Pietropaoli Anthony P, Frampton Mark W, Hyde Richard W, Morrow Paul E, Oberdörster Günter, Cox Christopher, Speers Donna M, Frasier Lauren M, Chalupa David C, Huang Li-Shan, Utell Mark J
Department of Medicine, University of Rochester School of Medicine and Dentistry, New York 14642, USA.
Inhal Toxicol. 2004;16 Suppl 1:59-72. doi: 10.1080/08958370490443079.
Particulate air pollution is associated with asthma exacerbations and increased morbidity and mortality from respiratory causes. Ultrafine particles (particles less than 0.1 microm in diameter) may contribute to these adverse effects because they have a higher predicted pulmonary deposition, greater potential to induce pulmonary inflammation, larger surface area, and enhanced oxidant capacity when compared with larger particles on a mass basis. We hypothesized that ultrafine particle exposure would induce airway inflammation in susceptible humans. This hypothesis was tested in a series of randomized, double-blind studies by exposing healthy subjects and mild asthmatic subjects to carbon ultrafine particles versus filtered air. Both exposures were delivered via a mouthpiece system during rest and moderate exercise. Healthy subjects were exposed to particle concentrations of 10, 25, and 50 microg/m(3), while asthmatics were exposed to 10 microg/m(3). Lung function and airway inflammation were assessed by symptom scores, pulmonary function tests, and airway nitric oxide parameters. Airway inflammatory cells were measured via induced sputum analysis in several of the protocols. There were no differences in any of these measurements in normal or asthmatic subjects when exposed to ultrafine particles at concentrations of 10 or 25 microg/m(3). However, exposing 16 normal subjects to the higher concentration of 50 microg/m(3) caused a reduction in maximal midexpiratory flow rate (-4.34 +/- 1.78% [ultrafine particles] vs. +1.08 +/- 1.86% [air], p =.042) and carbon monoxide diffusing capacity (-1.76 +/- 0.66 ml/min/mm Hg [ultrafine particles] vs. -0.18 +/- 0.41 ml/min/mm Hg [air], p =.040) at 21 h after exposure. There were no consistent differences in symptoms, induced sputum, or exhaled nitric oxide parameters in any of these studies. These results suggest that exposure to carbon ultrafine particles results in mild small-airways dysfunction together with impaired alveolar gas exchange in normal subjects. These effects do not appear related to airway inflammation. Additional studies are required to confirm these findings in normal subjects, compare them with additional susceptible patient populations, and determine their pathophysiologic mechanisms.
空气中的微粒污染与哮喘发作以及呼吸系统疾病导致的发病率和死亡率增加有关。超细颗粒(直径小于0.1微米的颗粒)可能会导致这些不良反应,因为与较大颗粒相比,它们在肺部的沉积预测值更高,诱发肺部炎症的潜力更大,表面积更大,且基于质量计算时氧化能力更强。我们假设,接触超细颗粒会在易感人群中诱发气道炎症。通过让健康受试者和轻度哮喘受试者接触碳超细颗粒与过滤空气,在一系列随机双盲研究中对这一假设进行了检验。两种暴露均通过吹嘴系统在休息和适度运动期间进行。健康受试者接触的颗粒浓度为10、25和50微克/立方米,而哮喘患者接触的浓度为10微克/立方米。通过症状评分、肺功能测试和气道一氧化氮参数评估肺功能和气道炎症。在一些方案中,通过诱导痰分析来测量气道炎症细胞。当正常受试者或哮喘患者接触浓度为10或25微克/立方米的超细颗粒时,这些测量结果均无差异。然而,让16名正常受试者接触浓度更高的50微克/立方米的超细颗粒,在接触后21小时导致最大呼气中期流速降低(-4.34±1.78%[超细颗粒]对+1.08±1.86%[空气],p = 0.042)以及一氧化碳弥散量降低(-1.76±0.66毫升/分钟/毫米汞柱[超细颗粒]对-0.18±0.41毫升/分钟/毫米汞柱[空气],p = 0.040)。在这些研究中,症状、诱导痰或呼出一氧化氮参数均无一致差异。这些结果表明,接触碳超细颗粒会导致正常受试者出现轻度小气道功能障碍以及肺泡气体交换受损。这些影响似乎与气道炎症无关。需要进一步的研究来在正常受试者中证实这些发现,将其与其他易感患者群体进行比较,并确定其病理生理机制。
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