Abstract

There is growing evidence that in utero and early developmental exposures to environmental chemicals may play a role in the development of obesity and related metabolic diseases later in life. Endocrine disrupting compounds are exogenous substances that mimic endogenous hormones in the endocrine pathway. Bisphenol-A (BPA) is a chemical plasticizer and xenoestrogen used in the production of polycarbonate plastics and epoxy resins. Human exposure to BPA is ubiquitous at low levels and occurs primarily through the diet. Studies in our laboratory and other investigators have shown that exposure of rodents to BPA during pregnancy results in increased adiposity and impaired glucose tolerance in adulthood. An important mechanism for in utero and early developmental effects of BPA is thought to be altered epigenetic regulation of gene expression. In support of this hypothesis is our preliminary data in mouse that BPA exposure during pregnancy results in loss of imprinting at two genes critical for development and obesity, Igf2 and Snrpn, in the embryo and placenta. These findings lead us to hypothesize that BPA exposure during development alters the epigenetic profile in key cells including the germline, resulting in altered gene expression, an abnormal phenotype, and transgenerational transmission of the phenotype. Other than the placenta, we cannot obtain target tissues such as islets, liver, or fat from humans during development. Thus an animal model can provide insight into mechanisms that can be later explored in the human. We propose the following specific aims:
Specific Aim 1 will assess the epigenome of F1 offspring exposed to BPA in utero as well as the F2-F3 generations. In addition to testing the expression and DNA methylation of imprinted genes, we will assay genome-wide DNA methylation changes and key histone modifications in F1-F3 offspring. The F1-F3 generations will also be metabolically phenotyped and germline of F2 and F3 epigenetically assayed.
Specific Aim 2 will ascertain whether BPA exposure of males during puberty and early adulthood alters the germline and leads to transgenerational transmission of an altered epigenotype and abnormal phenotype.
In Specific Aim 3 we will determine whether low dose BPA exposure in combination with DEHP, and vinclozolin alters the epigenome in the germline and leads to transgenerational transmission of an abnormal phenotype. Through the comprehensive analyses in the in vivo model, the results of the proposed project will build a solid standard for extrapolation of effects and mode of action to other classes of endocrine disrupting chemicals that are present in food and are identified as potential inducers of obesity and related metabolic diseases later in life. The proof of the principle of prenatal programming by environmental contaminants may change our awareness of critical assessment of the risk of such compounds.

Public Health Relevance

The proposed studies will provide new information regarding the association of BPA exposure with epigenetic changes and adverse phenotypes in the adult and whether these changes can be transmitted transgenerationally. The work will also assess the effects of combinations of endocrine disrupting compounds. The results of these studies will impact our assessment of risks due to environmental exposure of endocrine disrupting compounds.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES023284-03
Application #
8901171
Study Section
Special Emphasis Panel (ZES1-SET-J (TG))
Program Officer
Chadwick, Lisa
Project Start
2013-09-01
Project End
2018-07-31
Budget Start
2015-08-01
Budget End
2016-07-31
Support Year
3
Fiscal Year
2015
Total Cost
$400,000
Indirect Cost
$150,000

  Institution

Name
University of Pennsylvania
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Xin, Frances; Smith, Lauren M; Susiarjo, Martha et al. (2018) Endocrine-disrupting chemicals, epigenetics, and skeletal system dysfunction: exploration of links using bisphenol A as a model system. Environ Epigenet 4:dvy002
Xin, Frances; Fischer, Erin; Krapp, Christopher et al. (2018) Mice exposed to bisphenol A exhibit depressive-like behavior with neurotransmitter and neuroactive steroid dysfunction. Horm Behav 102:93-104
Bansal, Amita; Henao-Mejia, Jorge; Simmons, Rebecca A (2018) Immune System: An Emerging Player in Mediating Effects of Endocrine Disruptors on Metabolic Health. Endocrinology 159:32-45
Bansal, A; Li, C; Xin, F et al. (2018) Transgenerational effects of maternal bisphenol: a exposure on offspring metabolic health. J Dev Orig Health Dis :1-12
Bansal, Amita; Rashid, Cetewayo; Xin, Frances et al. (2017) Sex- and Dose-Specific Effects of Maternal Bisphenol A Exposure on Pancreatic Islets of First- and Second-Generation Adult Mice Offspring. Environ Health Perspect 125:097022
Susiarjo, Martha; Xin, Frances; Stefaniak, Martha et al. (2017) Bile Acids and Tryptophan Metabolism Are Novel Pathways Involved in Metabolic Abnormalities in BPA-Exposed Pregnant Mice and Male Offspring. Endocrinology 158:2533-2542
Vrooman, Lisa A; Xin, Frances; Bartolomei, Marisa S (2016) Morphologic and molecular changes in the placenta: what we can learn from environmental exposures. Fertil Steril 106:930-40
Xin, Frances; Susiarjo, Martha; Bartolomei, Marisa S (2015) Multigenerational and transgenerational effects of endocrine disrupting chemicals: A role for altered epigenetic regulation? Semin Cell Dev Biol 43:66-75
Rando, Oliver J; Simmons, Rebecca A (2015) I'm eating for two: parental dietary effects on offspring metabolism. Cell 161:93-105
Susiarjo, Martha; Xin, Frances; Bansal, Amita et al. (2015) Bisphenol a exposure disrupts metabolic health across multiple generations in the mouse. Endocrinology 156:2049-58