Acute exacerbation of idiopathic pulmonary fibrosis associated with air pollution exposure

Introduction

Idiopathic pulmonary fibrosis (IPF) is a progressive parenchymal lung disease of unknown cause with an estimated median survival of 2–3 years from the time of diagnosis [1]. It is the most common of the idiopathic interstitial pneumonias and increases in prevalence substantially with age [2]. Many patients with IPF experience sudden stepwise acute respiratory worsenings, which are associated with high mortality [3]. In about half of cases, a cause for the acute worsening (e.g. infection, pulmonary embolism or congestive heart failure) cannot be diagnosed. These idiopathic acute respiratory worsenings are termed acute exacerbations of IPF [4].

Preliminary evidence suggests that some cases of acute exacerbation of IPF may be triggered by occult viral infection [5], microaspiration [6] and procedures such as surgical lung biopsy [7]. However, in the majority of cases a trigger cannot be found. Exposure to environmental triggers, such as ambient air pollution, could be responsible for some of these cases.

The relationship between ambient air pollution and exacerbation of respiratory diseases, such as asthma and chronic obstructive pulmonary disease (COPD), is well established [8–11]. Few studies have investigated the effects of ambient air pollution on interstitial lung diseases, despite epidemiological data linking exposure to inhaled agents, such as cigarette smoke, organic antigens and metal and wood dusts to these conditions. In addition, translational data support a mechanistic relationship between air pollution exposure and the development of pulmonary fibrosis [12–14]. We hypothesised that the risk of acute exacerbations in patients with IPF would be higher following periods of increased air pollution exposure.

This study investigates the relationship between ambient air pollution exposure (ozone (O₃), nitrogen dioxide (NO₂), particles with a 50% cut-off aerodynamic diameter of <10 µm (PM₁₀), sulfur dioxide (SO₂) and carbon monoxide (CO)) and acute exacerbations of IPF in a large, well-characterised cohort with contemporaneous clinical and ambient air pollution data.

Results

Association of air pollution exposure with acute exacerbation risk

Acute exacerbation of IPF was significantly associated with increased mean levels, maximum levels, and number of exceedances of O₃ and NO₂ during the exposure period (fig. 1). There were no consistent relationships between PM₁₀, SO₂ or CO and acute exacerbation of IPF. Mean O₃ and NO₂ were weakly correlated and both were statistically significant independent predictors of acute exacerbation in a two-pollutant model. Hazard ratios for all five exposures remained consistent when cases were limited to only those occurring within 15 km of a monitoring station, those able to be corrected for temperature and humidity, or when all acute exacerbations (including those occurring in patients who had previously experienced an acute exacerbation) were included (table 2). O₃ and NO₂ exposures remained generally associated with acute exacerbation when varying the exposure period from 1 to 8 weeks prior to acute exacerbation diagnosis (fig. 2 and online supplementary table S1). The associations with O₃ and NO₂ were also consistent when exceedance analyses were performed according to alternative published reference standards or guidelines (online supplementary table S2). Finally, these associations remained consistent when adjusted for history of prednisone and/or GORD therapy use (data not shown).

• Download figure
• Open in new tab
• Download powerpoint

Figure 1–

Ozone (O₃) and nitrogen dioxide (NO₂) exposure and risk of acute exacerbation. Mean levels, maximum levels and number of exceedances above standards for O₃ and NO₂ exposure over a 6-week period were associated with significantly increased risk for acute exacerbation of idiopathic pulmonary fibrosis. There was no association of particulate matter <10 μm in aerodynamic diameter (PM₁₀), carbon monoxide (CO) or sulfur dioxide (SO₂) exposure with acute exacerbation risk. There were no exceedances above CO or SO₂ standards. HR: hazard ratio.

View this table:

• View inline
• View popup

Table 2– Secondary analyses for air pollution exposure and risk of acute exacerbation

• Download figure
• Open in new tab
• Download powerpoint

Figure 2–

Secondary sensitivity analyses for a) ozone and b) nitrogen dioxide exposures and risk of acute exacerbation, which show a consistent relationship with acute exacerbation across multiple cumulative exposure periods. HR: hazard ratio.

Discussion

Our study demonstrates a significant relationship between ambient O₃ and NO₂ levels and acute exacerbation of IPF, suggesting that increased exposure to these pollutants contributes to the development of acute exacerbation in some patients. The magnitude of the associated risk is comparable to what has been reported for exacerbation of other chronic lung diseases [10, 18, 19]. To our knowledge this is the first report describing this association in IPF. Air pollution is a potentially modifiable risk factor either via behavioural adaptation of the patient (i.e. exposure avoidance) or community-level reductions in exposure through environmental policy. Our findings suggest that reductions in ambient air pollution exposure may decrease the risk of acute exacerbation and improve the morbidity associated with IPF.

