Differential Sensitivity of Rat Kidney and Liver to Fumonisin Toxicity: Organ-Specific Differences in Toxin Accumulation and Sphingoid Base Metabolism

doi:10.1093/toxsci/kfj198

ToxSci Advance Access originally published online on April 12, 2006
Toxicological Sciences 2006 92(1):335-345; doi:10.1093/toxsci/kfj198

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Published by Oxford University Press 2006.

Differential Sensitivity of Rat Kidney and Liver to Fumonisin Toxicity: Organ-Specific Differences in Toxin Accumulation and Sphingoid Base Metabolism

Ronald T. Riley¹ and Kenneth A. Voss

Toxicology and Mycotoxin Research Unit, USDA-ARS, Athens, Georgia 30604-5677

Received January 31, 2006; accepted April 10, 2006

Fumonisins (FBs) are mycotoxins in maize and are inhibitorsof ceramide synthase (CS), the most likely proximate cause ofFB toxicity. In liver and kidney, the primary target organsin FB-fed rats, inhibition of CS results in a marked increasein the ceramide precursor sphinganine (Sa). This study was conductedto investigate the differential time- and dose-dependent changesin Sa, sphingosine (So), sphinganine 1-phosphate (Sa-1-P), andsphingosine 1-phosphate (So-1-P) in kidney, liver, serum, andheart of male Sprague-Dawley rats (3–4 weeks old) feddiets containing 1.1, 13.5, and 88.6 µg/g of total FBfor 10 days. The tissues were microscopically examined for thepresence and severity of lesions consistent with FB exposure.There was a time- and dose-dependent increase in Sa in bothliver and kidney, which was closely correlated with the tissueconcentration of fumonisin B₁ (FB₁) and histopathologic findings.However, the Sa alone greatly underestimated the degree of disruptionof sphingolipid metabolism since accumulated Sa and So werequickly metabolized to Sa-1-P and So-1-P as evidenced by largeincreases in these metabolites in kidney but not in liver. Theconcentration of FB₁ in liver and kidney that first elicitedan increase in Sa was similar in both tissues, however, overtime, the kidney accumulated significantly more FB₁ (10x) andtotal Sa (Sa plus Sa-1-P) compared to liver. Thus, the relativesensitivity of male Sprague-Dawley rat kidney and liver is mostlikely a consequence of differences in the mechanisms responsiblefor both FB₁ uptake/clearance and Sa metabolism.

Key Words: fumonisin; sphingolipids; sphinganine; sphinganine 1-phosphate; sphingosine 1-phosphate.

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