Figure 9. Determining whether the ATP/P2X₇ axis is central to the exacerbation response in vivo.

Mice (n = 8 per group) were challenged with the aerosolised vehicle of endotoxin-free saline or LPS (1 mg/ml) in Perspex chambers for 30 minutes. Four hours later the mice were intranasally dosed with saline (2 ml/kg) or ATPγs (0.001 mg/kg) whilst under light anaesthesia (4% isoflurane in oxygen). The mice received oral vehicle or P2X₇ inhibitor, A438079, 30 minutes prior to the ATP challenge, 4 hours after the challenge and 1 hour prior to cull. Twenty four hours after the LPS exposure the mice were culled and lavaged. IL-1β (A) and neutrophil (B) numbers were measured in the BALF. Data shown as mean +/− S.E.M. An unpaired T-test was used for the statistical analysis. *  = P = 0.0378 (Panel A); *  = P = 0.0162 (Panel B).