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大流行时代的慢性阻塞性肺疾病急性加重、空气污染物波动及个体层面因素

COPD Exacerbations, Air Pollutant Fluctuations, and Individual-Level Factors in the Pandemic Era.

作者信息

Mikaeeli Sahar, Doiron Dany, Bourbeau Jean, Li Pei Zhi, Aaron Shawn D, Chapman Kenneth R, Hernandez Paul, Maltais François, Marciniuk Darcy D, O'Donnell Denis E, Sin Don D, Walker Brandie L, Tan Wan C, Rousseau Simon, Ross Bryan A

机构信息

Respiratory Epidemiology and Clinical Research Unit, Centre for Outcomes Research and Evaluation, Research Institute of the McGill University Health Centre (RI-MUHC), Montreal, Quebec, Canada.

Division of Experimental Medicine, Department of Medicine, McGill University Health Centre, Montreal, Quebec, Canada.

出版信息

Int J Chron Obstruct Pulmon Dis. 2025 Mar 17;20:735-751. doi: 10.2147/COPD.S498088. eCollection 2025.

Abstract

PURPOSE

Pandemic-era associations between air pollutant exposures and exacerbations of chronic obstructive pulmonary disease (COPD) are under-explored. Given the considerable observed pandemic-era pollutant fluctuations, these associations were investigated along with possible individual-level risk factors.

PATIENTS AND METHODS

Participants with spirometry-confirmed COPD from Canadian Cohort Obstructive Lung Disease (CanCOLD) were included, with data collected before ("pre-pandemic") and during ("pandemic") the COVID-19 pandemic. Nitrogen dioxide (NO), fine particulate matter (PM), ground-level ozone (O), total oxidant (O) and weather data were obtained from national databases. Associations between each air pollutant and "symptom-based" exacerbations (increased dyspnea or sputum volume/purulence ≥48hrs) and "event-based" exacerbations ("symptom-based" plus requiring antibiotics, corticosteroids, or unscheduled healthcare use) were estimated in separate models. Generalized estimating equations (GEE) models were reported as rate ratios (RRs) per interquartile range (IQR) increment in pollutant concentration with 95% confidence intervals (95% CIs).

RESULTS

NO, PM, and O (NO+O) concentrations (but not O) fell significantly during the pandemic. In the 673 participants with COPD included, both symptom-based and event-based exacerbation rates were likewise significantly higher during the pre-pandemic period. During the pre-pandemic period, O was positively associated with symptom-based exacerbations (RR: 1.21 [1.08,1.36]). During the pandemic period, O was positively associated with symptom-based (1.46 [1.13,1.89]) and event-based (1.43 [1.00,2.05]) exacerbations. Fewer self-reported pandemic protective behaviors, and higher viral infectious symptoms, were also associated with exacerbations. In stepwise multivariable risk-factor analyses, female gender (1.23 [1.04,1.45] and 1.41 [1.13,1.76]) and co-morbid asthma (1.65 [1.34,2.03] and 1.54 [1.19,2.00]) were associated with symptom-based and event-based exacerbations, respectively, blood eosinophils (1.42 [1.10,1.84]) were associated with event-based exacerbations, and each IQR increment in O was associated with symptom-based exacerbations (1.31 [1.06,1.61]).

CONCLUSION

O exposure was consistently associated with symptom-based COPD exacerbations, and female gender, co-morbid asthma, and blood eosinophilia were found to be relevant risk factors.

摘要

目的

大流行时期空气污染物暴露与慢性阻塞性肺疾病(COPD)急性加重之间的关联尚未得到充分研究。鉴于在大流行时期观察到污染物有显著波动,对这些关联以及可能的个体层面风险因素进行了调查。

患者与方法

纳入了来自加拿大阻塞性肺病队列(CanCOLD)且经肺功能测定确诊为COPD的参与者,收集了COVID-19大流行之前(“大流行前”)和期间(“大流行期间”)的数据。二氧化氮(NO)、细颗粒物(PM)、地面臭氧(O₃)、总氧化剂(Ox)和气象数据均从国家数据库中获取。在单独的模型中估计了每种空气污染物与“基于症状的”急性加重(呼吸困难加重或痰液量/脓性增加≥48小时)以及“基于事件的”急性加重(“基于症状的”加上需要使用抗生素、皮质类固醇或非计划的医疗保健服务)之间的关联。广义估计方程(GEE)模型报告为污染物浓度每增加一个四分位数间距(IQR)的率比(RRs)及其95%置信区间(95% CIs)。

结果

大流行期间,NO、PM和O₃(NO + O₃)浓度(但不包括Ox)显著下降。在纳入的673例COPD参与者中,基于症状的和基于事件的急性加重率在大流行前同样显著更高。在大流行前时期,O₃与基于症状的急性加重呈正相关(RR:1.21 [1.08, 1.36])。在大流行期间,O₃与基于症状的(1.46 [1.13, 1.89])和基于事件的(1.43 [1.00, 2.05])急性加重呈正相关。自我报告的大流行防护行为较少以及病毒感染症状较多也与急性加重有关。在逐步多变量风险因素分析中,女性(1.23 [1.04, 1.45] 和1.41 [1.13, 1.76])和合并哮喘(1.65 [1.34, 2.03] 和1.54 [1.19, 2.00])分别与基于症状的和基于事件的急性加重相关,血液嗜酸性粒细胞(1.42 [1.10, 1.84])与基于事件的急性加重相关,并且O₃每增加一个IQR与基于症状的急性加重相关(1.31 [1.06, 1.61])。

结论

O₃暴露始终与基于症状的COPD急性加重相关,并且发现女性、合并哮喘和血液嗜酸性粒细胞增多是相关的风险因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bdff/11928299/90ba8109677f/COPD-20-735-g0001.jpg

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