Childhood DNA methylation as a marker of early life rapid weight gain and subsequent overweight

Robinson, Natassia, Brown, Heather, Antoun, Elie, Godfrey, Keith, Hanson, Mark, Lillycrop, Karen, Crozier, Sarah, Murray, Robert, Pearce, Mark, Relton, Caroline, Albani, Viviana and Mckay, Jill (2021) Childhood DNA methylation as a marker of early life rapid weight gain and subsequent overweight. Clinical Epigenetics, 13 (1). p. 8. ISSN 1868-7075

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Official URL: https://doi.org/10.1186/s13148-020-00952-z

Abstract

Background:
High early postnatal weight gain has been associated with childhood adiposity, however the mechanism remains unknown. DNA methylation is a hypothesised mechanism linking early life exposures and subsequent disease. However, epigenetic changes associated with high early weight gain have not previously been investigated. Our aim was to investigate the associations between early weight gain, peripheral blood DNA methylation, and subsequent overweight/obese.

Data from the UK Avon Longitudinal study of Parents and Children (ALSPAC) cohort were used to estimate associations between early postnatal weight gain and epigenome-wide DNA CpG site methylation (Illumina 450K Methylation Beadchip) in blood in childhood (n= 125) and late adolescence (n= 96). High weight gain in the first year (a change in weight z‐scores >0.67), both unconditional (rapid weight gain) and conditional on birthweight (rapid thrive), were related to individual CpG site methylation and across regions using the meffil pipeline, with and without adjustment for cell type proportions, and with 5% false discovery rate correction. Variation in methylation at high weight gain associated CpG sites were then examined with regards to body composition measures in childhood and adolescence. Replication of the differentially methylated CpG sites was sought using whole-blood DNA samples from 104 children from the UK Southampton Women’s Survey.

Results:
Rapid infant weight gain was associated with small (+1% change) increases in childhood methylation (age 7) for two distinct CpG sites (cg01379158 (NT5M) and cg11531579 (CHFR)). Childhood methylation at one of these CpGs (cg11531579) was also higher in those who experienced rapid weight gain and were subsequently overweight/obese in adolescence (age 17). Rapid weight gain was not associated with differential DNA methylation in adolescence. Childhood methylation at the cg11531579 site was also suggestively associated with rapid weight gain in the replication cohort.

Conclusions:
This study identified associations between rapid weight gain in infancy and small increases in childhood methylation at two CpG sites, one of which was replicated and was also associated with subsequent overweight/obese. It will be important to determine whether loci are markers of early rapid weight gain across different, larger populations. The mechanistic relevance of these differentially methylated sites requires further investigation.

Item Type: Article
Uncontrolled Keywords: Rapid weight gain, conditional weight gain, epigenetics, EWAS, DNA methylation, DOHAD, ALSPAC, SWS
Subjects: B900 Others in Subjects allied to Medicine
C100 Biology
C700 Molecular Biology, Biophysics and Biochemistry
Department: Faculties > Health and Life Sciences > Applied Sciences
Depositing User: John Coen
Date Deposited: 23 Oct 2020 09:57
Last Modified: 31 Jul 2021 14:33
URI: http://nrl.northumbria.ac.uk/id/eprint/44580

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