Complement Activation Is Critical to Airway Hyperresponsiveness after Acute Ozone Exposure

Abstract

Ozone (O₃) can induce airway hyperresponsiveness (AHR) and neutrophilic inflammation. We evaluated the role of complement in development of AHR and inflammation after acute O₃ exposure in mice. Mice were exposed to O₃ at 2 ppm for 3 hours, and airway responsiveness to methacholine was measured 8 hours after O₃ exposure. Complement was depleted or inhibited by intraperitoneal injection of cobra venom factor (CVF) or complement receptor–related gene y (Crry)–Ig, a potent C3 convertase inhibitor; neutrophils were depleted using an antineutrophil monoclonal antibody. CVF attenuated the development of AHR by O₃. Administration of Crry–Ig also prevented the development of AHR. Bronchoalveolar lavage (BAL) fluid neutrophilia after O₃ exposure was significantly decreased by administration of either CVF or Crry–Ig. Increased BAL fluid total protein after O₃ exposure was lowered by depletion or inhibition of complement. In contrast to the effects of complement inhibition or depletion, depletion of BAL neutrophil counts by more than 90% with the monoclonal antibody did not affect the development of AHR after O₃ exposure. These data indicated that activation of the complement system follows acute O₃ exposure and is important to the development of AHR and airway neutrophilia. However, this neutrophil response does not appear necessary for the development of AHR.