Issue 7, 2012

Roles of ZIP8, ZIP14, and DMT1 in transport of cadmium and manganese in mouse kidney proximal tubule cells

Abstract

Chronic exposure to cadmium causes preferential accumulation of cadmium in the kidney, leading to nephrotoxicity. In the process of renal cadmium accumulation, the cadmium bound to a low-molecular-weight metal-binding protein, metallothionein, has been considered to play an important role in reabsorption by epithelial cells of proximal tubules in the kidney. However, the role and mechanism of the transport of Cd2+ ions in proximal tubule cells remain unclear. Zinc transporters such as Zrt, Irt-related protein 8 (ZIP8) and ZIP14, and divalent metal transporter 1 (DMT1) have been reported to have affinities for Cd2+ and Mn2+. To examine the roles of these metal transporters in the absorption of luminal Cd2+ and Mn2+ into proximal tubule cells, we utilized a cell culture system, in which apical and basolateral transport of metals can be separately examined. The uptake of Cd2+ and Mn2+ from the apical side of proximal tubule cells was inhibited by simultaneous addition of Mn2+ and Cd2+, respectively. The knockdown of ZIP8, ZIP14 or DMT1 by siRNA transfection significantly reduced the uptake of Cd2+ and Mn2+ from the apical membrane. The excretion of Cd2+ and Mn2+ was detected predominantly in the apical side of the proximal tubule cells. In situ hybridization of these transporters revealed that ZIP8 and ZIP14 are highly expressed in the proximal tubules of the outer stripe of the outer medulla. These results suggest that ZIP8 and ZIP14 expressed in the S3 segment of proximal tubules play significant roles in the absorption of Cd2+ and Mn2+ in the kidney.

Graphical abstract: Roles of ZIP8, ZIP14, and DMT1 in transport of cadmium and manganese in mouse kidney proximal tubule cells

Article information

Article type
Paper
Submitted
01 Feb 2012
Accepted
03 Apr 2012
First published
25 Apr 2012

Metallomics, 2012,4, 700-708

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