Abstract

Physiologically-based kinetic models are increasingly being incorporated into the assessment of risk arising from exposure to toxicants, and development of models on the kinetic behavior of metals, including arsenic, has been actively investigated for several years. A rational approach to the development of models on the kinetic behavior of metals, including arsenic, has been actively investigated for several years. A rational approach to the development of a complex kinetic model such as that required for arsenic (with the several chemical forms that it can take) involves establishing the most fundamental components of the model first, upon which higher levels of interaction can be built. Exposure of the cells of target tissues requires first that the toxicant cross cell membranes to access intracellular sites of intoxication. This can be followed by export of chemically different forms of the toxicant which can then serve as substrate for distant sites. Consequently, knowledge of the pathways and rates of arsenic flux across target tissue cell membranes must be considered a fundamental element in the development and ultimate calibration and validation of a physiological kinetic model of arsenic behavior. The present proposal has two principal aims, namely the elucidation of the major arsenic transport processes within cells of two tissue/organ systems which play central roles in the elimination of arsenic from the body: the kidney (with an emphasis on the proximal tubule), and the urinary bladder (which is an important target of arsenic carcinogenicity). The studies outlined in this proposal will determine, for the first time, how the major forms of arsenic enter and leave cells of the kidney studies outlined in this proposal will determine, for the first time, how the major forms of arsenic enter and leave cells of the kidney and bladder. Specifically, we will define the mechanisms of cellular transport of As(III), As(V), methylarsonic acid and dimethylarsinic acid, and determine the kinetics of their transport in each test tissue. We will test the general hypothesis that interactions of several arsenic species with intracellular glutathione exerts a profound effect on the export of arsenic from cells and therefore, influences the nature of the arsenic species to which other target cells are exposed. We will also test the novel hypothesis that endocytosis plays a quantitatively significant role in the entry and exposure to arsenic in bladder cells. Our approach involves comparison of effects obtained with intact tissues with those obtained single cloned transport proteins. The latter system will permit a well- focused examination of the properties of single transporters, with the former provides the only means to assess how the integrate activity of a suite of processes influences net cellular transport of arsenic. These data will provide a means for transport processes on overall arsenic flux in these tissues. These results can be expected to provide needed refinements to ongoing efforts to develop a physiologically-based kinetic model for the behavior of arsenic in biological 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 #
2P42ES004940-11
Application #
6334784
Study Section
Special Emphasis Panel (ZES1-MAO-A (G1))
Project Start
1990-03-05
Project End
2005-03-31
Budget Start
Budget End
Support Year
11
Fiscal Year
2000
Total Cost
$142,166
Indirect Cost

  Institution

Name
University of Arizona
Department
Type
DUNS #
City
Tucson
State
AZ
Country
United States
Zip Code
85721

  Publications

Madeira, Camila L; Field, Jim A; Simonich, Michael T et al. (2018) Ecotoxicity of the insensitive munitions compound 3-nitro-1,2,4-triazol-5-one (NTO) and its reduced metabolite 3-amino-1,2,4-triazol-5-one (ATO). J Hazard Mater 343:340-346
Liu, Pengfei; Rojo de la Vega, Montserrat; Sammani, Saad et al. (2018) RPA1 binding to NRF2 switches ARE-dependent transcriptional activation to ARE-NRE-dependent repression. Proc Natl Acad Sci U S A 115:E10352-E10361
Thomas, Andrew N; Root, Robert A; Lantz, R Clark et al. (2018) Oxidative weathering decreases bioaccessibility of toxic metal(loid)s in PM10 emissions from sulfide mine tailings. Geohealth 2:118-138
Yan, Ni; Liu, Fei; Liu, Boyang et al. (2018) Treatment of 1,4-dioxane and trichloroethene co-contamination by an activated binary persulfate-peroxide oxidation process. Environ Sci Pollut Res Int :
Dehghani, Mansooreh; Sorooshian, Armin; Nazmara, Shahrokh et al. (2018) Concentration and type of bioaerosols before and after conventional disinfection and sterilization procedures inside hospital operating rooms. Ecotoxicol Environ Saf 164:277-282
Keshavarzi, Behnam; Abbasi, Sajjad; Moore, Farid et al. (2018) Contamination Level, Source Identification and Risk Assessment of Potentially Toxic Elements (PTEs) and Polycyclic Aromatic Hydrocarbons (PAHs) in Street Dust of an Important Commercial Center in Iran. Environ Manage 62:803-818
Dodson, Matthew; de la Vega, Montserrat Rojo; Harder, Bryan et al. (2018) Low-level arsenic causes proteotoxic stress and not oxidative stress. Toxicol Appl Pharmacol 341:106-113
Soltani, Naghmeh; Keshavarzi, Behnam; Sorooshian, Armin et al. (2018) Oxidative potential (OP) and mineralogy of iron ore particulate matter at the Gol-E-Gohar Mining and Industrial Facility (Iran). Environ Geochem Health 40:1785-1802
Simon-Pascual, Alvaro; Sierra-Alvarez, Reyes; Ramos-Ruiz, Adriana et al. (2018) Reduction of platinum (IV) ions to elemental platinum nanoparticles by anaerobic sludge. J Chem Technol Biotechnol 93:1611-1617
Lyu, Ying; Brusseau, Mark L; Chen, Wei et al. (2018) Adsorption of PFOA at the Air-Water Interface during Transport in Unsaturated Porous Media. Environ Sci Technol 52:7745-7753

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