Mechanisms of leukotriene‐induced contractions of guinea pig airways: Leukotriene C4 has a potent direct action whereas leukotriene B4 acts indirectly

Abstract

The leukotrienes (LT's) are a group of arachidonic acid derivatives implicated as mediators of allergic bronchoconstriction and acute inflammation. Tracheal spirals and strips of lung parenchyma from guinea pigs were used under non-flow conditions to characterize the contractions caused by LTA₄, LTB₄ and LTC₄. Cumulative administrations of leukotrienes desensitized the lung strip, whereas non-cumulative dose-response relationships for the leukotrienes and histamine were reasonably parallel. Half maximal contractions of the lung strips were obtained at a final bath concentration of 1 nM for LTC₄ and 300 nM for LTA₄ or LTB₄, as compared with 6000 nM for histamine. In the trachea, LTC₄ was approximately 100 times more potent than LTA₄ and histamine. Leukotrienes B₄ and C₄, but not acetylcholine or histamine, elicited release of the bronchoconstrictive thromboxane A₂ from the lung under non-flow conditions. Indomethacin blocked the contractile response to LTB₄, whereas the contractile effect of LTC₄ remained unaltered. The β-adrenoceptor agonist isoproterenol and the LTC₄ antagonist FPL 55712 attenuated the contraction, but not the release of thromboxane A₂, induced by LTC₄. Changing to a perifusion technique rendered the lung strips less sensitive to the direct action of LTC₄, and released thromboxane A₂ now contributed significantly to the contractile response. In addition, the perifusion experiments indicated that LTB₄ released histamine as well. We conclude that the chemoattractant LTB₄ is an indirectly acting bronchoconstrictor, whereas the slow reacting substance LTC₄ contracts the airway muscle by a predominantly direct mechanism. The exquisite bronchoconstrictive activity of LTC₄ may be unrelated to its ability to induce formation of thromboxane A₂.