Your search keyword '"Michael J. DeVito"' showing total 19 results

1. Mutational analysis of pentabrominated diphenyl-induced hepatocellular tumors in rats and mice, tissue levels of PBDE congeners in rats and mice, and AhR genotyping of Wistar Han rats

Author

June K. Dunnick, Arun R. Pandiri, B.A. Merrick, Grace E. Kissling, Helen Cunny, Esra Mutlu, Suramya Waidyanatha, Robert C. Sills, Hue-Hua. L. Hong, Thai-Vu Ton, Timonthy Maynor, Leslie Rescio, Siuzanne L. Phillips, Michael J. Devito, and Amy Brix

Subjects

Computer applications to medicine. Medical informatics, R858-859.7, Science (General), Q1-390

Abstract

This article describes data related to the research article entitled “Carcinogenic activity of pentabrominated diphenyl ether mixture (DE-71) in rats and mice” (Dunnick et al., 2018). PBDE-induced hepatocellular tumors harbored Hras and Ctnnb1 mutations and the methods for these studies are provided. Tissue levels of PBDE congeners in rats and mice after oral exposure to PBDE mixture increased with increasing dose of PBDE. There was no correlation between AhR status and the incidence of hepatocellular tumors in female Wistar Han rats. This manuscript provides additional information on the methods for conducting mutational analysis, PBDE tissue level determinations, and AhR genotyping.

Published

2018

2. Employing a Mechanistic Model for the Mapk Pathway to Examine the Impact of Cellular all or None Behavior on Overall Tissue Response

Author

Nicholas S. Luke, Michael J. DeVito, Christopher J. Portier, and Hisham A. El-Masri

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

The mitogen activated protein kinase (MAPK) cascade is a three-tiered phosphorylation cascade that is ubiquitously expressed among eukaryotic cells. Its primary function is to propagate signals from cell surface receptors to various cytosolic and nuclear targets. Recent studies have demonstrated that the MAPK cascade exhibits an all-or-none response to graded stimuli. This study quantitatively investigates MAPK activation in Xenopus oocytes using both empirical and biologically-based mechanistic models. Empirical models can represent overall tissue MAPK activation in the oocytes. However, these models lack description of key biological processes and therefore give no insight into whether the cellular response occurs in a graded or all-or-none fashion. To examine the propagation of cellular MAPK all-or-none activation to overall tissue response, mechanistic models in conjunction with Monte Carlo simulations are employed. An adequate description of the dose response relationship of MAPK activation in Xenopus oocytes is achieved. Furthermore, application of these mechanistic models revealed that the initial receptor-ligand binding rate contributes to the cells' ability to exhibit an all-or-none MAPK activation response, while downstream activation parameters contribute more to the magnitude of activation. These mechanistic models enable us to identify key biological events which quantitatively impact the shape of the dose response curve, especially at low environmentally relevant doses.

Published

2010

3. Toxicokinetics of perfluorobutane sulfonate (PFBS), perfluorohexane-1-sulphonic acid (PFHxS), and perfluorooctane sulfonic acid (PFOS) in male and female Hsd:Sprague Dawley SD rats after intravenous and gavage administration

Author

Michael J. DeVito, Chad R. Blystone, M.A. Eifrid, M.C. Huang, Anika L. Dzierlenga, Seth Gibbs, Courtney A. Granville, Veronica G. Robinson, and Suramya Waidyanatha

Subjects

medicine.medical_specialty, Perfluorinated chemicals, Health, Toxicology and Mutagenesis, Context (language use), 010501 environmental sciences, Toxicology, 01 natural sciences, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacokinetics, lcsh:RA1190-1270, PFOS, Internal medicine, medicine, Toxicokinetics, Perfluorinated alkyl acids, Perfluorohexane, lcsh:Toxicology. Poisons, 0105 earth and related environmental sciences, ComputingMethodologies_COMPUTERGRAPHICS, Chemistry, Perfluorobutane sulfonate, PFBS, 3. Good health, Rats, Perfluorooctane, Sulfonate, Endocrinology, PFHxS, Toxicity, Corrigendum, 030217 neurology & neurosurgery

Abstract

Graphical abstract, Highlights • In rats, the half-life of perfluoroalkyl sulfonic acids decreased with shorter chain lengths. • Sex differences in kinetics were found for PFBS and PFHxS but not PFOS. • Perfluoroalkyl sulfonic acids were highly present in the liver but not the brain., Perfluorinated alkyl substances (PFAS) are persistent contaminants that have been detected in the environment and in humans. With the PFAS chemical class, there are perfluorinated alkyl acids, many of which have been associated with certain toxicities. Because toxicity testing cannot feasibly be conducted for each individual PFAS, the National Toxicology Program (NTP) designed studies to compare toxicities across different subclasses of PFAS and across PFAS of different chain lengths to better understand the structure-toxicity relationship. Pharmacokinetic studies were conducted in parallel to these toxicity studies to facilitate comparisons across PFAS and to provide context for human relevance. Here, the toxicokinetic parameters of perfluorobutane sulfonate (PFBS), perfluorohexane-1-sulphonic acid (PFHxS), or perfluorooctane sulfonate (PFOS) after a single intravenous or gavage administration in male and female Hsd:Sprague-Dawley rats are reported. Concentrations of these PFAS were measured in the liver, kidney, and brain. Plasma half-life increased with longer chain length after gavage administration: PFBS- males averaged 3.3 h, females 1.3 h; PFHxS- males averaged 16.3 days, females 2.1 days; PFOS- males and females averaged ˜ 20 days. There were dose-dependent changes in clearance and systemic exposure for all administered chemicals and the direction of change was different in PFOS compared to the others. Liver:plasma ratios of PFOS were the highest followed by PFHxS and PFBS, while brain:plasma ratios were low in all three sulfonates. Sex differences in plasma half-life and tissue distribution were observed for PFBS and PFHxS, but not PFOS. These data provide a direct comparison of the kinetics of three different perfluoroalkyl sulfonic acids and allow for the contextualization of toxicity data in rats for human risk assessment of this chemical class.

