Reduced nonspecific bronchial reactivity and decreased airway response to antigen challenge in atopic asthmatic patients treated with the inhaled leukotriene D 4 antagonist, L‐648,051

We studied the effect of the inhaled leukotriene D 4 antagonist, L‐648,051, on antigen‐induced bronchoconstriction and nonspecific bronchial reactivity. Ten males with mild atopic asthma completed a double‐blind, randomized, two‐period, placebo‐controlled cross‐over study. For a 7‐day period patients inhaled either placebo or 6 mg of L‐648,051 four times daily. Bronchial reactivity to methacholine was measured at base line (day 1) and after 6 days, treatment (day 7). On day 8, after inhaling 6 mg of the antagonist (or placebo), the patients were challenged by inhaled antigen; they received an additional 6 mg of the antagonist (or placebo) 3 h later. Pulmonary function (forced expiratory volume in 1 s, FEV 1 ) was measured serially through an 8‐h post‐antigen challenge. Nonspecific airway reactivity was again measured on day 9. Compared to placebo, L‐648,051 treatment diminished the methacholine reactivity, on both day 7 (NS) and on day 9 ( P <0.05). In addition, the immediate and late bronchial responses to antigen challenge on day 8 were attenuated in the patients when treated with L‐648,051. In the immediate phase (0–3 h postchallenge), the airway response was significantly reduced at all recordings between 20 min and 1 h postchallenge. In the late phase (3–8 h postchallenge), the pulmonary response was also reduced. However, the reduction was statistically significant only at the 5–h recording. The results suggest that sulfidopeptide leukotrienes are of importance for nonspecific airway reactivity, and that leukotriene D 4 is a significant mediator in the immediate asthmatic reaction.