Am. J. Respir. Cell Mol. Biol., Vol 13, No. 4, 10 1995, 477-486.
Cellular infiltration and eicosanoid synthesis in brown Norway rat lungs after allergen challenge
W Yu, L Xu, JG Martin and WS Powell
Meakins-Christie Laboratories, Department of Medicine, McGill University, Montreal, Quebec, Canada.
Allergen challenge of sensitized Brown-Norway (BN) rats results in
increased excretion of cysteinyl-leukotrienes (cLTs) in bile. It is unclear
whether this reflects an increased capacity of lung cells to synthesize
5-lipoxygenase products, and, if so, which cells are of primary importance.
We have examined the effects of allergen challenge on the capacity of a
mixture of isolated lung cells from ovalbumin (OA)- sensitized BN rats to
synthesize LTs and other eicosanoids. Cells were isolated by enzymatic
digestion of lung tissue before and either 6 or 24 h after challenge of
sensitized rats with either OA or saline. A23187-induced synthesis of
eicosanoids by these cells was measured using high-pressure liquid
chromatography. OA challenge resulted in a significant influx of
neutrophils into the lungs and a significant increase in the synthesis of
5-lipoxygenase products, in particular LTB4, by lung cells after 6 h. There
was a positive correlation between the percentage of neutrophils in
unfractionated lung cells and the amounts of LTB4 produced by these cells.
OA challenge had little or no effect on the production of cLTs and the
cyclooxygenase product 12- hydroxy-5,8,10-heptadecatrienoic acid. There was
a significant increase in the infiltration of eosinophils into the lungs 24
h after OA challenge but no increase in the production of cLTs by lung
cells at this time, suggesting that eosinophils from BN rats are unlikely
to be the major site for the production of these substances. This was
confirmed in experiments with partially purified eosinophils obtained from
Sephadex-treated rats. In contrast, cLTs were major products of arachidonic
acid metabolism by alveolar macrophages from BN rats. We conclude that
allergen challenge results in an increased capacity of lung cells to
synthesize 5-lipoxygenase products, in particular LTB4. Macrophages, rather
than eosinophils, may be an important site for the synthesis of cLTs in BN
rat lungs.
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Copyright © 1995 American Thoracic Society.
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