[HTML][HTML] Physiological Impact of Abnormal Lipoxin A4 Production on Cystic Fibrosis Airway Epithelium and Therapeutic Potential

G Higgins, F Ringholz, P Buchanan… - BioMed Research …, 2015 - hindawi.com
G Higgins, F Ringholz, P Buchanan, P McNally, V Urbach
BioMed Research International, 2015hindawi.com
Lipoxin A 4 has been described as a major signal for the resolution of inflammation and is
abnormally produced in the lungs of patients with cystic fibrosis (CF). In CF, the loss of
chloride transport caused by the mutation in the cystic fibrosis transmembrane conductance
regulator (CFTR) Cl− channel gene results in dehydration, mucus plugging, and reduction of
the airway surface liquid layer (ASL) height which favour chronic lung infection and
neutrophil based inflammation leading to progressive lung destruction and early death of …
Lipoxin A4 has been described as a major signal for the resolution of inflammation and is abnormally produced in the lungs of patients with cystic fibrosis (CF). In CF, the loss of chloride transport caused by the mutation in the cystic fibrosis transmembrane conductance regulator (CFTR) Cl channel gene results in dehydration, mucus plugging, and reduction of the airway surface liquid layer (ASL) height which favour chronic lung infection and neutrophil based inflammation leading to progressive lung destruction and early death of people with CF. This review highlights the unique ability of LXA4 to restore airway surface hydration, to stimulate airway epithelial repair, and to antagonise the proinflammatory program of the CF airway, circumventing some of the most difficult aspects of CF pathophysiology. The report points out novel aspects of the cellular mechanism involved in the physiological response to LXA4, including release of ATP from airway epithelial cell via pannexin channel and subsequent activation of and P2Y11 purinoreceptor. Therefore, inadequate endogenous LXA4 biosynthesis reported in CF exacerbates the ion transport abnormality and defective mucociliary clearance, in addition to impairing the resolution of inflammation, thus amplifying the vicious circle of airway dehydration, chronic infection, and inflammation.
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