Genetic background in the rat affects endocrine and metabolic outcomes of bisphenol F exposure

Author:

Wagner Valerie A1ORCID,Holl Katie L1,Clark Karen C23,Reho John J14,Dwinell Melinda R125,Lehmler Hans-Joachim6ORCID,Raff Hershel1237ORCID,Grobe Justin L1248ORCID,Kwitek Anne E1258ORCID

Affiliation:

1. Department of Physiology, Medical College of Wisconsin , Milwaukee, Wisconsin 53226, USA

2. Cardiovascular Center, Medical College of Wisconsin , Milwaukee, Wisconsin 53226, USA

3. Department of Medicine, Medical College of Wisconsin , Milwaukee, Wisconsin 53226, USA

4. Comprehensive Rodent Metabolic Phenotyping Core, Medical College of Wisconsin , Milwaukee, Wisconsin 53226, USA

5. Rat Genome Database, Medical College of Wisconsin , Milwaukee, Wisconsin 53226, USA

6. Department of Occupational and Environmental Health, University of Iowa , Iowa City, Iowa 52246, USA

7. Endocrine Research Laboratory, Aurora St. Luke’s Medical Center, Advocate Aurora Research Institute , Milwaukee, Wisconsin 53233, USA

8. Department of Biomedical Engineering, Medical College of Wisconsin , Milwaukee, Wisconsin 53226, USA

Abstract

Abstract Environmental bisphenol compounds like bisphenol F (BPF) are endocrine-disrupting chemicals (EDCs) affecting adipose and classical endocrine systems. Genetic factors that influence EDC exposure outcomes are poorly understood and are unaccounted variables that may contribute to the large range of reported outcomes in the human population. We previously demonstrated that BPF exposure increased body growth and adiposity in male N/NIH heterogeneous stock (HS) rats, a genetically heterogeneous outbred population. We hypothesize that the founder strains of the HS rat exhibit EDC effects that were strain- and sex-dependent. Weanling littermate pairs of male and female ACI, BN, BUF, F344, M520, and WKY rats randomly received either vehicle (0.1% EtOH) or 1.125 mg BPF/l in 0.1% EtOH for 10 weeks in drinking water. Body weight and fluid intake were measured weekly, metabolic parameters were assessed, and blood and tissues were collected. BPF increased thyroid weight in ACI males, thymus and kidney weight in BUF females, adrenal weight in WKY males, and possibly increased pituitary weight in BN males. BUF females also developed a disruption in activity and metabolic rate with BPF exposure. These sex- and strain-specific exposure outcomes illustrate that HS rat founders possess diverse bisphenol-exposure risk alleles and suggest that BPF exposure may intensify inherent organ system dysfunction existing in the HS rat founders. We propose that the HS rat will be an invaluable model for dissecting gene EDC interactions on health.

Funder

University of Iowa Environmental Health Sciences Research Center

NIH

National Institutes of Health Predoctoral Training

National Institutes of Health

Hybrid Rat Diversity Panel

Medical College of Wisconsin

The University of Virginia Center for Research in Reproduction Ligand Assay and Analysis Core

Eunice Kennedy Shriver NICHD

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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