Am. J. Respir. Cell Mol. Biol., Vol 13, No. 4, 10 1995, 426-433.
Regulation of rat pulmonary dendritic cell immunostimulatory activity by alveolar epithelial cell-derived granulocyte macrophage colony- stimulating factor
PJ Christensen, LR Armstrong, JJ Fak, GH Chen, RA McDonald, GB Toews and R Paine 3rd
Pulmonary Section, VA Medical Center, Ann Arbor, Michigan, USA.
The presentation and recognition of foreign antigen is the critical initial
event in the development of local immunity. In the lung, antigen-presenting
cell activity is largely attributable to pulmonary dendritic cells (DC)
that are distributed along the airways and throughout the pulmonary
interstitium in close proximity to overlying alveolar epithelial cells. To
test the hypothesis that DC immunostimulatory activity might be locally
regulated by overlying alveolar epithelial cells, we evaluated the ability
of rat type II alveolar epithelial cells to influence the capacity of
purified rat pulmonary DC to stimulate T-cell proliferation in an
allogeneic, mixed leukocyte reaction. We found that alveolar epithelial
cells greatly enhanced the ability of dendritic cells to induce T-cell
proliferation. This effect on DC immunostimulatory activity was mediated by
a soluble factor preferentially secreted from the basolateral epithelial
cell surface. Alveolar epithelial cultures were found to express mRNA for
granulocyte macrophage colony-stimulating factor (GM-CSF), and blocking
antibodies against GM-CSF partially neutralized the effect of epithelial
cell-conditioned media on DC stimulatory activity, indicating that the
effect was due at least in part to alveolar epithelial cell-derived GM-CSF.
Through the polar secretion of GM-CSF, alveolar epithelial cells may play
an important role in creating distinct immunologic environments within the
lung.
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Copyright © 1995 American Thoracic Society.
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