Efficient killing of inhaled bacteria in ΔF508 mice:: role of airway surface liquid composition

Cystic fibrosis mice have been generated by gene targeting but show little lung disease without repeated exposure to bacteria. We asked if murine mucosal defenses and airway surface liquid (ASL) Cl- were altered by the Delta F508 cystic fibrosis transmembrane conductance regulator mutation. Naive Delta F508 -/- and +/- mice showed no pulmonary inflammation and after inhaled Pseudomonas aeruginosa had similar inflammatory responses and bacterial clearance rates. We therefore investigated components of the innate immune system. Bronchoalveolar lavage fluid from mice killed Escherichia coli, and the microbicidal activity was inhibited by NaCl. Because beta-defensins are salt-sensitive epithelial products, we looked for pulmonary beta-defensin expression. A mouse homolog of human beta-defensin-1 (termed "MBD-1") was identified; the mRNA was expressed in the lung. Using a radiotracer technique, ASL volume and Cl- concentration ([Cl-]) were measured in cultured tracheal epithelia from normal and Delta F508 -/- mice. The estimated ASL volume was similar for both groups. There were no differences in ASL [Cl-] in Delta FS08 -/- and normal mice (13.8 +/- 2.6 vs. 17.8 +/- 5.6 meq/l). Because ASL [Cl-] is low in normal and mutant mice, salt-sensitive antimicrobial factors, including MBD-1, may be normally active.