Published

2019

4. A PBPK model describing the pharmacokinetics of γ-HBCD exposure in mice

Author

Michael J. DeVito, Claude Emond, and Linda S. Birnbaum

Subjects

Pharmacology, Hexabromocyclododecane, Physiologically based pharmacokinetic modelling, Adipose tissue, Alpha (ethology), Brain, Toxicology, Models, Biological, Article, Hydrocarbons, Brominated, Mice, Inbred C57BL, chemistry.chemical_compound, Mice, chemistry, Pharmacokinetics, Adipose Tissue, Liver, Internal dose, Toxicity, Brominated flame retardant, Animals, Female, Flame Retardants

Abstract

The brominated flame retardant, hexabromocyclododecane (HBCD), is added—but not bound—to consumer products and is eventually found in the environment and human tissues. Commercial-grade HBCD mixtures contain three major stereoisomers, alpha (α), beta (β), and gamma (γ), that are typically at a ratio of 12%:6%:82%, respectively. Although HBCD is widely used, the toxicological effects from its exposure in humans are not clearly understood. Using a physiologically based pharmacokinetic (PBPK) model could help improve our understanding of the toxicity of HBCD. The aim of this work was to develop a PBPK model, consisting of five permeability limited compartments (i.e., brain, liver, adipose tissue, blood, and rest of the body), to evaluate the pharmacokinetics of γ-HBCD in C57BL/6 mice. Physiological parameters related to body size, organ weights, and blood flow were taken from the literature. All partition coefficients were calculated based on the log K(ow). The elimination in urine and feces was optimized to reflect the percent dose eliminated, as published in the literature. Compared with data from the literature for brain, liver, blood, and adipose tissue, the model simulations accurately described the mouse data set within 1.5-fold of the data points. Also, two examples showing the utility of the PBPK model supplement the information regarding the internal dose that caused the health effects observed during these studies. Although this version of the PBPK model expressly describes γ-HBCD, more efforts are needed to clarify and improve the model to discriminate between the α, β, and γ stereoisomers.

Published

2021

5. Human and animal evidence of potential transgenerational inheritance of health effects: An evidence map and state-of-the-science evaluation

Author

Robyn Blain, Andrew J. Shapiro, Pamela A. Hartman, Katherine E. Pelch, Retha R. Newbold, Michael J. DeVito, Andrew A. Rooney, Stephanie Holmgren, Abee L. Boyles, Kristina A. Thayer, Vickie R. Walker, and Chad R. Blystone

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Biomedical Research, Databases, Factual, 03 medical and health sciences, 0302 clinical medicine, Transgenerational epigenetics, Pregnancy, Environmental health, medicine, Animals, Humans, lcsh:Environmental sciences, General Environmental Science, Protocol (science), lcsh:GE1-350, Public health, Stressor, Inheritance (genetic algorithm), Environmental Exposure, 030104 developmental biology, Categorization, Health assessment, Health effect, Maternal Exposure, Prenatal Exposure Delayed Effects, Paternal Exposure, Female, Psychology, 030217 neurology & neurosurgery

Abstract

Background An increasing number of reports suggest early life exposures result in adverse effects in offspring who were never directly exposed; this phenomenon is termed “transgenerational inheritance.” Given concern for public health implications for potential effects of exposures transmitted to subsequent generations, it is critical to determine how widespread and robust this phenomenon is and to identify the range of exposures and possible outcomes. Objectives This scoping report examines the evidence for transgenerational inheritance associated with exposure to a wide range of stressors in humans and animals to identify areas of consistency, uncertainty, data gaps, and to evaluate general risk of bias issues for the transgenerational study design. Methods A protocol was developed to collect and categorize the literature into a systematic evidence map for transgenerational inheritance by health effects, exposures, and evidence streams following the Office of Health Assessment and Translation (OHAT) approach for conducting literature-based health assessments. Results A PubMed search yielded 63,758 unique records from which 257 relevant studies were identified and categorized into a systematic evidence map by evidence streams (46 human and 211 animal), broad health effect categories, and exposures. Data extracted from the individual studies are available in the Health Assessment Workspace Collaborative (HAWC) program. There are relatively few bodies of evidence where multiple studies evaluated the same exposure and the same or similar outcomes. Studies evaluated for risk of bias generally had multiple issues in design or conduct. Conclusions The evidence mapping illustrated that risk of bias, few studies, and heterogeneity in exposures and endpoints examined present serious limitations to available bodies of evidence for assessing transgenerational effects. Targeted research is suggested to addressed inconsistencies and risk of bias issues identified, and thereby establish more robust bodies of evidence to critically assess transgenerational effects - particularly by adding data on exposure-outcome pairs where there is some evidence (i.e., reproductive, metabolic, and neurological effects).

