{alpha}2u-Globulin Nephropathy and Carcinogenicity following Exposure to Decalin (Decahydronaphthalene) in F344/N Rats

doi:10.1093/toxsci/kfg028

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Toxicological Sciences 72, 223-234 (2003)
Copyright © 2003 by the Society of Toxicology

CARCINOGENICITY

${alpha}$ _2u-Globulin Nephropathy and Carcinogenicity following Exposure to Decalin (Decahydronaphthalene) in F344/N Rats

Jeffrey A. Dill^*^,1, Kyeonghee M. Lee^*, Roger A. Renne^*, Rodney A. Miller^*, Alfred F. Fuciarelli^*, Kathy M. Gideon^*, Po C. Chan, Leo T. Burka and Joseph H. Roycroft

^* Battelle, Toxicology Northwest, Richland, Washington 99352; and National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709

Decalin (decahydronaphthalene) is a widely used industrial solventknown to cause male rat-specific ${alpha}$ _2u-globulin nephropathy. Inthis project, 13-week and two-year inhalation studies of decalinwere conducted consecutively in both sexes of F344/N rats. Thekey objectives were to (1) characterize the 13-week toxicityof decalin in rats, with an emphasis on nephropathy in males;(2) compare the kidney concentrations of decalin, 2-decalone,and ${alpha}$ _2u-globulin in males over 2 to 13 weeks of decalin exposure;and (3) correlate male rat nephropathy observed in the 13-weekstudy with renal carcinogenicity in the two-year study. F344rats (M/F) were exposed via whole-body inhalation to 0, 25,50, 100, 200, or 400 ppm decalin for 13 weeks. Urine was collectedat weeks 2 and 6 for creatinine and decalol analyses and atweek 12 for clinical urinalysis. Right kidneys were collectedfrom male rats at weeks 2 and 6 and from both sexes at week13, homogenates were prepared using the whole kidney, and thesehomogenates were analyzed for ${alpha}$ _2u-globulin, decalin, and 2-decalone.Left kidneys were evaluated for histopathology and cell proliferationutilizing a proliferating cell nuclear antigen technique andcounting proximal renal tubular epithelial cells to determinecell labeling indices. Necropsies and histopathologic evaluationswere performed at week 13. Decalin exposure caused increasesin kidney weight, urinalysis parameters (protein, AST, LDH),kidney ${alpha}$ _2u-globulin concentration, and proximal convoluted renaltubular cell proliferation in males. These changes were accompaniedby microscopic lesions (accumulation of hyaline droplets incortical tubules, regeneration of proximal tubular epithelium,and granular casts in medullary tubules) clearly linked to ${alpha}$ _2u-globulinnephropathy. Both decalin and 2-decalone were related to increased ${alpha}$ _2u-globulin in male kidneys. Kidney concentrations of decalin,2-decalone, and ${alpha}$ _2u-globulin in exposed females were negligible,while females excreted greater amounts of decalol metabolitesin urine than males at weeks 2 and 6. There were no exposure-relatedmicroscopic lesions in females. For chronic exposure, F344 ratswere exposed via whole-body inhalation to 0, 25, 50 (males only),100, or 400 ppm decalin for two years. Chronic exposure induceda spectrum of nonneoplastic and neoplastic lesions in the renalcortex of males, ranging from regenerative lesions of chronicnephropathy to tubular carcinomas. Incidences of renal tubularadenoma, tubular carcinoma, combined tubular adenomas and carcinomas,cortical tubular hyperplasia, hyaline droplet accumulation,hyperplasia of pelvic epithelium, and mineralization in renalpapilla were increased in exposed males compared to controls.There was a clear increase in the mean severity of chronic nephropathyin decalin-exposed males. It was concluded that the carcinogeniceffect on the renal cortical epithelium of male rats exposedto decalin was related to increased turnover of this epithelium,resulting from the cytotoxic effects of ${alpha}$ _2u-globulin accumulationin the renal cortical tubular cell cytoplasm.

Key Words: decalin (decahydronaphthalene); 2-decalone; decalol; ${alpha}$ _2u-globulin; hyaline droplet; cell proliferation; hyperplasia; nephropathy; toxicity; carcinogenicity; sex; F344/N.

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