Your search keyword '"Barker, E.D. (Edward D.)"' showing total 4 results

1. Epigenetic profiling of social communication trajectories and co-occurring mental health problems: A prospective, methylome-wide association study

Author

Rijlaarsdam, J. (Jolien), Cecil, C.A.M. (Charlotte), Relton, C.L. (Caroline), Barker, E.D. (Edward D.), Rijlaarsdam, J. (Jolien), Cecil, C.A.M. (Charlotte), Relton, C.L. (Caroline), and Barker, E.D. (Edward D.)

Abstract

While previous studies suggest that both genetic and environmental factors play an important role in the development of autism-related traits, little is known about potential biological mechanisms underlying these associations. Using data from the Avon Longitudinal Study of Parents and Children (ALSPAC), we examined prospective associations between DNA methylation (DNAm: nbirth = 804, nage 7 = 877) and trajectories of social communication deficits at age 8-17 years. Methylomic variation at three loci across the genome (false discovery rate = 0.048) differentiated children following high (n = 80) versus low (n = 724) trajectories of social communication deficits. This differential DNAm was specific to the neonatal period and not observed at 7 years of age. Associations between DNAm and trajectory membership remained robust after controlling for co-occurring mental health problems (i.e., hyperactivity/inattention, conduct problems). The three loci identified at birth were not replicated in the Generation R Study. However, to the best of our knowledge, ALSPAC is the only study to date that is prospective enough to examine DNAm in relation to longitudinal trajectories of social communication deficits from childhood to adolescence. Although the present findings might point to potentially novel sites that differentiate between a high versus low trajectory of social communication deficits, the results should be considered tentative until further replicated.

Published

2021

2. Exposure to Bullying and General Psychopathology: A Prospective, Longitudinal Study

Author

Rijlaarsdam, J. (Jolien), Cecil, C.A.M. (Charlotte), Buil, M. (Marieke), Lier, P.A.C. (Pol) van, Barker, E.D. (Edward D.), Rijlaarsdam, J. (Jolien), Cecil, C.A.M. (Charlotte), Buil, M. (Marieke), Lier, P.A.C. (Pol) van, and Barker, E.D. (Edward D.)

Abstract

Although there is mounting evidence that the experience of being bullied associates with both internalizing and externalizing symptoms, it is not known yet whether the identified associations are specific to these symptoms, or shared between them. The primary focus of this study is to assess the prospective associations o

Published

2021

3. Prenatal unhealthy diet, insulin-like growth factor 2 gene (IGF2) methylation, and attention deficit hyperactivity disorder symptoms in youth with early-onset conduct problems

Author

Rijlaarsdam, J. (Jolien), Cecil, C.A.M. (Charlotte), Walton, E. (Esther), Mesirow, M.S.C. (Maurissa S. C.), Relton, C.L. (Caroline), Gaunt, T.R. (Tom), McArdle, W.L. (Wendy), Barker, E.D. (Edward D.), Rijlaarsdam, J. (Jolien), Cecil, C.A.M. (Charlotte), Walton, E. (Esther), Mesirow, M.S.C. (Maurissa S. C.), Relton, C.L. (Caroline), Gaunt, T.R. (Tom), McArdle, W.L. (Wendy), and Barker, E.D. (Edward D.)

Abstract

Background: Conduct problems (CP) and attention deficit hyperactivity disorder (ADHD) are often comorbid and have each been linked to 'unhealthy diet'. Early-life diet also associates with DNA methylation of the insulin-like growth factor 2 gene (IGF2), involved in fetal and neural development. We investigated the degree to which prenatal high-fat and -sugar diet might relate to ADHD symptoms via IGF2 DNA methylation for early-onset persistent (EOP) versus low CP youth. Methods: Participants were 164 youth with EOP (n = 83) versus low (n = 81) CP drawn from the Avon Longitudinal Study of Parents and Children. We assessed if the interrelationships between high-fat and -sugar diet (prenatal, postnatal), IGF2 methylation (birth and age 7, collected from blood), and ADHD symptoms (age 7-13) differed for EOP versus low CP youth. Results: Prenatal 'unhealthy diet' was positively associated with IGF2 methylation at birth for both the EOP and low CP youth. For EOP only: (a) higher IGF2 methylation predicted ADHD symptoms; and (b) prenatal 'unhealthy diet' was associated with higher ADHD symptoms indirectly via higher IGF2 methylation. Conclusions: Preventing 'unhealthy diet' in pregnancy might reduce the risk of ADHD symptoms in EOP youth via lower offspring IGF2 methylation.

Published

2017

4. An epigenome-wide association meta-analysis of prenatal maternal stress in neonates: A model approach for replication

Author

Rijlaarsdam, J. (Jolien), Pappa, I. (Irene), Walton, E. (Esther), Bakermans-Kranenburg, M.J. (Marian), Mileva-Seitz, V. (Viara), Rippe, R.C.A. (Ralph C.A.), Roza, S.J. (Sabine), Jaddoe, V.W.V. (Vincent), Verhulst, F.C. (Frank), Felix, J.F. (Janine), Cecil, C.A.M. (Charlotte), Relton, C.L. (Caroline), Gaunt, T.R. (Tom), McArdle, W.L. (Wendy), Mill, J. (Jonathan), Barker, E.D. (Edward D.), Tiemeier, H.W. (Henning), IJzendoorn, M.H. (Rien) van, Rijlaarsdam, J. (Jolien), Pappa, I. (Irene), Walton, E. (Esther), Bakermans-Kranenburg, M.J. (Marian), Mileva-Seitz, V. (Viara), Rippe, R.C.A. (Ralph C.A.), Roza, S.J. (Sabine), Jaddoe, V.W.V. (Vincent), Verhulst, F.C. (Frank), Felix, J.F. (Janine), Cecil, C.A.M. (Charlotte), Relton, C.L. (Caroline), Gaunt, T.R. (Tom), McArdle, W.L. (Wendy), Mill, J. (Jonathan), Barker, E.D. (Edward D.), Tiemeier, H.W. (Henning), and IJzendoorn, M.H. (Rien) van

Abstract

Prenatal maternal stress exposure has been associated with neonatal differential DNA methylation. However, the available evidence in humans is largely based on candidate gene methylation studies, where only a few CpG sites were evaluated. The aim of this study was to examine the association between prenatal exposure to maternal stress and offspring genome-wide cord blood methylation using different methods. First, we conducted a meta-analysis and follow-up pathway analyses. Second, we used novel region discovery methods [i.e., differentially methylated regions (DMRs) analyses]. To this end, we used data from two independent population-based studies, the Generation R Study (n = 912) and the Avon Longitudinal Study of Parents and Children (ALSPAC, n = 828), to (i) measure genome-wide DNA methylation in cord blood and (ii) extract a prenatal maternal stress composite. The meta-analysis (ntotal = 1,740) revealed no epigenome-wide (meta P <1.00e-07) associations of prenatal maternal stress exposure with neonatal differential DNA methylation. Follow-up analyses of the top hits derived from our epigenome-wide meta-analysis (meta P <1.00e-04) indicated an over-representation of the methyltransferase activity pathway. We identified no Bonferroni-corrected (P <1.00e-06) DMRs associated with prenatal maternal stress exposure. Combining data from two independent population-based samples in an epigenome-wide meta-analysis, the current study indicates that there are no large effects of prenatal maternal stress exposure on neonatal DNA methylation. Such replication efforts are essential in the search for robust associations, whether derived from candidate gene methylation or epigenome-wide studies.

Published

2016