Published

2018

6. Mixed Organic and Inorganic Tapwater Exposures and Potential Effects in Greater Chicago Area, USA

Author

Celeste A. Journey, Zachary R. Laughrey, Rachael F. Lane, Carrie A. McDonough, Carrie E. Givens, Paul M. Bradley, Nicola Evans, Joshua M. Allen, Michael T. Meyer, Kristin M. Romanok, Andrea R. Holthouse Putz, Alan Stark, Ariel R. Donovan, Michelle L. Hladik, Julie E. Dietze, Maria Argos, Christopher P. Weis, Abderrahman Zehraoui, Keith A. Loftin, Christopher P. Higgins, Michael J. Focazio, Kelly L. Smalling, Vickie S. Wilson, Michael J. DeVito, James L. Gray, Dana W. Kolpin, Luke R. Iwanowicz, R. Blaine McCleskey, Shannon M. Meppelink, Susan D. Richardson, and Elizabeth Medlock-Kakaley

Subjects

Tribromomethane, Michigan, Environmental Engineering, 010504 meteorology & atmospheric sciences, chemistry.chemical_element, 010501 environmental sciences, Bromodichloromethane, 01 natural sciences, Article, Water Purification, Human health, chemistry.chemical_compound, Environmental Chemistry, Maximum Contaminant Level, Pesticides, Waste Management and Disposal, Arsenic, 0105 earth and related environmental sciences, Chicago, Drinking Water, Treatment options, Pesticide, Pollution, United States, chemistry, Environmental chemistry, Environmental science, Water treatment, Water Pollutants, Chemical

Abstract

Safe drinking water at the point of use (tapwater, TW) is a public-health priority. TW exposures and potential human-health concerns of 540 organics and 35 inorganics were assessed in 45 Chicago-area United States (US) homes in 2017. No US Environmental Protection Agency (EPA) enforceable Maximum Contaminant Level(s) (MCL) were exceeded in any residential or water treatment plant (WTP) pre-distribution TW sample. Ninety percent (90%) of organic analytes were not detected in treated TW, emphasizing the high quality of the Lake Michigan drinking-water source and the efficacy of the drinking-water treatment and monitoring. Sixteen (16) organics were detected in >25% of TW samples, with about 50 detected at least once. Low-level TW exposures to unregulated disinfection byproducts (DBP) of emerging concern, per/polyfluoroalkyl substances (PFAS), and three pesticides were ubiquitous. Common exceedances of non-enforceable EPA MCL Goal(s) (MCLG) of zero for arsenic [As], lead [Pb], uranium [U]), bromodichloromethane, and tribromomethane suggest potential human-health concerns and emphasize the continuing need for improved understanding of cumulative effects of low-concentration mixtures on vulnerable sub-populations. Because DBP dominated TW organics, residential-TW concentrations are potentially predictable with expanded pre-distribution DBP monitoring. However, several TW chemicals, notably Pb and several infrequently detected organic compounds, were not readily explained by pre-distribution samples, illustrating the need for continued broad inorganic/organic TW characterization to support consumer assessment of acceptable risk and point-of-use treatment options.

Published

2020

7. Three-Dimensional (3D) HepaRG Spheroid Model With Physiologically Relevant Xenobiotic Metabolism Competence and Hepatocyte Functionality for Liver Toxicity Screening

Author

Sreenivasa C. Ramaiahgari, Suramya Waidyanatha, Darlene Dixon, Michael J. DeVito, Richard S. Paules, and Stephen S. Ferguson

Subjects

Cytochrome P-450 Enzyme System, Liver, Spheroids, Cellular, Humans, 3D HepaRG SPHEROID MODEL TO ASSESS XENOBIOTIC METABOLISM, Toxicology, Corrigendum, Models, Biological, Cell Line, Xenobiotics

Abstract

Effective prediction of human responses to chemical and drug exposure is of critical importance in environmental toxicology research and drug development. While significant progress has been made to address this challenge using invitro liver models, these approaches often fail due to inadequate tissue model functionality. Herein, we describe the development, optimization, and characterization of a novel three-dimensional (3D) spheroid model using differentiated HepaRG cells that achieve and maintain physiologically relevant levels of xenobiotic metabolism (CYP1A2, CYP2B6, and CYP3A4/5). This invitro model maintains a stable phenotype over multiple weeks in both 96- and 384-well formats, supports highly reproducible tissue-like architectures and models pharmacologically- and environmentally important hepatic receptor pathways (ie AhR, CAR, and PXR) analogous to primary human hepatocyte cultures. HepaRG spheroid cultures use 50–100× fewer cells than conventional two dimensional cultures, and enable the identification of metabolically activated toxicants. Spheroid size, time in culture and culture media composition were important factors affecting basal levels of xenobiotic metabolism and liver enzyme inducibility with activators of hepatic receptors AhR, CAR and PXR. Repeated exposure studies showed higher sensitivity than traditional 2D cultures in identifying compounds that cause liver injury and metabolism-dependent toxicity. This platform combines the well-documented impact of 3D culture configuration for improved tissue functionality and longevity with the requisite throughput and repeatability needed for year-over-year toxicology screening.

Published

2017

8. F344/NTac Rats Chronically Exposed to Bromodichloroacetic Acid Develop Mammary Adenocarcinomas With Mixed Luminal/Basal Phenotype and Tgfβ Dysregulation

Author

Shyamal D. Peddada, Yu Wang, Hue-Hua L. Hong, Abraham Nyska, Arun R. Pandiri, Thai-Vu T. Ton, Michelle J. Hooth, Michael J. DeVito, Janice B. Harvey, Sachin Bhusari, Julie F. Foley, and Mark J. Hoenerhoff

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Mammary gland, Biology, Acetates, Adenocarcinoma, Article, 03 medical and health sciences, Basal (phylogenetics), 0302 clinical medicine, Breast cancer, Transforming Growth Factor beta, medicine, Animals, Humans, Carcinogen, General Veterinary, Cancer, Mammary Neoplasms, Experimental, Hyperplasia, medicine.disease, Fibroadenoma, Rats, Inbred F344, Rats, 030104 developmental biology, medicine.anatomical_structure, Phenotype, 030220 oncology & carcinogenesis, Female

