Abstract
BackgroundNitric oxide (NO) is produced within the respiratory tract and can be detected in exhaled bronchial and nasal air. The concentration varies in specific diseases, being elevated in patients with asthma and bronchiectasis, but decreased in primary ciliary dyskinesia. In cystic fibrosis (CF), conflicting data exist on NO levels, which are reported unexplained as either decreased or normal. Functionally, NO production in the paranasal sinuses is considered as a location-specific first-line defence mechanism. The aim of this study was to investigate the correlation between upper and lower airway NO levels and blood inflammatory parameters, CF-pathogen colonisation, and clinical data.Methods and FindingsNasal and bronchial NO concentrations from 57 CF patients were determined using an electrochemical analyser and correlated to pathogen colonisation of the upper and lower airways which were microbiologically assessed from nasal lavage and sputum samples. Statistical analyses were performed with respect to clinical parameters (lung function, BMI), laboratory findings (CRP, leucocytes, total-IgG, fibrinogen), and anti-inflammatory and antibiotic therapy. There were significant correlations between nasal and bronchial NO levels (rho = 0.48, p<0.001), but no correlation between NO levels and specific pathogen colonisation. In patients receiving azithromycin, significantly reduced bronchial NO and a tendency to reduced nasal NO could be found. Interestingly, a significant inverse correlation of nasal NO to CRP (rho = −0.28, p = 0.04) and to leucocytes (rho = −0.41, p = 0.003) was observed. In contrast, bronchial NO levels showed no correlation to clinical or inflammatory parameters.ConclusionGiven that NO in the paranasal sinuses is part of the first-line defence mechanism against pathogens, our finding of reduced nasal NO in CF patients with elevated systemic inflammatory markers indicates impaired upper airway defence. This may facilitate further pathogen acquisition in the sinonasal area, with consequences for lung colonisation and the overall outcome in CF.
Highlights
Cystic fibrosis (CF) is one of the most frequent autosomal recessive disorders in Caucasians
Upper airway sampling does not belong to the current standards, but nasal lavage enables a noninvasive and repeated sampling that can be used as a supplementary diagnostic tool [2,4,5]
The body mass index (BMI) was used as nutritional status indicator for adult patients, while BMI percentiles were used for children
Summary
Cystic fibrosis (CF) is one of the most frequent autosomal recessive disorders in Caucasians. The upper airways (UAW), especially the nasal cavity and paranasal sinuses have come into scientific focus as site of first and persistent airway colonisation in CF. In this regard, anatomical and immunological conditions facilitating sinonasal colonisation with pathogens are of special interest [1,2]. The standard of airway sampling in CF comprises the lower airways with sputum, throat swab, and – for special scientific and clinical questions – bronchoalveolar lavage [3]. The aim of this study was to investigate the correlation between upper and lower airway NO levels and blood inflammatory parameters, CF-pathogen colonisation, and clinical data
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