Guinea Pig Lung Lavage Cells After Intranasal BCG Sensitization

Author:

Terai T.1,Ganguly Rama23,Waldman Robert H.2

Affiliation:

1. Department of Medicine, University of Florida, Gainesville, Florida 32610

2. Department of Medicine, West Virginia University Medical Center, Morgantown, West Virginia, 26506

3. Department of Microbiology, West Virginia University Medical Center, Morgantown, West Virginia, 26506

Abstract

Recent studies have suggested that intranasal administration of antigen can induce local cell-mediated immunity in lung lavage cells. The present study was designed to examine the changes in composition of lung lavage cells and their capacity to produce the lymphokine migration inhibitory factor after intranasal immunization with BCG in guinea pigs. Results indicate that guinea pigs responded to respiratory tract BCG infection with an increase in immunocompetent cells in the bronchoalveolar tract and with production of migration inhibitory factor. After local pulmonary BCG administration, the total number of cells increased as compared with that of the uninfected animals, the increase being statistically significant within 2 weeks. This marked increase in the total cell population is due to a more than doubling of the number of macrophages in the lavage fluid. Animals also developed at this time positive delayed hypersensitivity to intradermally administered purified protein derivative. A significant increase in the total lymphoid cells and macrophage population was observed again at 6 weeks after sensitization, suggesting that the response is biphasic in nature. At 6 weeks, however, there was also a significant rise in total lymphocytes and T cell population in addition to macrophage numbers. This increase in T cells correlated with an increase in production of migration inhibitory factor in the presence of purified protein derivative. These data suggest that the immune response of the respiratory tract after BCG challenge involves increased recruitment of immunocompetent cells locally at the site of infection and that these cells are capable of producing effector molecules in terms of the elaboration of migration inhibitory factor.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference20 articles.

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3. Adaptive responses of the pulmonary macrophagic system to carbon. I. Kinetic studies;Boweden D. H.;Lab. Invest.,1978

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5. Migratory response of granulomatous alveolar cells from BCG-sensitized rabbits;Galindo B.;J. Immunol.,1970

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