Abstract

Breast cancer is the most common cancer and the second-leading cause of cancer mortality in women in the United States. A recent 2-year National Toxicology Program carcinogenicity study showed an increased incidence of proliferative mammary lesions (hyperplasia, fibroadenoma, adenocarcinoma) in F344/NTac rats exposed to bromodichloroacetic acid (BDCA), a disinfection by-product in finished drinking water with widespread human exposure. We hypothesized that the increase in mammary tumors observed in BDCA-exposed F344/NTac rats may be due to underlying molecular changes relevant for human breast cancer. The objective of the study was to compare (1) gene and protein expression and (2) mutation spectra of relevant human breast cancer genes between normal untreated mammary gland and mammary tumors from control and BDCA-exposed animals to identify molecular changes relevant for human cancer. Histologically, adenocarcinomas from control and BDCA-exposed animals were morphologically very similar, were estrogen/progesterone receptor positive, and displayed a mixed luminal/basal phenotype. Gene expression analysis showed a positive trend in the number of genes associated with human breast cancer, with proportionally more genes represented in the BDCA-treated tumor group. Additionally, a 5-gene signature representing possible Tgfβ pathway activation in BDCA-treated adenocarcinomas was observed, suggesting that this pathway may be involved in the increased incidence of mammary tumors in BDCA-exposed animals.

Published

2015

9. Parameters for Pesticide QSAR and PBPK/PD Models for Human Risk Assessment

Author

James B. Knaak, Charles Timchalk, Rogelio Tornero-Velez, M. R. Goldsmith, J. C. Johnson, D. T. Chang, R. Tornero-Velez, J. B. Knaak, Curtis C. Dary, Robert W. Gerlach, Masahiko Okamoto, Hideo Kaneko, J. V. Bruckner, T. G. Osmitiz, S. Anand, D. Minnema, W. Schmitt, N. Assaf, J. Zastre, Mai A. Ngo, Howard I. Maibach, William G. Reifenrath, Ernest Hodgson, Andrew D. Wallace, Clement E. Furlong, Rebecca J. Richter, Lucio G. Costa, Gail P. Jarvik, Matthew K. Ross, Mariola J. Edelmann, Virginia C. Moser, Janice E. Chambers, Edward C. Meek, Howard W. Chambers, Jordan Ned Smith, Andrea Hjerpe, Torka S. Poet, Sookwang Lee, David M. Soderlund, Michael F. Hughes, Melissa P. L. Chan, James M. Starr, Timothy J. Shafer, Edward J. Scollon, Michael J. DeVito, Daniel T. Chang, Michael-Rock Goldsmith, Yu-Mei Tan, Christopher M. Grulke, Ling-Jen Chen, Elin M. Ulrich, Andrew B. Lindstrom, Melissa A. Pasquinelli, James R. Rabinowitz, Christopher D. Ruark, C. Eric Hack, Peter J. Robinson, Jeffery M. Gearhart, Jimena L. Davis, R. Woodrow Setzer, Corie A. Ellison, Robi, James B. Knaak, Charles Timchalk, Rogelio Tornero-Velez, M. R. Goldsmith, J. C. Johnson, D. T. Chang, R. Tornero-Velez, J. B. Knaak, Curtis C. Dary, Robert W. Gerlach, Masahiko Okamoto, Hideo Kaneko, J. V. Bruckner, T. G. Osmitiz, S. Anand, D. Minnema, W. Schmitt, N. Assaf, J. Zastre, Mai A. Ngo, Howard I. Maibach, William G. Reifenrath, Ernest Hodgson, Andrew D. Wallace, Clement E. Furlong, Rebecca J. Richter, Lucio G. Costa, Gail P. Jarvik, Matthew K. Ross, Mariola J. Edelmann, Virginia C. Moser, Janice E. Chambers, Edward C. Meek, Howard W. Chambers, Jordan Ned Smith, Andrea Hjerpe, Torka S. Poet, Sookwang Lee, David M. Soderlund, Michael F. Hughes, Melissa P. L. Chan, James M. Starr, Timothy J. Shafer, Edward J. Scollon, Michael J. DeVito, Daniel T. Chang, Michael-Rock Goldsmith, Yu-Mei Tan, Christopher M. Grulke, Ling-Jen Chen, Elin M. Ulrich, Andrew B. Lindstrom, Melissa A. Pasquinelli, James R. Rabinowitz, Christopher D. Ruark, C. Eric Hack, Peter J. Robinson, Jeffery M. Gearhart, Jimena L. Davis, R. Woodrow Setzer, Corie A. Ellison, and Robi

Subjects

Medical care, Pesticides, Statistics, Public health, Health services administration, Risk assessment, Chemical models, QSAR (Biochemistry), Pharmacokinetics, Risk, Structure-activity relationships (Biochemistry), Risk assessment--Congresses, Chemical models--Congresses, Pharmacokinetics--Congresses, Agricultural chemicals, Probabilities, Organization, Metabolism, Mathematical models, Risk management

Published

2012

10. Polybrominated Dibenzo-p-Dioxins, Dibenzofurans, and Biphenyls: Inclusion in the Toxicity Equivalency Factor Concept for Dioxin-Like Compounds

Author

Stephen Safe, Michael S. Denison, Linda S. Birnbaum, Martin Rose, Martin van den Berg, Mats Tysklind, Jerzy Falandysz, Richard E. Peterson, Dieter Schrenk, Heidelore Fiedler, Chiharu Tohyama, Angelika Tritscher, and Michael J. DeVito

