Abstract

Chemicals, such as PCB's, PBB's, TCDD, DDT, peroxisomes, proliferators, etc., which have been associated with birth defects, cancer, reproductive and neuro-behavioral dysfunctions in experimental animals, work by """"""""epigenetic"""""""", not by genotoxic mechanisms [They all have been demonstrated to inhibit gap junctional intercellular communication (GJIC)]. The goal of the interdisciplinary project is to use an in vitro human neuron cell line with stem cell-like potential, to study the molecular (altered gene expression), biochemical (various mitogenetic/differentiation, signal transducing systems) and cellular (GFIC), cell proliferation, cell differentiation, apoptosis] mechanisms that might be affected by exposure to environmental toxicants prior to, or post, biological or chemical remediation processes. The proposal contains both an extension of our collaboration in the previous Superfund Program Project with Dr. Susan and Dr. W. Weber to assess the efficacy of their remediation techniques using our rat liver epithelial GJIC assay, as well as a new project to study the relationship of the modulation of GJIC in human neurons cells to chemically-induced signal transduction, to alterations in gene expression. The working hypothesis will be to determine if the blockage of GJIC by toxic chemicals is mediated by specific signal transduction mechanisms which might alter the expression of specific battery of genes which, in turn, could affect the cell's ability to regulate proliferation, cell differentiation or apoptosis.
Three specific aims are proposed:
Aim 1 : To use known model toxicants with known structure/function relations to identify specific intracellular signaling associated with alterations of cell behavior;
Aim : To study the signaling pathways, as in Aim 1, with the remediated mixtures to screen the efficacy of various remediation strategies;
Aim 3 : To test if the new DNA microarray technology can be used to identify altered gene expression associated with the altered GJIC and cellular endpoint studies of Aims 1 and 2. The significance is to provide validation of the inhibition of GJIC as a predictive endpoint of chemicals that can be toxic via their ability to trigger various signal transduction mechanisms that alter gene expression controlling either cell proliferation, cell differentiation, apoptosis or adaptive response of differentiated cells. In addition, using DNA microarray technology on a human in vitro system where many confounding factors can be controlled, identification of those genes associated with chemical-induced signal transduction systems and their associated biological effects might be easier and more relevant to the extrapolation of risk assessment in human beings, than the use of tissues from animal systems.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Hazardous Substances Basic Research Grants Program (NIEHS) (P42)
Project #
5P42ES004911-14
Application #
6579884
Study Section
Project Start
2002-04-01
Project End
2003-03-31
Budget Start
Budget End
Support Year
14
Fiscal Year
2002
Total Cost
$204,127
Indirect Cost

  Institution

Name
Michigan State University
Department
Type
DUNS #
193247145
City
East Lansing
State
MI
Country
United States
Zip Code
48824

  Publications

Nault, Rance; Doskey, Claire M; Fader, Kelly A et al. (2018) Comparison of Hepatic NRF2 and Aryl Hydrocarbon Receptor Binding in 2,3,7,8-Tetrachlorodibenzo-p-dioxin-Treated Mice Demonstrates NRF2-Independent PKM2 Induction. Mol Pharmacol 94:876-884
Dornbos, Peter; LaPres, John J (2018) Incorporating population-level genetic variability within laboratory models in toxicology: From the individual to the population. Toxicology 395:1-8
Zhang, Shuai; Liu, Qinfu; Gao, Feng et al. (2018) Interfacial Structure and Interaction of Kaolinite Intercalated with N-methylformamide Insight from Molecular Dynamics Modeling. Appl Clay Sci 158:204-210
Fader, Kelly A; Nault, Rance; Raehtz, Sandi et al. (2018) 2,3,7,8-Tetrachlorodibenzo-p-dioxin dose-dependently increases bone mass and decreases marrow adiposity in juvenile mice. Toxicol Appl Pharmacol 348:85-98
Zhang, Shuai; Liu, Qinfu; Cheng, Hongfei et al. (2018) Mechanism Responsible for Intercalation of Dimethyl Sulfoxide in Kaolinite: Molecular Dynamics Simulations. Appl Clay Sci 151:46-53
Zhang, Qiang; Li, Jin; Middleton, Alistair et al. (2018) Bridging the Data Gap From in vitro Toxicity Testing to Chemical Safety Assessment Through Computational Modeling. Front Public Health 6:261
Fader, K A; Nault, R; Kirby, M P et al. (2018) Corrigendum to ""Convergence of hepcidin deficiency, systemic iron overloading, heme accumulation, and REV-ERB?/? activation in aryl hydrocarbon receptor-elicited hepatotoxicity"" [Toxicol. Appl. Pharmacol. 321 (2017) 1-17]. Toxicol Appl Pharmacol 344:74
Konganti, Kranti; Ehrlich, Andre; Rusyn, Ivan et al. (2018) gQTL: A Web Application for QTL Analysis Using the Collaborative Cross Mouse Genetic Reference Population. G3 (Bethesda) 8:2559-2562
Zhang, Shuai; Liu, Qinfu; Gao, Feng et al. (2018) Molecular Dynamics Simulation of Basal Spacing, Energetics, and Structure Evolution of a Kaolinite-Formamide Intercalation Complex and Their Interfacial Interaction. J Phys Chem C Nanomater Interfaces 122:3341-3349
Li, Jinpeng; Bhattacharya, Sudin; Zhou, Jiajun et al. (2017) Aryl Hydrocarbon Receptor Activation Suppresses EBF1 and PAX5 and Impairs Human B Lymphopoiesis. J Immunol 199:3504-3515

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