Progression of Airway Dysplasia and C-reactive Protein in Smokers at High Risk of Lung Cancer

doi:10.1164/rccm.200508-1305OC

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Progression of Airway Dysplasia and C-reactive Protein in Smokers at High Risk of Lung Cancer

Don D Sin¹, S.F. Paul Man¹, Annette McWilliams², and Stephen Lam³^*

¹ Department of Medicine (Division of Respirology), University of British Columbia, Vancouver, BC, Canada; Department of Medicine, James Hogg iCAPTURE Center for Cardiovascular and Pulmonary Research, Vancouver, BC, Canada, ² Department of Medicine, British Columbia Cancer Agency (Lung Tumor Group), Vancouver, BC, Canada, ³ Department of Medicine, James Hogg iCAPTURE Center for Cardiovascular and Pulmonary Research, Vancouver, BC, Canada; Department of Medicine, British Columbia Cancer Agency (Lung Tumor Group), Vancouver, BC, Canada

^* To whom correspondence should be addressed. E-mail: slam{at}bccancer.bc.ca.

Rationale : Chronic inflammation has been implicated in thedevelopment of airway dysplasia and lung cancer. It is unclearwhether circulating biomarkers of inflammation could be usedto predict progression of airway dysplasia. Objective: We determinedwhether circulating levels of C-reactive protein (CRP) or otherinflammatory biomarkers could predict progression of bronchialdysplasia in smokers over 6 months. Methods: The plasma levelsof CRP, interleukin (IL)-6, and 8 and monocyte chemoattractantprotein-1 were measured at baseline in 65 ex-and current smokerswho had at least one site of bronchial dysplasia > 1.2 mmin size. Additional bronchial biopsies were taken after 6 monthsfrom the same sites where dysplastic lesions were discoveredat baseline. Progressive dysplastic lesions were defined asworsening of the dysplastic lesion by at least two grades ordevelopment of new dsyplastic lesions. Results: Half of theparticipants developed progressive dysplastic lesions after6 months. The baseline CRP levels in these participants were64% higher than those without progressive disease (P=0.027).Only 1 out of 8 (13%) participants with CRP $≤$ 0.5 mg/L developedprogressive disease, while 31 out of 57 (54%) participants withCRP > 0.5 mg/L developed progressive disease (p=0.011). Theodds of developing progressive disease were 9.6 fold higherin the latter than in the former group. Conclusion: PlasmaCRP, in concert with lung function, and pack-years of smoking,appear to have excellent predictive powers in identifying participantswith bronchial dyplastic lesions whose lesions progress to moreadvanced stages of dysplasia.

Key words: C-reactive protein, airway dysplasia, lung inflammation

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