Subjects

polychlorinated biphenyls, Polybrominated Biphenyls, Review, Toxicology, Dioxins, persistent organic chemicals, Risk Assessment, World health, regulatory/policy, Toxicity Tests, Animals, Humans, Soil Pollutants, ResearchInstitutes_Networks_Beacons/MERI, Benzofurans, Dose-Response Relationship, Drug, Chemistry, biomarkers, Expert consultation, Environmental Exposure, dioxin, Manchester Environmental Research Institute, Regulatory policy, halogenated hydrocarbon, Environmental chemistry, Environmental Monitoring

Abstract

In 2011, a joint World Health Organization (WHO) and United Nations Environment Programme (UNEP) expert consultation took place, during which the possible inclusion of brominated analogues of the dioxin-like compounds in the WHO Toxicity Equivalency Factor (TEF) scheme was evaluated. The expert panel concluded that polybrominated dibenzo-p-dioxins (PBDDs), dibenzofurans (PBDFs), and some dioxin-like biphenyls (dl-PBBs) may contribute significantly in daily human background exposure to the total dioxin toxic equivalencies (TEQs). These compounds are also commonly found in the aquatic environment. Available data for fish toxicity were evaluated for possible inclusion in the WHO-UNEP TEF scheme (van den Berg et al., 1998). Because of the limited database, it was decided not to derive specific WHO-UNEP TEFs for fish, but for ecotoxicological risk assessment, the use of specific relative effect potencies (REPs) from fish embryo assays is recommended. Based on the limited mammalian REP database for these brominated compounds, it was concluded that sufficient differentiation from the present TEF values of the chlorinated analogues (van den Berg et al., 2006) was not possible. However, the REPs for PBDDs, PBDFs, and non-ortho dl-PBBs in mammals closely follow those of the chlorinated analogues, at least within one order of magnitude. Therefore, the use of similar interim TEF values for brominated and chlorinated congeners for human risk assessment is recommended, pending more detailed information in the future.

Published

2013

11. Evaluation of the Association between Persistent Organic Pollutants (POPs) and Diabetes in Epidemiological Studies: A National Toxicology Program Workshop Review

Author

Duk Hee Lee, Kristina A. Thayer, Anna Rignell-Hydbom, Rogelio Tornero-Velez, David E. Jacobs, Kyla W. Taylor, Lars Lind, Henry A. Anderson, Mary Turyk, Abee L. Boyles, Josef Köhrle, Lars Rylander, Michael J. DeVito, Raymond F. Novak, Linda S. Birnbaum, and Chad R. Blystone

Subjects

medicine.medical_specialty, insulin, obesity, Health, Toxicology and Mutagenesis, hormone, Environmental Health and Occupational Health, Type 2 diabetes, Review, persistent organic pollutants, metabolic syndrome, Toxicology, chemistry.chemical_compound, Mice, Diabetes mellitus, Epidemiology, medicine, Hydrocarbons, Chlorinated, Animals, Humans, pollution, glucose, Exposure assessment, diabetes, business.industry, Public health, Public Health, Environmental and Occupational Health, Environmental exposure, Environmental Exposure, medicine.disease, Obesity, Rats, Dichlorodiphenyldichloroethylene, chemistry, Diabetes Mellitus, Type 2, pollutants, chemically induced, Environmental Pollutants, epidemiology, persistent organic, business, environment, toxicology

Abstract

BACKGROUND: Diabetes is a major threat to public health in the United States and worldwide. Understanding the role of environmental chemicals in the development or progression of diabetes is an emerging issue in environmental health. OBJECTIVE: We assessed the epidemiologic literature for evidence of associations between persistent organic pollutants (POPs) and type 2 diabetes. METHODS: Using a PubMed search and reference lists from relevant studies or review articles, we identified 72 epidemiological studies that investigated associations of persistent organic pollutants (POPs) with diabetes. We evaluated these studies for consistency, strengths and weaknesses of study design (including power and statistical methods), clinical diagnosis, exposure assessment, study population characteristics, and identification of data gaps and areas for future research. CONCLUSIONS: Heterogeneity of the studies precluded conducting a meta-analysis, but the overall evidence is sufficient for a positive association of some organochlorine POPs with type 2 diabetes. Collectively, these data are not sufficient to establish causality. Initial data mining revealed that the strongest positive correlation of diabetes with POPs occurred with organochlorine compounds, such as trans-nonachlor, dichlorodiphenyldichloroethylene (DDE), polychlorinated biphenyls (PCBs), and dioxins and dioxin-like chemicals. There is less indication of an association between other nonorganochlorine POPs, such as perfluoroalkyl acids and brominated compounds, and type 2 diabetes. Experimental data are needed to confirm the causality of these POPs, which will shed new light on the pathogenesis of diabetes. This new information should be considered by governmental bodies involved in the regulation of environmental contaminants.

Published

2013

12. Environmentally relevant mixtures in cumulative assessments: An acute study of toxicokinetics and effects on motor activity in rats exposed to a mixture of pyrethroids

Author

James M. Starr, David G. Ross, Stephen E. Graham, Edward J. Scollon, Kevin M. Crofton, Marcelo Javier Wolansky, Michael F. Hughes, Rogelio Tornero-Velez, and Michael J. DeVito

Subjects

Male, Insecticides, Toxicodynamics, CIENCIAS MÉDICAS Y DE LA SALUD, PYRETHROIDS, Ciencias de la Salud, TOXICOKINETICS, Motor Activity, Pharmacology, Toxicology, Models, Biological, Risk Assessment, Cypermethrin, chemistry.chemical_compound, Limit of Detection, Pyrethrins, parasitic diseases, medicine, Animals, Toxicokinetics, Rats, Long-Evans, Tissue Distribution, MOTOR ACTIVITY, Pyrethroid, Salud Ocupacional, Behavior, Animal, Dose-Response Relationship, Drug, Otras Ciencias Químicas, Ciencias Químicas, Brain, Reproducibility of Results, CUMULATIVE RISK, Rats, Deltamethrin, Adipose Tissue, Liver, chemistry, Models, Animal, Toxicity, Body Burden, Environmental Pollutants, Neurotoxicity Syndromes, Esfenvalerate, CIENCIAS NATURALES Y EXACTAS, Environmental Monitoring, Half-Life, Permethrin, medicine.drug

