Short-term Exposure to Nitrogen Dioxide Enhances Susceptibility to Murine Respiratory Mycoplasmosis and Decreases Intrapulmonary Killing ofMycoplasma pulmonis
- 1 August 1989
- journal article
- research article
- Published by American Thoracic Society in American Review of Respiratory Disease
- Vol. 140 (2), 502-512
- https://doi.org/10.1164/ajrccm/140.2.502
Abstract
In C57BL/6N and C3H/HeN mice known to be free of all murine pathogens and matched for age, sex, microbiologic, and environmental factors, exposure to NO2 for 4 h prior to exposure to infectious aerosols of Mycoplasma pulmonis resulted in potentiation of murine respiratory mycoplasmosis (MRM). In the C57BL/6N mice, NO2 increased the incidence of death, incidence of gross lung lesions, and incidence of microscopic lung lesions, but did not increase the incidence of infection in the lungs. Nitrogen dioxide affected the C3H/HeN mice (a strain known to be more susceptible than the C57BL/6N strain to MRM) similarly, with the exception that the incidence of death and microscopic lesions were not affected in this strain at the concentrations of M. pulmonis used. Exposure to the oxidant also increased the severity of microscopic lesions and the number of Mycoplasma organisms in the lungs of both mouse strains. Thus, NO2 appeared to affect host lung defense mechanisms responsible for limiting the extent of infection. The NO2 exposure level required to produce potentiation varied with the genetic background of the host, the number of Mycoplasma organisms administered, and the end point measured. In further experiments in C57BL/6N mice, exposure to 5 or 10 ppm of NO2 for 4 h prior to infection with aerosolized, radiolabeled M. pulmonis reduced clearance of these organisms from the lungs over a 72-h time period. Nitrogen dioxide exposure did not change the rate of physical removal of Mycoplasma organisms from the lung. Reduced clearance was due to impaired intrapulmonary killing of Mycoplasma organisms in NO2-exposed mice. In filtered-air control mice, there were no increases in leukocytes recovered from mechanically disaggregated lungs within 72 h after injection. In contrast, by that time after infection, NO2-exposed mice showed a 400% increase in neutrophil numbers, which occurred after changes in mycoplasmacidal activity. No differences were found in the level of specific anti-M. pulmonis IgM in the sera of NO2-exposed and filtered-air control mice. These results directly link decreased pulmonary clearance after NO2 exposure with increased disease severity.This publication has 17 references indexed in Scilit:
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