Associations between antibiotic exposure during pregnancy, birth weight and aberrant methylation at imprinted genes among offspring
Abstract
Objectives: Low birth weight (LBW) has been associated with common adult-onset chronic
diseases, including obesity, cardiovascular disease, type II diabetes and some cancers.
The etiology of LBW is multi-factorial. However, recent evidence suggests exposure
to antibiotics may also increase the risk of LBW. The mechanisms underlying this association
are unknown, although epigenetic mechanisms are hypothesized. In this study, we evaluated
the association between maternal antibiotic use and LBW and examined the potential
role of altered DNA methylation that controls growth regulatory imprinted genes in
these associations. Methods: Between 2009-2011, 397 pregnant women were enrolled and
followed until delivery. Prenatal antibiotic use was ascertained through maternal
self-report. Imprinted genes methylation levels were measured at differentially methylated
regions (DMRs) using bisulfite pyrosequencing. Generalized linear models were used
to examine associations among antibiotic use, birth weight and DMR methylation fractions.
Results: After adjusting for infant gender, race/ethnicity, maternal body mass index,
delivery route, gestational weight gain, gestational age at delivery, folic acid intake,
physical activity, maternal smoking and parity, antibiotic use during pregnancy was
associated with 138 g lower birth weight compared with non-antibiotic use (β-coefficient=-132.99,
s.e.=50.70, P=0.008). These associations were strongest in newborns of women who reported
antibiotic use other than penicillins (β-coefficient=-135.57, s.e.=57.38, P=0.02).
Methylation at five DMRs, IGF2 (P=0.05), H19 (P=0.15), PLAGL1 (P=0.01), MEG3 (P=0.006)
and PEG3 (P=0.08), was associated with maternal antibiotic use; among these, only
methylation at the PLAGL1 DMR was also associated with birth weight. Conclusion: We
report an inverse association between in utero exposure to antibiotics and lower infant
birth weight and provide the first empirical evidence supporting imprinted gene plasticity
in these associations. © 2013 Macmillan Publishers Limited.
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https://hdl.handle.net/10161/24664Published Version (Please cite this version)
10.1038/ijo.2013.47Publication Info
Vidal, AC; Murphy, SK; Murtha, AP; Schildkraut, JM; Soubry, A; Huang, Z; ... Hoyo,
C (2013). Associations between antibiotic exposure during pregnancy, birth weight and aberrant
methylation at imprinted genes among offspring. International Journal of Obesity, 37(7). pp. 907-913. 10.1038/ijo.2013.47. Retrieved from https://hdl.handle.net/10161/24664.This is constructed from limited available data and may be imprecise. To cite this
article, please review & use the official citation provided by the journal.
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Bernard Frank Fuemmeler
Adjunct Associate Professor in the Department of Community and Family Medicine
Unhealthy lifestyle factors, such as tobacco use, poor dietary intake, lack of physical
activity, and high body mass index are the leading causes of cancer and chronic disease.
The prevention of such diseases will be advanced through a more thorough understanding
of the complex determinants of these lifestyle factors and the development of novel
interventions that help change individual behavior for the better. Dr. Fuemmeler’s
program of research takes a lifespan approach toward understand
This author no longer has a Scholars@Duke profile, so the information shown here reflects
their Duke status at the time this item was deposited.
Edwin Severin Iversen Jr.
Research Professor of Statistical Science
Bayesian statistical modeling with application to problems in genetic epidemiology
and cancer research; models for epidemiological risk assessment, including hierarchical
methods for combining related epidemiological studies; ascertainment corrections for
high risk family data; analysis of high-throughput genomic data sets.
Joanne Kurtzberg
Jerome S. Harris Distinguished Professor of Pediatrics
Dr. Kurtzberg conducts both clinical and laboratory-based translational research
efforts, all involving various aspects of normal and malignant hematopoiesis. In the
laboratory, her early work focused on studies determining the mechanisms that regulate
the choice between the various pathways of differentiation available to the pluripotent
hematopoietic stem cell. Her laboratory established a CD7+ cell line, DU.528, capable
of multilineage differentiation as well as self-renewal, and subse
Susan Kay Murphy
Associate Professor in Obstetrics and Gynecology
My research interests are largely centered around epigenetics and the role of epigenetic
modifications in health and disease. My research projects include studies of gynecologic
malignancies, including working on approaches to target ovarian cancer cells that
survive chemotherapy and later give rise to recurrent disease. I have ongoing collaborative
projects in which we investigate the nature of the Developmental Origins of Health
and Disease (DOHaD) hypothesis. DOHaD reflects the ide
Amy Patricia Murtha
Professor of Obstetrics and Gynecology
Dr. Amy Murtha is a Professor in the Department of Obstetrics and Gynecology and Department
of Pediatrics, and past Vice Chair for Research in Obstetrics and Gynecology. After
graduating from the Medical College of Pennsylvania in 1992 she completed her residency
in OB-GYN and fellowship in Maternal Fetal Medicine (MFM) at Duke University then
joined the faculty at Duke in 1998.
Dr. Murtha served as interim Chair for the Department of OB-GYN and Fellowship Director
for the mater
Sara Elizabeth Neelon
Adjunct Associate Professor in the Department of Community and Family Medicine
Joellen Martha Schildkraut
Professor Emeritus in Family Medicine and Community Health
Dr. Schildkraut is an epidemiologist whose research includes the molecular epidemiology
of ovarian, breast and brain cancers. Dr. Schildkraut's research interests include
the study of the interaction between genetic and environmental factors. She is currently
involved in a large study of genome wide association and ovarian cancer risk and survival.
Some of her work is also focused on particular genetic pathways including the DNA
repair and apoptosis pathways. She currently leads a study of
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