Insulin-like growth factor 2/H19 methylation at birth and risk of overweight and obesity in children.

dc.contributor.author

Perkins, Ellen

dc.contributor.author

Murphy, Susan K

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Murtha, Amy P

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Schildkraut, Joellen

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Jirtle, Randy L

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Demark-Wahnefried, Wendy

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Forman, Michele R

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Kurtzberg, Joanne

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Overcash, Francine

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Huang, Zhiqing

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Hoyo, Cathrine

dc.date.accessioned

2022-03-23T20:16:54Z

dc.date.available

2022-03-23T20:16:54Z

dc.date.issued

2012-07

dc.date.updated

2022-03-23T20:16:53Z

dc.description.abstract

Objective

To determine whether aberrant DNA methylation at differentially methylated regions (DMRs) regulating insulin-like growth factor 2 (IGF2) expression in umbilical cord blood is associated with overweight or obesity in a multiethnic cohort.

Study design

Umbilical cord blood leukocytes of 204 infants born between 2005 and 2009 in Durham, North Carolina, were analyzed for DNA methylation at two IGF2 DMRs by using pyrosequencing. Anthropometric and feeding data were collected at age 1 year. Methylation differences were compared between children >85th percentile of the Centers for Disease Control and Prevention growth charts weight-for-age (WFA) and children ≤ 85th percentile of WFA at 1 year by using generalized linear models, adjusting for post-natal caloric intake, maternal cigarette smoking, and race/ethnicity.

Results

The methylation percentages at the H19 imprint center DMR was higher in infants with WFA >85th percentile (62.7%; 95% CI, 59.9%-65.5%) than in infants with WFA ≤ 85th percentile (59.3%; 95% CI, 58.2%-60.3%; P = .02). At the intragenic IGF2 DMR, methylation levels were comparable between infants with WFA ≤ 85th percentile and infants with WFA >85th percentile.

Conclusions

Our findings suggest that IGF2 plasticity may be mechanistically important in early childhood overweight or obese status. If confirmed in larger studies, these findings suggest aberrant DNA methylation at sequences regulating imprinted genes may be useful identifiers of children at risk for the development of early obesity.
dc.identifier

S0022-3476(12)00034-0

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0022-3476

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1097-6833

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https://hdl.handle.net/10161/24681

dc.language

eng

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Elsevier BV

dc.relation.ispartof

The Journal of pediatrics

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10.1016/j.jpeds.2012.01.015

dc.subject

Humans

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Obesity

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Insulin-Like Growth Factor II

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Risk

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Prospective Studies

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DNA Methylation

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Infant

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Female

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Male

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Overweight

dc.title

Insulin-like growth factor 2/H19 methylation at birth and risk of overweight and obesity in children.

dc.type

Journal article

duke.contributor.orcid

Murphy, Susan K|0000-0001-8298-7272

duke.contributor.orcid

Kurtzberg, Joanne|0000-0002-3370-0703

pubs.begin-page

31

pubs.end-page

39

pubs.issue

1

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Duke

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Nicholas School of the Environment

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School of Medicine

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Faculty

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Clinical Science Departments

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Institutes and Centers

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Family Medicine and Community Health

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Pathology

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Pediatrics

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Family Medicine and Community Health, Prevention Research

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Duke Cancer Institute

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Environmental Sciences and Policy

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Institutes and Provost's Academic Units

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Initiatives

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Duke Innovation & Entrepreneurship

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Pediatrics, Transplant and Cellular Therapy

pubs.publication-status

Published

pubs.volume

161

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