Pentoxifylline Attenuates Bacterial Lipopolysaccharide-Induced Enhancement of Allyl Alcohol Hepatotoxicity

doi:10.1093/toxsci/56.1.203

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Toxicological Sciences 56, 203-210 (2000)
Copyright © 2000 by the Society of Toxicology

Pentoxifylline Attenuates Bacterial Lipopolysaccharide-Induced Enhancement of Allyl Alcohol Hepatotoxicity

Rosie A. Sneed^*, John P. Buchweitz^*, Paul A. Jean^* and Patricia E. Ganey^*^,^,1

^* Department of Pharmacology and Toxicology, Michigan State University, East Lansing, Michigan 48824; and Institute for Environmental Toxicology and National Food Safety and Toxicology Center, Michigan State University, East Lansing, Michigan 48824

Small amounts of exogenous lipopolysaccharide (LPS) (10 ng/kg–100µg/kg) enhance the hepatotoxicity of allyl alcohol inmale Sprague-Dawley rats. This augmentation of allyl alcoholhepatotoxicity appears to be linked to Kupffer cell function,but the mechanism of Kupffer cell involvement is unknown. SinceKupffer cells produce tumor necrosis factor-alpha (TNF ${alpha}$ ) uponexposure to LPS, and this cytokine has been implicated in liverinjury from large doses of LPS, we tested the hypothesis thatTNF ${alpha}$ contributes to LPS enhancement of allyl alcohol hepatotoxicity.Rats were treated with LPS (10–100 µg/kg iv) 2 hbefore allyl alcohol (30 mg/kg ip). Co-treatment with LPS andallyl alcohol caused liver injury as assessed by an increasein activity of alanine aminotransferase in plasma. Treatmentwith LPS caused an increase in plasma TNF ${alpha}$ concentration, whichwas prevented by administration of either pentoxifylline (PTX)(100 mg/kg iv) or anti-TNF ${alpha}$ serum (1ml/rat iv) one h prior toLPS. Only PTX protected rats from LPS-induced enhancement ofallyl alcohol hepatotoxicity; anti-TNF ${alpha}$ serum had no effect.Exposure of cultured hepatocytes to LPS (1–10 µg/ml)or to TNF ${alpha}$ (15–150 ng/ml) for 2 h did not increase thecytotoxicity of allyl alcohol (0.01–200 µM). Thesedata suggest that neither LPS nor TNF ${alpha}$ alone was sufficient toincrease the sensitivity of isolated hepatocytes to allyl alcohol.Furthermore, hepatocytes isolated from rats treated 2 h earlierwith LPS (i.e., hepatocytes which were exposed in vivo to TNF ${alpha}$ and other inflammatory mediators) were no more sensitive toallyl alcohol-induced cytotoxicity than hepatocytes from naïverats. These data suggest that circulating TNF ${alpha}$ is not involvedin the mechanism by which LPS enhances hepatotoxicity of allylalcohol and that the protective effect of PTX may be due toanother of its biological effects.

Key Words: tumor necrosis factor-alpha (TNF ${alpha}$ ); liver damage; Kupffer cells; allyl alcohol.

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