Mortality in Dioxin-Exposed Mice Infected with Influenza: Mitochondrial Toxicity (Reye's-Like Syndrome) Versus Enhanced Inflammation as the Mode of Action

doi:10.1093/toxsci/69.1.109

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Toxicological Sciences 69, 109-116 (2002)
Copyright © 2002 by the Society of Toxicology

IMMUNOTOXICOLOGY

Mortality in Dioxin-Exposed Mice Infected with Influenza: Mitochondrial Toxicity (Reye's-Like Syndrome) Versus Enhanced Inflammation as the Mode of Action

Robert W. Luebke¹, Carey B. Copeland, Lisa R. Bishop, Mary J. Daniels and M. Ian Gilmour

Immunotoxicology Branch, Experimental Toxicology Division, National Health and Environmental Effects Research Laboratory, Office of Research and Development, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina 27711

Increased mortality following influenza A infection was reportedin B6C3F1 mice exposed to a low (0.01 µg/kg) dose of dioxin.However, mortality was not associated with increased viral loadand antibody titers to the virus were not decreased at dosesof TCDD $<=$ 10 µg/kg, suggesting that viral overgrowth, secondaryto immunosuppression, was not the proximate cause of death.We tested the hypothesis that mitochondrial toxicity and dysfunction,similar to Reye's syndrome (RS) in humans, is responsible forincreased mortality in dioxin-exposed, infected B6C3F1 femalemice, based on similarities in the biochemical and immunologicalevents that occur in RS and in TCDD-exposed animals. Endpointswere also included to test the hypothesis that increased pulmonaryinflammation following dioxin exposure, in the absence of mitochondrialtoxicity, was associated with increased mortality. Dose-relatedeffects of TCDD alone, infection with influenza A alone, andcombined TCDD exposure/influenza infection were evaluated. Micewere given a single ip injection of 0, 0.001, 0.01, 0.1, or1.0 µg TCDD/kg, 7 days before infection by intranasalinstillation of an estimated LD_10–20 of influenza A HongKong/8/68 (H3N2) and were terminated 1, 7, and 10 days afterinfection. Serum, bronchoalveolar lavage fluid (BALF), and lungtissue were collected for various measurements, including clinicalchemistries, cell counts, cytokine analysis, and viral titers.Exposure to $<=$ 1.0 µg TCDD/kg did not increase mortality;virus titers were similar at all doses of TCDD and there wasno dioxin-related effect on serum NH₃ or glucose concentrations,two prominent indicators of the altered mitochondrial oxidativemetabolism typically observed in RS. A study was therefore conductedover a wider range of TCDD doses. A single injection of 0, 0.025,0.5, or 10 µg TCDD/kg preceded infection by 7 days; subgroupsof noninfected control and highest dose group (10 µg TCDD/kg)mice were also evaluated for biochemical and immunological endpointson the equivalent of infection day 4 to provide baseline data.Five days after infection the same endpoints described abovewere evaluated. The 10 µg TCDD/kg dose increased mortality,but once again did not increase virus titer; as in previousexperiments, serum biochemistry endpoints did not support mitochondrialdysfunction. These results suggest that RS is an unlikely explanationfor increased influenza mortality in TCDD-exposed mice. Rather,constituents in BALF implicate increased pulmonary inflammationas the mode of TCDD action.

Key Words: dioxin; immunotoxicity; host resistance; Reye's Syndrome; influenza infection; pulmonary inflammation.

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