Based on the clinical presentations of patients with acute exacerbations of IPF, we hypothesised that ambient air pollution-associated events, unlike acute exacerbation of asthma or acute myocardial infarction, would have a delayed clinical presentation. The 6-week exposure period was defined a priori based on the assumption that an interval of up to 30 days might occur between symptom onset (and therefore likely exposure risk) and time of diagnosis, and to allow for a potential lag-time from pollutant exposure to symptom development. Sensitivity analyses varying the exposure period from 1 to 8 weeks prior to acute exacerbation demonstrated a consistent association, strengthening the results, and suggesting that the exposure period of highest risk lies between 2 and 8 weeks before diagnosis. Because O₃ levels are known to be lower during the winter and at night, outcomes were analysed in relation to peak O₃ concentration using 8-h midday levels during the warmer months only, an approach commonly used in epidemiological studies of O₃ [20, 21]. For the exceedance analyses, the United States Environmental Protection Agency National Ambient Air Quality Standards were chosen a priori because they are regulatory standards and not merely guidelines.

O₃ and NO₂ are known risk factors for poor outcomes and exacerbations in chronic lung diseases [22–25]. A long-term population analysis found a relative risk of respiratory-related death of 1.04 for every 10 ppb increase in O₃ [20]. O₃ has been associated with increasing risk for the development of airways diseases like asthma and with increased exacerbation risk in asthma and cystic fibrosis [18, 23, 26]. NO₂ exposure has been associated with increased risk of respiratory hospitalisation in COPD and asthma, and traffic-related air pollution exposure increases the risk of post lung transplant bronchiolitis obliterans syndrome [8–10, 19]. It is not entirely surprising, therefore, that exposure to O₃ and NO₂ appear to contribute to worsening of IPF.

Air pollution exposure may trigger acute exacerbation of IPF via the production of excess reactive oxygen species (ROS), such as hydroxide radical and superoxide anion [27]. Intrinsic antioxidants, such as glutathione, are generally capable of counterbalancing the effects of ROS, but when the production of ROS exceeds the lung’s ability to remove them, cellular damage ensues. Patients with IPF have evidence of reduced antioxidant capacity, suggesting they may have increased vulnerability to excess ROS caused by exposure to air pollution [28].

The greatest modifiable source of O₃ and NO₂ in the industrialised world is from motor vehicle emissions. While our results do not inform strategies for exposure reduction, they do suggest that patients with IPF might benefit from avoiding excess pollutant exposure perhaps through reduced physical exertion or staying indoors on days with high air pollution levels. In addition, IPF patients might benefit from relocating to environments with lower emissions and better air quality. At a policy level, adherence to and enforcement of air quality standards may reduce the incidence of acute exacerbation of IPF. Understanding more fully the implications of these findings will require the continued integration of the fields of clinical research, environmental health and public policy.

The IPF cohort used for this study is well-characterised and probably represents the largest such cohort available for this type of analysis, but the sample size is still relatively small for air pollution studies. This makes the consistent relationship between O₃ and NO₂ exposure and acute exacerbation all the more striking. The consistency of hazard ratios across sensitivity analyses further strengthens the reliability of the results. It is possible that significant associations with fine or ultrafine particulate matter were missed, as the only particulate matter metric available for this analysis was PM₁₀. There is the potential for exposure misclassification given that exposure estimates were based on regional air quality monitoring data and, therefore, could not account adequately for individual-level exposure differences such as time spent indoors and in traffic or subregional geographical variation. Reported residential addresses were confirmed before geo-coding, but some patients may have moved or spent significant amounts of time in other locations. Due to the retrospective nature of this study, other potential sources of pollutant exposures (e.g. cooking stoves and biofuels) could not be assessed. Also, it was not possible to adjust for temperature and relative humidity for the whole cohort, but a sensitivity analysis in the subgroup with available temperature and humidity data showed a consistent relationship between air pollution and acute exacerbation.

We did not find any relationship between cigarette smoking, the use of immunosuppressive medications or the use of anti-acid therapies and the risk of acute exacerbation. However, our study’s small numbers and lack of detailed data regarding cigarette smoking and immunosuppressive medication use at the time of exacerbation limit any conclusions regarding these relationships. These questions can best be addressed in large prospective trials.

In summary, these data suggest that exposure to O₃ and NO₂ contributes to the risk of acute exacerbation of IPF, and we speculate that air pollution represents one of a series of factors (e.g. viral infection and microaspiration) that serve as triggers for these clinically important events. It is possible that variations in ambient pollutant exposure contribute to differences in rates of acute exacerbation by geographical region, but further study is required to evaluate this relationship. O₃ and NO₂ have the potential for mitigation through behavioural and environmental policy changes, which could reduce the risk to these susceptible patients. Further research is needed to validate these findings and to better delineate the pathobiological role of air pollution in IPF.