Abstract

Previous studies on impaired fetal growth have identified multiple risk factors including environmental tobacco smoke (ETS), social stress, lead exposure and air pollution. In parallel, a growing body of literature has demonstrated that all 4 of these risk factors can alter DNA methylation, suggesting a common pathway by which such environmental factors impair fetal growth. The key to understanding the role of environment in impairing fetal growth is to 1) measure environmental risk factors prospectively in pregnancy, to ensure that exposure and subsequent epigenetic changes are temporally associated and 2) to measure epigenetic changes in the correct target tissues. While a case control design may be more efficient, such a design could not tease out whether methylation changes were due to environmental factors or were constitutive in impaired growth. This point is critical as reducing risk by intervening on environmental factors requires knowledge of their mechanisms. To this end, this proposal will utilize the existing infrastructure of the ELEMENT birth cohort study in Mexico and a second ongoing study of similar design in Boston-PRISM. ELEMENT and PRISM have archived umbilical cord vessels and placenta as well as ETS, stress, air pollution and lead exposure measured prospectively beginning in the early 2nd trimester and data on fetal growth. We are therefore uniquely positioned to address these important questions. In this proposal, we hypothesize that common environmental risk factors that impair fetal growth will alter methylomic marks in target tissues critical for fetal growth. Fetal growth depends on maternal transport of nutrients as well as the transport and excretion of toxicants and waste products. Logical target tissues for fetal growth would be tissues of the vascular system (vessels, blood and placenta). Perhaps the greatest strength of our proposal is that we can assess multiple """"""""target tissues"""""""" and can compare and contrast 450,000 unique methylation sites across these tissues in the context of environmental exposures. This study will make substantial contributions to our understanding the role of environment in fetal growth.

Public Health Relevance

/ Statement of Public Health Significance: This project will identify DNA methylation alterations in umbilical vessels, placenta and fetal blood that are induced by exposure to environmental tobacco smoke, social stress, lead and air pollution. By conducting analyses on multiple tissues relevant to fetal growth, it will contribute to establishing how different exposures and tissues contribute to fetal growth.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
7R01ES020268-02
Application #
8334545
Study Section
Special Emphasis Panel (ZRG1-GGG-H (50))
Program Officer
Chadwick, Lisa
Project Start
2011-09-19
Project End
2014-07-31
Budget Start
2012-08-01
Budget End
2013-07-31
Support Year
2
Fiscal Year
2012
Total Cost
$900,659
Indirect Cost
$133,527

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Pediatrics
Type
Schools of Medicine
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Sanders, Alison P; Saland, Jeffrey M; Wright, Robert O et al. (2018) Perinatal and childhood exposure to environmental chemicals and blood pressure in children: a review of literature 2007-2017. Pediatr Res 84:165-180
Wu, Shaowei; Gennings, Chris; Wright, Rosalind J et al. (2018) Prenatal Stress, Methylation in Inflammation-Related Genes, and Adiposity Measures in Early Childhood: the Programming Research in Obesity, Growth Environment and Social Stress Cohort Study. Psychosom Med 80:34-41
Rodosthenous, Rodosthenis S; Burris, Heather H; Svensson, Katherine et al. (2017) Prenatal lead exposure and fetal growth: Smaller infants have heightened susceptibility. Environ Int 99:228-233
Chen, Jun; Behnam, Ehsan; Huang, Jinyan et al. (2017) Fast and robust adjustment of cell mixtures in epigenome-wide association studies with SmartSVA. BMC Genomics 18:413
Zhang, Haixiang; Zheng, Yinan; Yoon, Grace et al. (2017) Regularized estimation in sparse high-dimensional multivariate regression, with application to a DNA methylation study. Stat Appl Genet Mol Biol 16:159-171
Sanders, Alison P; Gennings, Chris; Svensson, Katherine et al. (2017) Bacterial and cytokine mixtures predict the length of gestation and are associated with miRNA expression in the cervix. Epigenomics 9:33-45
Rodosthenous, Rodosthenis S; Burris, Heather H; Sanders, Alison P et al. (2017) Second trimester extracellular microRNAs in maternal blood and fetal growth: An exploratory study. Epigenetics 12:804-810
Zheng, Laura Y; Sanders, Alison P; Saland, Jeffrey M et al. (2017) Environmental exposures and pediatric kidney function and disease: A systematic review. Environ Res 158:625-648
Xiao, Xirong; Zhao, Yan; Jin, Rong et al. (2016) Fetal growth restriction and methylation of growth-related genes in the placenta. Epigenomics 8:33-42
Chen, Jun; Just, Allan C; Schwartz, Joel et al. (2016) CpGFilter: model-based CpG probe filtering with replicates for epigenome-wide association studies. Bioinformatics 32:469-71

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