Abstract

We contributed to several rodent studies that investigated sources of variability in response to genetics and environmental agents. The NTP was considering including environmental enrichment materials (e.g., nesting materials, polycarbonate shelters) in rodent cages within its testing program. We designed a study and analyzed data to confirm that these materials will not affect toxicity endpoints in short-term rat and mouse studies. In the past, the NTP has used genetically identical mice in its testing program. While these provide for a homogeneous response to chemical toxins, they do not reliably represent the potential range of responses of genetically diverse humans. The NTP conducted a large study of benzene using Diversity Outbred (DO) mice to examine the range of responses that could be obtained using mice that were approximately as genetically diverse as the human population. The primary endpoint in this study was micronucleus formation in response to DNA damage. We analyzed the data and contributed to NTP showing that there were regions within two genes associated with resistance to the DNA damaging effects of benzene. We also performed low dose extrapolation to determine the benchmark doses for this damage, suggesting that allowable human exposure levels should probably be reduced. Also in a demonstration of the effects of genetic diversity, we tested the effects of ozone exposure on clinical and histopathological indicators of cardiovascular disease in eight rat strains. We helped design this study and analyzed the data. The study showed distinct differences among the strains in susceptibility to cardiovascular disease following ozone exposure. In a mouse study of perfluorooctanoic acid (PFOA), mice were fed either a regular or high-fat diet while exposed to PFOA or control. Although mice on the high fat diet had higher body weights and blood lipid values than those on the regular diet, diet did not appear to affect their response to PFOA. Similarly, histopathological changes in the liver were associated with a high fat diet, but the diet did not affect liver changes seen with exposure to PFOA. Thus, the effects of diet appeared to be independent of the effects of PFOA.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIAES045003-20
Application #
9352093
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
20
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
U.S. National Inst of Environ Hlth Scis
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Stanko, Jason P; Kissling, Grace E; Chappell, Vesna A et al. (2016) Differences in the Rate of in Situ Mammary Gland Development and Other Developmental Endpoints in Three Strains of Female Rat Commonly Used in Mammary Carcinogenesis Studies: Implications for Timing of Carcinogen Exposure. Toxicol Pathol 44:1021-33
Churchill, Sheba R; Morgan, Daniel L; Kissling, Grace E et al. (2016) Impact of Environmental Enrichment Devices on NTP In Vivo Studies. Toxicol Pathol 44:233-45
French, John E; Gatti, Daniel M; Morgan, Daniel L et al. (2015) Diversity Outbred Mice Identify Population-Based Exposure Thresholds and Genetic Factors that Influence Benzene-Induced Genotoxicity. Environ Health Perspect 123:237-45
Filgo, Adam J; Quist, Erin M; Hoenerhoff, Mark J et al. (2015) Perfluorooctanoic Acid (PFOA)-induced Liver Lesions in Two Strains of Mice Following Developmental Exposures: PPAR? Is Not Required. Toxicol Pathol 43:558-68
Quist, Erin M; Filgo, Adam J; Cummings, Connie A et al. (2015) Hepatic Mitochondrial Alteration in CD-1 Mice Associated with Prenatal Exposures to Low Doses of Perfluorooctanoic Acid (PFOA). Toxicol Pathol 43:546-57
Ramot, Yuval; Kodavanti, Urmila P; Kissling, Grace E et al. (2015) Clinical and pathological manifestations of cardiovascular disease in rat models: the influence of acute ozone exposure. Inhal Toxicol 27 Suppl 1:26-38
Jayes, Friederike L; Burns, Katherine A; Rodriguez, Karina F et al. (2014) The naturally occurring luteinizing hormone surge is diminished in mice lacking estrogen receptor Beta in the ovary. Biol Reprod 90:24
Ray, Mitas; Shockley, Keith; Kissling, Grace (2014) Minimizing Systematic Errors in Quantitative High Throughput Screening Data Using Standardization, Background Subtraction, and Non-Parametric Regression. J Exp Second Sci 3:
Ferguson, Sherry A; Law, Charles Delbert; Kissling, Grace E (2014) Developmental treatment with ethinyl estradiol, but not bisphenol A, causes alterations in sexually dimorphic behaviors in male and female Sprague Dawley rats. Toxicol Sci 140:374-92
Cora, Michelle C; Neel, Jennifer A; Grindem, Carol B et al. (2013) Comparison of automated versus manual neutrophil counts for the detection of cellular abnormalities in dogs receiving chemotherapy: 50 cases (May to June 2008). J Am Vet Med Assoc 242:1539-43

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