4.7 Article

Association between pulmonary function and sputum biomarkers in cystic fibrosis

Journal

Publisher

AMER THORACIC SOC
DOI: 10.1164/rccm.200609-1354OC

Keywords

cystic fibrosis; pulmonary function; sputum; infection; inflammation

Funding

  1. NCRR NIH HHS [M01-RR00037, M01-RR00069] Funding Source: Medline

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Rationale: Sputum biomarkers of infection and inflammation are noninvasive measures that enable quantification of the complex pathophysiology of cystic fibrosis (CF) lung disease. Validation of these biomarkers as correlates of disease severity is a key step for their application. Objectives: We constructed a large database from four multicenter studies to quantify the strength of association between expectorated sputum biomarkers and FEV1, Methods: FEV1 (range, 25-120% predicted) and quantitative data on expectorated sputum biomarkers including free neutrophil elastase, IL-8, neutrophils, Pseudomonas aeruginosa, and Staphylococcus aureus were obtained from 269 participants (ages, 9-54 years) from 33 centers. Cross-sectional and longitudinal statistical analyses were performed to estimate associations between the markers and FEV1, including the use of multivariable analyses. \ Results: Elastase was negatively correlated with FEV1 (correlation [r] - -0.35; 95% confidence interval [Cl]: -0.46, -0.22). On average, patients with CF who differed in their elastase measurements by 0.5 log differed in their FEV, values by -7.3% (95% Cl: -9.7, -4.6). Neutrophil counts and IL-8 were also each negatively correlated. In a multivariable regression, elastase and neutrophil counts were able to explain the majority of variation in FEV1. Elastase was further shown to have a significant longitudinal association with FEV, specifically a -2.9% decline in FEV, (95% Cl: -5.0, -0.9) per 1-log increase in elastase. Although correlated with FEV1, bacterial densities were unable to explain clinically meaningful differences in FEV, within and across patients. Conclusions: These data support the role of sputum biomarkers as correlates of disease severity in a diverse CIF population.

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