Abstract

Due to extensive use, human exposure to multiple pyrethroid insecticides occurs frequently. Studies of pyrethroid neurotoxicity suggest a common mode of toxicity and that pyrethroids should be considered cumulatively to model risk. The objective of this work was to use a pyrethroid mixture that reflects human exposure to common pyrethroids to develop comparative toxicokinetic profiles in rats, and then model the relationship between brain concentration and motor activity. Data from a national survey of child care centers were used to make a mixture reflecting proportions of the most prevalent pyrethroids: permethrin, cypermethrin, β-cyfluthrin, deltamethrin, and esfenvalerate. The mixture was administered orally at one of two concentrations (11.2 and 27.4 mg/kg) to adult male rats. At intervals from 1 to 24h, motor activity was assessed and the animals were sacrificed. Pyrethroid concentrations were measured in the blood, liver, fat, and brain. After controlling for dose, there were no differences in any tissue concentrations, except blood at the initial time point. Elimination half-lives for all pyrethroids in all tissues were < 7h. Brain concentrations of all pyrethroids (when cis- and trans-permethrin were pooled) at the initial time point were proportional to their relative doses. Decreases in motor activity indicated dose additivity, and the relationship between pyrethroid brain concentration and motor activity was described by a four-parameter sigmoidal Emax model. This study links environmental data with toxicokinetic and neurobehavioral assays to support cumulative risk assessments of pyrethroid pesticides. The results support the additive model of pyrethroid effect on motor activity and suggest that variation in the neurotoxicity of individual pyrethroids is related to toxicodynamic rather than toxicokinetic differences. Fil: Starr, James M.. United States Environmental Protection Agency; Estados Unidos Fil: Scollon, Edward J.. United States Environmental Protection Agency; Estados Unidos Fil: Hughes, Michael F.. United States Environmental Protection Agency; Estados Unidos Fil: Ross, David G.. United States Environmental Protection Agency; Estados Unidos Fil: Graham, Stephen E.. United States Environmental Protection Agency; Estados Unidos Fil: Crofton, Kevin M.. United States Environmental Protection Agency; Estados Unidos Fil: Wolansky, Marcelo Javier. United States Environmental Protection Agency; Estados Unidos. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Ciudad Universitaria. Instituto de Química Biológica de la Facultad de Ciencias Exactas y Naturales. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales. Instituto de Química Biológica de la Facultad de Ciencias Exactas y Naturales; Argentina Fil: DeVito, Michael J.. United States Environmental Protection Agency; Estados Unidos Fil: Tornero-Velez, Rogelio. United States Environmental Protection Agency; Estados Unidos

Published

2012

13. Developmental triclosan exposure decreases maternal, fetal, and early neonatal thyroxine: A dynamic and kinetic evaluation of a putative mode-of-action

Author

Ruby Bansal, Michael J. DeVito, R. Thomas Zoeller, Katie B. Paul, Joan M. Hedge, Robert Peter, and Kevin M. Crofton

Subjects

medicine.medical_specialty, CYP3A, Offspring, Radioimmunoassay, Thyrotropin, Biology, Toxicology, Article, Fetus, Pregnancy, Internal medicine, Cytochrome P-450 CYP1A1, medicine, Animals, Rats, Long-Evans, Glucuronosyltransferase, Triiodothyronine, Catabolism, Thyroid, Triclosan, Rats, Thyroxine, Endocrinology, medicine.anatomical_structure, Animals, Newborn, Liver, Hypothyroxinemia, Cytochrome P-450 CYP2B1, Female, Hormone

Abstract

This work tests the mode-of-action (MOA) hypothesis that maternal and developmental triclosan (TCS) exposure decreases circulating thyroxine (T4) concentrations via up-regulation of hepatic catabolism and elimination of T4. Time-pregnant Long-Evans rats received TCS po (0–300 mg/kg/day) from gestational day (GD) 6 through postnatal day (PND) 21. Serum and liver were collected from dams (GD20, PND22) and offspring (GD20, PND4, PND14, PND21). Serum T4, triiodothyronine (T3), and thyroid-stimulating hormone (TSH) concentrations were measured by radioimmunoassay. Ethoxy-O-deethylase (EROD), pentoxyresorufin-O-depentylase (PROD) and uridine diphosphate glucuronyltransferase (UGT) enzyme activities were measured in liver microsomes. Custom Taqman ® qPCR arrays were employed to measure hepatic mRNA expression of select cytochrome P450s, UGTs, sulfotransferases, transporters, and thyroid hormone-responsive genes. TCS was quantified by LC/MS/MS in serum and liver. Serum T4 decreased approximately 30% in GD20 dams and fetuses, PND4 pups and PND22 dams (300 mg/kg/day). Hepatic PROD activity increased 2–3 fold in PND4 pups and PND22 dams, and UGT activity was 1.5 fold higher in PND22 dams only (300 mg/kg/day). Minor up-regulation of Cyp2b and Cyp3a expression in dams was consistent with hypothesized activation of the constitutive androstane and/or pregnane X receptor. T4 reductions of 30% for dams and GD20 and PND4 offspring with concomitant increases in PROD (PND4 neonates and PND22 dams) and UGT activity (PND22 dams) suggest that up-regulated hepatic catabolism may contribute to TCS-induced hypothyroxinemia during development. Serum and liver TCS concentrations demonstrated greater fetal than postnatal internal exposure, consistent with the lack of T4 changes in PND14 and PND21 offspring. These data support the MOA hypothesis that TCS exposure leads to hypothyroxinemia via increased hepatic catabolism; however, the minor effects on thyroid hormone metabolism may reflect the low efficacy of TCS as thyroid hormone disruptor or highlight the possibility that other MOAs may also contribute to the observed maternal and early neonatal hypothyroxinemia.

