Enhanced cadmium-induced testicular necrosis and renal proximal tubule damage caused by gene-dose increase in a Slc39a8-transgenic mouse line

doi:10.1152/ajpcell.00409.2006

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Am J Physiol Cell Physiol 292: C1523-C1535, 2007. First published November 15, 2006; doi:10.1152/ajpcell.00409.2006
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MEMBRANE TRANSPORTERS, ION CHANNELS, AND PUMPS

Enhanced cadmium-induced testicular necrosis and renal proximal tubule damage caused by gene-dose increase in a Slc39a8-transgenic mouse line

Bin Wang,¹ Scott N. Schneider,¹ Nadine Dragin,¹ Kuppuswami Girijashanker,¹ Timothy P. Dalton,¹ Lei He,¹ Marian L. Miller,¹ Keith F. Stringer,² Manoocher Soleimani,³ Douglas D. Richardson,⁴ and Daniel W. Nebert¹

¹Department of Environmental Health, and the Center for Environmental Genetics (CEG), University Cincinnati Medical Center, ²Department of Pathology, Cincinnati Children's Hospital Medical Center, ³Department of Internal Medicine, Division of Nephrology and Hypertension, University Cincinnati Medical Center, and ⁴Department of Chemistry, University Cincinnati School of Arts and Sciences, Cincinnati Ohio

Submitted 30 July 2006 ; accepted in final form 11 November 2006

Resistance to cadmium (Cd)-induced testicular necrosis is anautosomal recessive trait defined as the Cdm locus. Using positionalcloning, we previously identified the Slc39a8 (encoding an apical-surfaceZIP8 transporter protein) as the gene most likely responsiblefor the phenotype. In situ hybridization revealed that endothelialcells of the testis vasculature express high ZIP8 levels intwo sensitive inbred mouse strains and negligible amounts intwo resistant strains. In the present study, we isolated a 168.7-kbbacterial artificial chromosome (BAC), carrying only the Slc39a8gene, from a Cd-sensitive 129/SvJ BAC library and generatedBAC-transgenic mice. The BTZIP8-3 line, having three copiesof the 129/SvJ Slc39a8 gene inserted into the Cd-resistant C57BL/6Jgenome (having its normal two copies of the Slc39a8 gene), showedtissue-specific ZIP8 mRNA expression similar to wild-type mice,mainly in lung, testis, and kidney. The $~$ 2.5-fold greater expressionparalleled the fact that the BTZIP8-3 line has five copies,whereas wild-type mice have two copies, of the Slc39a8 gene.The ZIP8 mRNA and protein localized especially to endothelialcells of the testis vasculature in BTZIP8-3 mice. Cd treatmentreversed Cd resistance (seen in nontransgenic littermates) toCd sensitivity in BTZIP8-3 mice; reversal of the testicularnecrosis phenotype confirms that Slc39a8 is unequivocally theCdm locus. ZIP8 also localized specifically to the apical surfaceof proximal tubule cells in the BTZIP8-3 kidney. Cd treatmentcaused acute renal failure and signs of proximal tubular damagein the BTZIP8-3 but not nontransgenic littermates. BTZIP8-3mice should be a useful model for studying Cd-induced diseasein kidney.

kidney; testis; ZIP8; bacterial artificial chromosome

Address for reprint requests and other correspondence: D. W. Nebert, Dept. of Environmental Health, Univ. of Cincinnati Medical Center, PO Box 670056, Cincinnati OH 45267-0056 (e-mail: dan.nebert{at}uc.edu)

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