Kilgour Joanne D, Rattray Nicola J, Foster John, Soames Anthony, Hext Paul M
Syngenta CTL, Alderley Park, Macclesfield, Cheshire SK10 4TJ, UK.
J Appl Toxicol. 2002 Nov-Dec;22(6):371-85. doi: 10.1002/jat.872.
Acute and repeated inhalation exposures (for 28 days) to polymeric methylene diphenyl diisocyanate (PMDI) were performed in rats. Investigations were made at the end of exposures and after 3, 10 and 30 days of recovery following single acute exposures and after 30 days of recovery following 28 days of exposure. Acute exposures to 10, 30 or 100 mg m(-3) PMDI produced clinical signs in all animals that were consistent with exposure to irritant aerosols. An exposure concentration-related body weight loss and increase in lung weight were seen post-exposure, with complete recovery by day 8. The time course of changes in the lung over the initial days following exposure consisted of a pattern of initial toxicity, rapid and heavy influx of inflammatory cells and soluble markers of inflammation and cell damage, increased lung surfactant, a subsequent recovery and epithelial proliferative phase and, finally, a return to the normal status quo of the lung. During these stages there was evidence for perturbation of lung surfactant homeostasis, demonstrated by increased amounts of crystalline surfactant and increased number and size of lamellar bodies within type II alveolar cells. Repeated exposure over 28 days to the less toxic concentrations of 1, 4 or 10 mg m(-3) PMDI produced no clinical signs or body weight changes, but an increase in lung weight was seen in animals exposed to 10 mg m(-3), which resolved following the 30-day recovery period. Other effects seen were again consistent with exposure to irritant aerosols, but were less severe than those seen in the acute study. Analysis of bronchoalveolar lavage fluid revealed similar changes to those seen in the acute study. At both 10 and 4 mg m(-3) PMDI increased numbers of 'foamy' macrophages in lung lavage cell pellet correlated with the increased phospholipid content of the pellet. Changes in lung lavage parameters and electron microscopic evidence again suggested perturbations in surfactant homeostasis. Histologically, bronchiolitis and thickening of the central acinar regions was seen at 10 and 4 mg m(-3), reflecting changes in cell proliferation in the terminal bronchioles and centro-acinar regions. Almost all effects seen had recovered by day 30 post-exposure. Both acute and subacute studies demonstrate rapid recovery of effects in the lung following exposure to PMDI, with no progression of these effects even at concentrations higher than those shown to produce tumours in a chronic study. These findings add weight to the hypothesis that pulmonary tumours seen following chronic exposure to PMDI are most likely due to a combination of the chronic irritant effects of repeated exposure, coupled with the presence of insoluble polyureas formed by polymerization of PMDI (found in studies reported here and previous chronic studies), and therefore acute or short-term exposures to PMDI are likely to be of little concern for long-term pulmonary health.
在大鼠中进行了急性和反复吸入(持续28天)聚合亚甲基二苯基二异氰酸酯(PMDI)的实验。在单次急性暴露后的暴露结束时、恢复3天、10天和30天后以及在28天暴露后的30天恢复期后进行了研究。急性暴露于10、30或100 mg m(-3)的PMDI会使所有动物出现与刺激性气溶胶暴露一致的临床症状。暴露后出现了与暴露浓度相关的体重减轻和肺重量增加,到第8天完全恢复。暴露后最初几天肺内变化的时间进程包括初始毒性模式、炎症细胞和炎症及细胞损伤可溶性标志物的快速大量涌入、肺表面活性物质增加、随后的恢复和上皮增殖期,最后恢复到肺的正常状态。在这些阶段,有证据表明肺表面活性物质稳态受到干扰,表现为结晶表面活性物质数量增加以及II型肺泡细胞内板层小体数量和大小增加。反复暴露28天于毒性较低的浓度1、4或10 mg m(-3)的PMDI未产生临床症状或体重变化,但暴露于10 mg m(-3)的动物出现了肺重量增加,在30天的恢复期后恢复。观察到的其他影响同样与刺激性气溶胶暴露一致,但比急性研究中观察到的影响轻。支气管肺泡灌洗流体分析显示与急性研究中观察到的变化相似。在10和4 mg m(-3)的PMDI浓度下,肺灌洗细胞沉淀中“泡沫状”巨噬细胞数量增加与沉淀中磷脂含量增加相关。肺灌洗参数的变化和电子显微镜证据再次表明表面活性物质稳态受到干扰。组织学上,在10和4 mg m(-3)的浓度下观察到细支气管炎和中央腺泡区域增厚,反映了终末细支气管和中央腺泡区域细胞增殖的变化。几乎所有观察到的影响在暴露后30天已恢复。急性和亚急性研究均表明,暴露于PMDI后肺内的影响能快速恢复,即使在高于慢性研究中显示会产生肿瘤的浓度下,这些影响也不会进展。这些发现进一步支持了以下假设:长期暴露于PMDI后出现的肺部肿瘤很可能是反复暴露的慢性刺激作用与PMDI聚合形成的不溶性聚脲(在此处报告的研究和先前的慢性研究中均有发现)共同作用的结果,因此急性或短期暴露于PMDI可能对长期肺部健康影响不大。
