Cargando…

Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy

BACKGROUND: Preterm birth confers a high risk of adverse long term health outcomes for survivors, yet the underlying molecular mechanisms are unclear. We hypothesized that effects of preterm birth can be mediated through measurable epigenomic changes throughout development. We therefore used a longi...

Descripción completa

Detalles Bibliográficos
Autores principales: Cruickshank, Mark N, Oshlack, Alicia, Theda, Christiane, Davis, Peter G, Martino, David, Sheehan, Penelope, Dai, Yun, Saffery, Richard, Doyle, Lex W, Craig, Jeffrey M
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3978871/
https://www.ncbi.nlm.nih.gov/pubmed/24134860
http://dx.doi.org/10.1186/gm500
_version_ 1782310639983656960
author Cruickshank, Mark N
Oshlack, Alicia
Theda, Christiane
Davis, Peter G
Martino, David
Sheehan, Penelope
Dai, Yun
Saffery, Richard
Doyle, Lex W
Craig, Jeffrey M
author_facet Cruickshank, Mark N
Oshlack, Alicia
Theda, Christiane
Davis, Peter G
Martino, David
Sheehan, Penelope
Dai, Yun
Saffery, Richard
Doyle, Lex W
Craig, Jeffrey M
author_sort Cruickshank, Mark N
collection PubMed
description BACKGROUND: Preterm birth confers a high risk of adverse long term health outcomes for survivors, yet the underlying molecular mechanisms are unclear. We hypothesized that effects of preterm birth can be mediated through measurable epigenomic changes throughout development. We therefore used a longitudinal birth cohort to measure the epigenetic mark of DNA methylation at birth and 18 years comparing survivors of extremely preterm birth with infants born at term. METHODS: Using 12 extreme preterm birth cases and 12 matched, term controls, we extracted DNA from archived neonatal blood spots and blood collected in a similar way at 18 years of age. DNA methylation was measured at 347,789 autosomal locations throughout the genome using Infinium HM450 arrays. Representative methylation differences were confirmed by Sequenom MassArray EpiTYPER. RESULTS: At birth we found 1,555 sites with significant differences in methylation between term and preterm babies. At 18 years of age, these differences had largely resolved, suggesting that DNA methylation differences at birth are mainly driven by factors relating to gestational age, such as cell composition and/or maturity. Using matched longitudinal samples, we found evidence for an epigenetic legacy associated with preterm birth, identifying persistent methylation differences at ten genomic loci. Longitudinal comparisons of DNA methylation at birth and 18 years uncovered a significant overlap between sites that were differentially-methylated at birth and those that changed with age. However, we note that overlapping sites may either differ in the same (300/1,555) or opposite (431/1,555) direction during gestation and aging respectively. CONCLUSIONS: We present evidence for widespread methylation differences between extreme preterm and term infants at birth that are largely resolved by 18 years of age. These results are consistent with methylation changes associated with blood cell development, cellular composition, immune induction and age at these time points. Finally, we identified ten probes significantly associated with preterm individuals and with greater than 5% methylation discordance at birth and 18 years that may reflect a long term epigenetic legacy of preterm birth.
format Online
Article
Text
id pubmed-3978871
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-39788712014-04-09 Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy Cruickshank, Mark N Oshlack, Alicia Theda, Christiane Davis, Peter G Martino, David Sheehan, Penelope Dai, Yun Saffery, Richard Doyle, Lex W Craig, Jeffrey M Genome Med Research BACKGROUND: Preterm birth confers a high risk of adverse long term health outcomes for survivors, yet the underlying molecular mechanisms are unclear. We hypothesized that effects of preterm birth can be mediated through measurable epigenomic changes throughout development. We therefore used a longitudinal birth cohort to measure the epigenetic mark of DNA methylation at birth and 18 years comparing survivors of extremely preterm birth with infants born at term. METHODS: Using 12 extreme preterm birth cases and 12 matched, term controls, we extracted DNA from archived neonatal blood spots and blood collected in a similar way at 18 years of age. DNA methylation was measured at 347,789 autosomal locations throughout the genome using Infinium HM450 arrays. Representative methylation differences were confirmed by Sequenom MassArray EpiTYPER. RESULTS: At birth we found 1,555 sites with significant differences in methylation between term and preterm babies. At 18 years of age, these differences had largely resolved, suggesting that DNA methylation differences at birth are mainly driven by factors relating to gestational age, such as cell composition and/or maturity. Using matched longitudinal samples, we found evidence for an epigenetic legacy associated with preterm birth, identifying persistent methylation differences at ten genomic loci. Longitudinal comparisons of DNA methylation at birth and 18 years uncovered a significant overlap between sites that were differentially-methylated at birth and those that changed with age. However, we note that overlapping sites may either differ in the same (300/1,555) or opposite (431/1,555) direction during gestation and aging respectively. CONCLUSIONS: We present evidence for widespread methylation differences between extreme preterm and term infants at birth that are largely resolved by 18 years of age. These results are consistent with methylation changes associated with blood cell development, cellular composition, immune induction and age at these time points. Finally, we identified ten probes significantly associated with preterm individuals and with greater than 5% methylation discordance at birth and 18 years that may reflect a long term epigenetic legacy of preterm birth. BioMed Central 2013-10-18 /pmc/articles/PMC3978871/ /pubmed/24134860 http://dx.doi.org/10.1186/gm500 Text en Copyright © 2013 Cruickshank et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Cruickshank, Mark N
Oshlack, Alicia
Theda, Christiane
Davis, Peter G
Martino, David
Sheehan, Penelope
Dai, Yun
Saffery, Richard
Doyle, Lex W
Craig, Jeffrey M
Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
title Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
title_full Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
title_fullStr Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
title_full_unstemmed Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
title_short Analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
title_sort analysis of epigenetic changes in survivors of preterm birth reveals the effect of gestational age and evidence for a long term legacy
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3978871/
https://www.ncbi.nlm.nih.gov/pubmed/24134860
http://dx.doi.org/10.1186/gm500
work_keys_str_mv AT cruickshankmarkn analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT oshlackalicia analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT thedachristiane analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT davispeterg analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT martinodavid analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT sheehanpenelope analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT daiyun analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT safferyrichard analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT doylelexw analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy
AT craigjeffreym analysisofepigeneticchangesinsurvivorsofpretermbirthrevealstheeffectofgestationalageandevidenceforalongtermlegacy