Published

2012

14. Correlation of tissue concentrations of the pyrethroid bifenthrin with neurotoxicity in the rat

Author

Marcelo Javier Wolansky, Edward J. Scollon, Kevin M. Crofton, James M. Starr, Michael F. Hughes, and Michael J. DeVito

Subjects

Male, Insecticides, BLOOD CONCENTRATIONS, Bifenthrin, Motor Activity, Pharmacology, Toxicology, Article, purl.org/becyt/ford/1 [https], chemistry.chemical_compound, Pharmacokinetics, BRAIN CONCENTRATIONS, Pyrethrins, medicine, purl.org/becyt/ford/1.4 [https], Animals, Rats, Long-Evans, Tissue Distribution, MOTOR ACTIVITY, Whole blood, Pyrethroid, Chemistry, Otras Ciencias Químicas, Neurotoxicity, Ciencias Químicas, Brain, medicine.disease, BIFENTHRIN, Rats, Brain concentrations, Pharmacodynamics, Corn oil, CIENCIAS NATURALES Y EXACTAS

Abstract

The potential for human exposure to pyrethroid pesticides has prompted pharmacodynamic and pharmacokinetic research to better characterize risk. This work tested the hypothesis that blood and brain concentrations of the pyrethroid bifenthrin are predictive of neurotoxic effects. Adult male Long Evans rats received a single oral dose of bifenthrin dissolved in corn oil. Using figure-eight mazes, motor activity was measured for 1h at 4- and 7-h following exposure to bifenthrin (0-16mg/kg or 0-9mg/kg, respectively; n=4-8/group). Whole blood and brains were collected immediately following motor activity assays. Bifenthrin concentrations in blood and brain were quantified using HPLC/MS/MS. Bifenthrin exposure decreased motor activity from 20% to 70% in a dose-dependent manner at both time points. The relationship between motor activity data and administered dose, and blood and brain bifenthrin concentrations were described using a sigmoidal E max model. The relationships between motor activity and administered dose or blood concentrations were different between the 4- and 7-h time points. The relationship between motor activity and brain concentration was not significantly different between the two time points. These data suggest that momentary brain concentration of bifenthrin may be a more precise dose metric for predicting behavioral effects because the relationship between brain concentration and locomotor activity is independent of the time of exposure. Fil: Scollon, Edward J.. National Health And Environmental Effects Research Laboratory; Estados Unidos Fil: Starr, James M.. United States Environmental Protection Agency; Estados Unidos Fil: Crofton, Kevin M.. National Health And Environmental Effects Research Laboratory; Estados Unidos Fil: Wolansky, Marcelo Javier. National Research Council; Estados Unidos. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Ciudad Universitaria. Instituto de Química Biológica de la Facultad de Ciencias Exactas y Naturales. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales. Instituto de Química Biológica de la Facultad de Ciencias Exactas y Naturales; Argentina Fil: DeVito, Michael J.. National Health And Environmental Effects Research Laboratory; Estados Unidos Fil: Hughes, Michael F.. National Health And Environmental Effects Research Laboratory; Estados Unidos

Published

2011

15. Employing a Mechanistic Model for the Mapk Pathway to Examine the Impact of Cellular all or None Behavior on Overall Tissue Response

Author

Hisham A. El-Masri, Christopher J. Portier, Michael J. DeVito, and Nicholas S. Luke

Subjects

MAPK/ERK pathway, Chemical Health and Safety, biology, Health, Toxicology and Mutagenesis, lcsh:RM1-950, Public Health, Environmental and Occupational Health, Xenopus, Articles, MAPK cascade, Toxicology, Bioinformatics, biology.organism_classification, Phosphorylation cascade, Cell biology, Cytosol, lcsh:Therapeutics. Pharmacology, Cell surface receptor, Mitogen-activated protein kinase, biology.protein, Function (biology)

Abstract

The mitogen activated protein kinase (MAPK) cascade is a three-tiered phosphorylation cascade that is ubiquitously expressed among eukaryotic cells. Its primary function is to propagate signals from cell surface receptors to various cytosolic and nuclear targets. Recent studies have demonstrated that the MAPK cascade exhibits an all-or-none response to graded stimuli. This study quantitatively investigates MAPK activation in Xenopus oocytes using both empirical and biologically-based mechanistic models. Empirical models can represent overall tissue MAPK activation in the oocytes. However, these models lack description of key biological processes and therefore give no insight into whether the cellular response occurs in a graded or all-or-none fashion. To examine the propagation of cellular MAPK all-or-none activation to overall tissue response, mechanistic models in conjunction with Monte Carlo simulations are employed. An adequate description of the dose response relationship of MAPK activation in Xenopus oocytes is achieved. Furthermore, application of these mechanistic models revealed that the initial receptor-ligand binding rate contributes to the cells' ability to exhibit an all-or-none MAPK activation response, while downstream activation parameters contribute more to the magnitude of activation. These mechanistic models enable us to identify key biological events which quantitatively impact the shape of the dose response curve, especially at low environmentally relevant doses.

