Competitive swimmers with allergic asthma show a mixed type of airway inflammation

To the Editors: 

Elite swimmers are at increased risk of asthma 1. This has been attributed to airway inflammation and increased airway responsiveness induced by high-intensity long-term exercise and repeated exposure to the chlorine-rich atmosphere in swimming pools during training and competition 2, 3. Recently, increased levels of leukotriene (LT)B4 in exhaled breath condensate and normal exhaled nitric oxide fraction ( F eNO) levels have been reported in five elite swimmers, suggesting possible underlying neutrophilic airway inflammation 4. Previous analysis of induced sputum in nonasthmatic elite swimmers showed increased proportion of eosinophils and neutrophils compared with healthy controls 3.

We aimed to characterise the airway inflammation in competitive asthmatic swimmers. Athletes from the FC Porto main swimming team and 20 nonathlete asthmatics were recruited; participants gave informed consent. Subjects were classified by their asthma and training status as asthmatic swimmers (n = 6, two female, aged 17±2 yrs, competing 8±3 yrs, training 16±4 h·week−1), asthmatics (n = 20, eight female, aged 14±3 yrs) and swimmers (n = 20, six female, aged 17±2 yrs, competing 8±3 yrs, training 17±3 h·week−1).

All asthmatics and nine (45%) of the swimmers were atopic according …

Competitive swimmers with allergic asthma show a mixed type of airway inflammation To the Editors: Elite swimmers are at increased risk of asthma [1]. This has been attributed to airway inflammation and increased airway responsiveness induced by high-intensity long-term exercise and repeated exposure to the chlorine-rich atmosphere in swimming pools during training and competition [2,3]. Recently, increased levels of leukotriene (LT)B 4 in exhaled breath condensate and normal exhaled nitric oxide fraction (FeNO) levels have been reported in five elite swimmers, suggesting possible underlying neutrophilic airway inflammation [4]. Previous analysis of induced sputum in nonasthmatic elite swimmers showed increased proportion of eosinophils and neutrophils compared with healthy controls [3].
All asthmatics and nine (45%) of the swimmers were atopic according to skin-prick test results. None smoked. During two visits to the clinic, 1 week apart, subjects' sputum cell counts, FeNO, lung volumes and airway responsiveness to methacholine (provocative dose causing a 20% fall in forced expiratory volume in one second (FEV1); PD20) were determined. Sputum cell counts were further compared with reference values from a group of healthy schoolchildren (n515, five female, aged 9¡2 yrs, 40% atopic) [5]. Sputum was examined as described previously [3]. Briefly, after induction using an inhalation of hypertonic saline, sputum was selected and treated with dithiothreitol (Sputolysin1; Calbiochem Corporation, San Diego, CA, USA). The suspension was centrifuged and the cell pellet was resuspended. Cytospins were prepared and stained using May-Grü nwald/Giemsa. Differential cell counts were made by counting a minimum of 500 nonsquamous cells. FeNO was measured by chemiluminescence (NIOX; Aerocrine, Stockholm, Sweden) and PD20 methacholine was determined using the dosimeter method, according to recommendations [6,7]. ANOVA was used to detect differences between groups. Due to the skewed distribution, eosinophil counts and PD20 methacholine comparisons were made after logarithmic transformation. In order to permit analysis in the log scale, a constant (0.01) was added to each value to eliminate 0 values. A p-value ,0.05 was considered to be stastically significant.
Induced sputum samples of asthmatic swimmers showed increased numbers of eosinophils and neutrophils compared with both healthy subjects and asthmatic patients respectively, and lymphocytes compared with healthy subjects, although the numbers were approximately the same as in swimmers or c asthmatic patients. Asthmatic swimmers had a similar magnitude of FeNO but significantly more pronounced airway responsiveness than asthmatics ( fig. 1).
Features of asthma in competitive swimmers seem to be the result of mixed type effects. Although the cross-sectional nature of our study does not allow us to establish causal relationships, allergic inflammation results in sputum eosinophilia and increased FeNO, while sputum neutrophils may result from the daily exposure of the pool training environment. Increased bronchial responsiveness and lymphocyte numbers could be the result of both processes as they occurred similarly in swimmers and asthmatics.
Two factors could contribute to the neutrophilic airway inflammation in asthmatic competitive swimmers. First, endurance exercise associated hyperventilation and the inhalation of hypotonic aerosolised droplets from the pool surface during training may cause epithelial damage [1] and subsequent inflammation. Secondly, chronic low-grade exposure to chlorine derivatives may be related to the observed increased levels of exhaled LTB 4 in elite swimmers [4]. This observation is also supported by the findings in children accidentally exposed to chlorine, with development of respiratory symptoms, lung function impairment and exhaled breath alterations, represented mainly by an increase in LTs and a decrease in FeNO [8]. If this is the case, new therapeutic approaches that, in addition to inhaled corticosteroids, would target the 5-lipoxygenase pathway could have a role attenuating the neutrophilic airway inflammation in swimmers with asthma.
In conclusion, asthma in allergic competitive swimmers is characterised by mixed type of eosinophilic and neutrophilic inflammation, which increase normal exhaled nitric oxide fraction and cause airway hyperresponsiveness. Daily exposure to aerosolised water droplets and chlorine derivatives probably contribute to the neutrophilic inflammation, which might respond poorly to standard asthma medication.