Skip Navigation

Publication Detail

Title: ZIP8, member of the solute-carrier-39 (SLC39) metal-transporter family: characterization of transporter properties.

Authors: He, Lei; Girijashanker, Kuppuswami; Dalton, Timothy P; Reed, Jodie; Li, Hong; Soleimani, Manoocher; Nebert, Daniel W

Published In Mol Pharmacol, (2006 Jul)

Abstract: Cadmium is a dangerous metal distributed widely in the environment. Members of our laboratory recently identified the ZIP8 transporter protein, encoded by the mouse Slc39a8 gene, to be responsible for genetic differences in response to cadmium damage of the testis. Stable retroviral infection of the ZIP8 cDNA in mouse fetal fibroblast cultures (rvZIP8 cells) leads to as much as a 10-fold increase in the rate of intracellular cadmium influx and accumulation. In the present study, we showed that cadmium uptake operated maximally at pH 7.5 and a temperature of 37 degrees C and was inhibited by cyanide. Of more than a dozen cations tested, manganese(II) was the best competitive cation for cadmium uptake. The Km for Cd2+ uptake was 0.62 microM, and the Km for Mn2+ uptake was 2.2 microM; thus, manganese is probably the physiological substrate for ZIP8. Cadmium uptake was independent of sodium, potassium or chloride ions, but strongly dependent on the presence of bicarbonate. By Western blot analysis of rvZIP8 cells, we showed that ZIP8 protein was glycosylated. Using Z-stack confocal microscopy in Madin-Darby canine kidney polarized epithelial cells, we found that ZIP8 was localized on the apical side-implying an important role for manganese or cadmium uptake and disposition. It is likely that ZIP8 is a Mn2+/HCO3- symporter, that a HCO3- gradient across the plasma membrane acts as the driving force for manganese uptake, and that cadmium is a rogue hitchhiker displacing manganese to cause cadmium-associated disease.

PubMed ID: 16638970 Exiting the NIEHS site

MeSH Terms: Adenosine Triphosphate/metabolism; Animals; Bicarbonates/pharmacology; Biological Transport/drug effects; Cadmium/metabolism; Cadmium/toxicity; Cation Transport Proteins/genetics; Cation Transport Proteins/metabolism; Cation Transport Proteins/physiology*; Cell Line; Cell Survival/drug effects; Cells, Cultured; Chlorides/metabolism; Chlorides/pharmacology; Dogs; Dose-Response Relationship, Drug; Glycosylation; Kinetics; Male; Manganese/metabolism; Manganese/toxicity; Metals, Heavy/metabolism*; Metals, Heavy/toxicity; Mice; Mice, Inbred C57BL; Potassium/metabolism; Potassium/pharmacology; Research Support, N.I.H., Extramural; Sodium/metabolism; Sodium/pharmacology; Temperature; Transfection; Zinc/metabolism; Zinc/toxicity

Back
to Top
Last Reviewed: October 07, 2024