinted loci by bisulfite pyrosequencing [ 25 ]. Of note, the children with evidence for DNA-methylation defects at the loci IGF2 , H19 , GRB10 , MEG3 and NDN in the latter study were excluded from the present study.…”
Section: Methodsmentioning
confidence: 99%