Abstract

Cadmium exposure is an important problem in human toxicology. A major site of action is the kidney where Cd2+ causes moderate renal failure including an inability to resorb nutrients such as glucose, phosphate, calcium, and amino acids. The mechanisms that produce this aggregate of toxic effects are not understood. In mouse kidney cortical cells concentrations of Cd2+, which do not affect cell viability, ATP levels, or the activity of the Na+,K+-ATPase, inhibit Na+-glucose and -phosphate cotransport. Further studies have led to the hypothesis that Cd2+ acts directly and specifically on transporter biochemistry not indirectly through disruption of energy conservation mechanisms. It has also been found that metallothionein, the principal site of binding of Cd2+ in cells, can protect against this type of toxicity when present before but not after exposure. To define further both the mechanisms of inhibition of Na+-nutrient transport by Cd2+ and the chemistry and cellular roles of metallothionein related to cadmium exposure, the following specific aims will be explored: (1) To inquire how Cd2+ downregulates the Na+- glucose cotransporter and whether the same type of mechanism applies to inhibition of Na+-phosphate cotransport. (2) To examine whether similar mechanisms of transport inhibition occur in culture and in mice chronically exposed to Cd2+. (3) To determine whether Ca2+-transport is inhibited by Cd2+ in distal tubular cells. (4) To establish the mechanism by which chelating agents remove Cd2+ from kidney cells containing Cd,Zn-MT. (5) To investigate whether the presence of Cd,Zn-MT in kidney cells enhances the toxicity of aminoglycosides. (6) To define the pathway of reaction of apoMT with Cd2+ to form Cd7-MT. (7) To study the mechanism of reaction of apo-MT with Cd-protein complexes. (9) To examine the effect of protein concentration on the reactivity of MT. (8) To define 3-dimensional structure-reactivity relationships in MT. Cultured kidney tubular cells or whole animals will be the subject of experiments in 1-5. Molecular biological and transport methodologies will be used to address the aims in 1-4. Various chemical methods including NMR spectroscopy, radiochemistry, and spectrophotometry will be applied to native MT and its alpha- and beta-domains to investigate aims 5-9.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
2R01ES004026-09
Application #
2153516
Study Section
Special Emphasis Panel (ZRG4-PHRA (01))
Project Start
1987-07-01
Project End
2000-06-30
Budget Start
1995-07-01
Budget End
1996-06-30
Support Year
9
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Milwaukee
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
City
Milwaukee
State
WI
Country
United States
Zip Code
53201

  Publications

Namdarghanbari, Mohammad Ali; Bertling, Joseph; Krezoski, Susan et al. (2014) Toxic metal proteomics: reaction of the mammalian zinc proteome with Cd²?. J Inorg Biochem 136:115-21
Tabatabai, Niloofar M; North, Paula E; Regner, Kevin R et al. (2014) De novo expression of sodium-glucose cotransporter SGLT2 in Bowman's capsule coincides with replacement of parietal epithelial cell layer with proximal tubule-like epithelium. J Membr Biol 247:675-83
Meeusen, Jeffrey W; Tomasiewicz, Henry; Nowakowski, Andrew et al. (2011) TSQ (6-methoxy-8-p-toluenesulfonamido-quinoline), a common fluorescent sensor for cellular zinc, images zinc proteins. Inorg Chem 50:7563-73
Kothinti, Rajendra; Tabatabai, Niloofar M; Petering, David H (2011) Electrophoretic mobility shift assay of zinc finger proteins: competition for Zn(2+) bound to Sp1 in protocols including EDTA. J Inorg Biochem 105:569-76
Nowakowski, Andrew B; Petering, David H (2011) Reactions of the fluorescent sensor, Zinquin, with the zinc-proteome: adduct formation and ligand substitution. Inorg Chem 50:10124-33
Blodgett, Amy B; Kothinti, Rajendra K; Kamyshko, Ivan et al. (2011) A fluorescence method for measurement of glucose transport in kidney cells. Diabetes Technol Ther 13:743-51
Kothinti, Rajendra; Blodgett, Amy; Tabatabai, Niloofar M et al. (2010) Zinc finger transcription factor Zn3-Sp1 reactions with Cd2+. Chem Res Toxicol 23:405-12
Zhu, Jianyu; Meeusen, Jeffrey; Krezoski, Susan et al. (2010) Reactivity of Zn-, Cd-, and apo-metallothionein with nitric oxide compounds: in vitro and cellular comparison. Chem Res Toxicol 23:422-31
Kothinti, Rajendra K; Blodgett, Amy B; Petering, David H et al. (2010) Cadmium down-regulation of kidney Sp1 binding to mouse SGLT1 and SGLT2 gene promoters: possible reaction of cadmium with the zinc finger domain of Sp1. Toxicol Appl Pharmacol 244:254-62
Ejnik, John; Shaw 3rd, C Frank; Petering, David H (2010) Mechanism of cadmium ion substitution in mammalian zinc metallothionein and metallothionein alpha domain: kinetic and structural studies. Inorg Chem 49:6525-34

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