Factors that Influence the Suppression of Pulmonary Antibacterial Defenses in Mice Exposed to Ozone

Abstract

Exposure to ozone (O₃) has been shown to increase susceptibility of mice to bacterial infection; however, the underlying mechanism has not been well elucidated. This study investigated the effect of O₃ exposure on the ability of mice to combat an infectious challenge of Streptococcus zooepidemicus. Following a 3-h exposure to either air, 0.4 ppm O₃, or 0.8 ppm O₃, 5- and 9-week-old mice received an aerosol infection of bacteria. Intrapulmonary killing of the bacteria was impaired in the Oyexposed mice. The effect was most severe at the higher dose of O₃ in the younger mice, and showed good correlation to subsequent mortality assessed over a 20-day period. Alveolar macrophages (AM) from O₃-exposed mice had an impaired ability to phagocytose the bacteria. Additionally, prostaglandin E₂ (PGE₂) levels, which are known to depress AM function, were increased in the bronchoalveolar lavage fluid of the younger mice following exposure to O₃, while pretreatment with indomethacin in the drinking water blunted the increased of PGE₂ and reduced O₃ enhanced mortality from 53 to 33%. The data show that O₃ inhalation can reduce the defensive capability of the murine lung and that this is associated with a reduction in AM phagocytosis. The defect is more marked in young mice, suggesting that they may be more susceptible to oxidant exposure. Further studies are required to distinguish between direct toxicity of O₃ on the AM and indirect suppression due to modulation of pharmacologic or inflammatory mediators.