Published

2010

16. Evidence for dose-additive effects of pyrethroids on motor activity in rats

Author

Kevin M. Crofton, Marcelo Javier Wolansky, Michael J. DeVito, and Chris Gennings

Subjects

Male, additivity, Insecticides, CIENCIAS MÉDICAS Y DE LA SALUD, Serial dilution, Adult male, Health, Toxicology and Mutagenesis, PYRETHROIDS, Ciencias de la Salud, Salud Pública y Medioambiental, Pharmacology, Motor Activity, Toxicology, chemistry.chemical_compound, purl.org/becyt/ford/3.3 [https], pyrethroids, In vivo, Peak effect, neurotoxicity, Pyrethrins, parasitic diseases, Toxicología, ADDITIVITY, Animals, Rats, Long-Evans, Motor activity, Pyrethroid, Dose-Response Relationship, Drug, Research, cumulative, Public Health, Environmental and Occupational Health, MIXTURES, purl.org/becyt/ford/3.1 [https], Rats, Medicina Básica, mixtures, chemistry, NEUROTOXICITY, Dose addition, CUMULATIVE, purl.org/becyt/ford/3 [https], Corn oil

Abstract

BACKGROUND: Pyrethroids are neurotoxic insecticides used in a variety of indoor and outdoor applications. Previous research characterized the acute dose-effect functions for 11 pyrethroids administered orally in corn oil (1 mL/kg) based on assessment of motor activity. OBJECTIVES: We used a mixture of these 11 pyrethroids and the same testing paradigm used in single-compound assays to test the hypothesis that cumulative neurotoxic effects of pyrethroid mixtures can be predicted using the default dose-addition theory. METHODS: Mixing ratios of the 11 pyrethroids in the tested mixture were based on the ED30 (effective dose that produces a 30% decrease in response) of the individual chemical (i.e., the mixture comprised equipotent amounts of each pyrethroid). The highest concentration of each individual chemical in the mixture was less than the threshold for inducing behavioral effects. Adult male rats received acute oral exposure to corn oil (control) or dilutions of the stock mixture solution. The mixture of 11 pyrethroids was administered either simultaneously (2 hr before testing) or after a sequence based on times of peak effect for the individual chemicals (4, 2, and 1 hr before testing). A threshold additivity model was fit to the single-chemical data to predict the theoretical dose-effect relationship for the mixture under the assumption of dose additivity. RESULTS: When subthreshold doses of individual chemicals were combined in the mixtures, we found significant dose-related decreases in motor activity. Further, we found no departure from the predicted dose-additive curve regardless of the mixture dosing protocol used. CONCLUSION: In this article we present the first in vivo evidence on pyrethroid cumulative effects supporting the default assumption of dose addition. Fil: Wolansky, Marcelo Javier. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina. Universidad de Buenos Aires. Facultad de Ciencias Exactas y Naturales. Departamento de Química Biológica; Argentina Fil: Gennings, Chris. Solveritas; Estados Unidos Fil: DeVito, Michael J.. U.S. Environmental Protection Agency; Estados Unidos Fil: Crofton, Kevin M.. U.S. Environmental Protection Agency; Estados Unidos

Published

2009

17. THE EFFECT OF ATROPINE UPON THE OUTPUT OF THE HEARTS OF NORMAL MEN

Author

C. Sidney Burwell, W. Carter Smith, and Michael J. DeVito

Subjects

medicine.medical_specialty, Atropine, Text mining, business.industry, Internal medicine, Cardiology, Medicine, General Medicine, Articles, business, medicine.drug

Published

1928

18. Coordinated Changes in Xenobiotic Metabolizing Enzyme Gene Expression in Aging Male Rats.

Author

Janice S. Lee, William O. Ward, Douglas C. Wolf, James W. Allen, Camilla Mills, Michael J. DeVito, and J. Christopher Corton

Subjects

XENOBIOTICS, ENVIRONMENTAL toxicology, GENE expression, LABORATORY rats

Abstract

In order to gain insight into the effects of aging on susceptibility to environmental toxins, we characterized the expression of xenobiotic metabolizing enzymes (XMEs) from the livers of male F344 and Brown Norway (BN) rats across the adult lifespan. Using full-genome Affymetrix arrays, principal component analysis showed a clear age-dependent separation between young and old animals in both rat strains. Out of 1135 or 1435 genes altered between the old and young groups in the F344 or BN rats, 7 or 3% were XMEs and included members of the phase I, II, and III classes of genes. There was a 20 or 32% overlap in the gene expression profile between the two strains for F344 or BN, respectively. Lipid, ergosterol, alcohol, and fatty acid metabolism genes were also altered with age in both strains. Some of the genes altered by age exhibited a gender-dependent expression pattern in young adult rats, suggesting an increasingly feminized pattern of gene expression with age in male rats. To examine transcriptional responses across lifespan after challenge with a xenobiotic compound, BN rats were exposed to toluene by oral gavage. Toluene exposure decreased the expression of glutathione synthetase, and dramatically increased the number of phase III genes being downregulated. The expression of CYP2B2 and glutathione-S-transferase decreased with age but increased in all age groups after toluene exposure. Decreased ability to detoxify and transport chemicals out of the body with age could result in increased susceptibility to some classes of chemicals in the aging population. [ABSTRACT FROM AUTHOR]

Published

2008

19. Accumulation of PBDE-47 in Primary Cultures of Rat Neocortical Cells.

Author

William R. Mundy, Theresa M. Freudenrich, Kevin M. Crofton, and Michael J. DeVito

Subjects

NEOCORTEX

Abstract

A correction to the article "Accumulation of PBDE-47 in Primary Cultures of Rat Neocortical Cells," that was published in the 2004 issue is presented.

Published

2005