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臭氧与内毒素共同暴露对大鼠气道上皮的影响:增强毒物诱导的改变。

Effects of ozone and endotoxin coexposure on rat airway epithelium: potentiation of toxicant-induced alterations.

作者信息

Wagner J G, Hotchkiss J A, Harkema J R

机构信息

Department of Pathology and Diagnostic Investigation, College of Veterinary Medicine, Michigan State University, East Lansing, Michigan 48824, USA.

出版信息

Environ Health Perspect. 2001 Aug;109 Suppl 4(Suppl 4):591-8. doi: 10.1289/ehp.01109s4591.

Abstract

Tropospheric ozone is the major oxidizing component in photochemical smog and is one of the most pervasive problems to human health of the criteria air pollutants for which the National Ambient Air Quality Standards have been designated by the Clean Air Act. Although many adverse health effects of ozone exposure have been documented in both humans and laboratory animals, controversy surrounds the establishment and implementation of ozone standards set forth by the U.S. Environmental Protection Agency. Because people are commonly exposed to more than one air pollutant at a time, studies that examine coexposures to airborne materials may be more relevant for assessing their risks to human health. Airborne biogenic substances such as pollens, spores, and bacterial products are ubiquitous in the environment, and when inhaled can cause adverse respiratory symptoms. One such biogenic agent, bacterial endotoxin, is a potent stimulus of airway inflammation and is a ubiquitous airborne contaminant commonly found in domestic, agricultural, and industrial settings. Little is known about the interaction of exposures to biogenic substances and criteria air pollutants such as ozone. In the last few years we have performed a series of studies in rodents that examined the biologic responses of the respiratory epithelium after airway exposures to both endotoxin and ozone. When exposed to ozone (0.5 ppm 8 hr/day for 3 days), Fischer rats develop lesions in the nasal transitional epithelium, whereas intranasal instillation of endotoxin (20 microg) elicits epithelial lesions in the respiratory epithelium of the nose and conducting airways. Our studies were designed to examine how exposure to one toxicant may affect the airway epithelial lesions induced by the other toxicant. We investigated the potential role of acute inflammation in the enhancement of airway epithelial lesions after exposure of these two toxicants in neutrophil-sufficient and neutrophil-deficient rodents. A summary of these results indicates that epithelial and inflammatory responses to coexposure of these two pollutants are greater than those elicited by either agent alone. Interestingly, each toxicant enhances the epithelial alterations induced by the other. Furthermore, the synergistic effects elicited by coexposure to ozone and endotoxin are mediated partly by neutrophils. These studies provided some new insights into how inhaled co-pollutants interact to initiate and promote alterations of airway epithelium. Further studies with these and other air pollutants will help define their true risk to human health.

摘要

对流层臭氧是光化学烟雾中的主要氧化成分,也是《清洁空气法》规定了国家环境空气质量标准的标准空气污染物中,对人类健康影响最为普遍的问题之一。尽管在人类和实验动物中都记录了许多臭氧暴露对健康的不利影响,但美国环境保护局制定和实施的臭氧标准仍存在争议。由于人们通常同时接触多种空气污染物,因此研究空气传播物质的共同暴露情况,可能对评估其对人类健康的风险更为相关。空气中的生物源物质,如花粉、孢子和细菌产物,在环境中普遍存在,吸入后可引起不良呼吸道症状。一种这样的生物源物质,细菌内毒素,是气道炎症的有力刺激物,是一种普遍存在的空气传播污染物,常见于家庭、农业和工业环境中。关于生物源物质暴露与臭氧等标准空气污染物之间的相互作用,人们了解甚少。在过去几年中,我们在啮齿动物身上进行了一系列研究,考察了气道暴露于内毒素和臭氧后,呼吸道上皮的生物学反应。当暴露于臭氧(0.5 ppm,每天8小时,持续3天)时,Fischer大鼠鼻过渡上皮会出现病变,而经鼻滴注内毒素(20微克)会引发鼻和传导气道呼吸上皮的上皮病变。我们的研究旨在考察暴露于一种毒物如何影响另一种毒物诱导的气道上皮病变。我们研究了急性炎症在中性粒细胞充足和中性粒细胞缺乏的啮齿动物暴露于这两种毒物后,增强气道上皮病变中的潜在作用。这些结果的总结表明,这两种污染物共同暴露引起的上皮和炎症反应,大于单独由任何一种物质引起的反应。有趣的是,每种毒物都会增强另一种毒物诱导的上皮改变。此外,臭氧和内毒素共同暴露引起的协同效应部分由中性粒细胞介导。这些研究为吸入性混合污染物如何相互作用引发和促进气道上皮改变提供了一些新见解。对这些以及其他空气污染物的进一步研究将有助于确定它们对人类健康的真正风险。

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本文引用的文献

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ENDOTOXIN ACTIVITY OF A HOUSE DUST EXTRACT.室内灰尘提取物的内毒素活性
J Allergy. 1964 Mar-Apr;35:134-42. doi: 10.1016/0021-8707(64)90027-9.
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Ozone: a trigger for hospital pediatric asthma emergency room visits.臭氧:引发医院儿科哮喘急诊室就诊的因素。
Pediatr Pulmonol. 2000 Jul;30(1):41-6. doi: 10.1002/1099-0496(200007)30:1<41::aid-ppul7>3.0.co;2-4.
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Epithelial damage and response.上皮损伤与反应。
Clin Exp Allergy. 2000 Jun;30 Suppl 1:37-41. doi: 10.1046/j.1365-2222.2000.00095.x.
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Trophic slime, allergic slime.营养黏液,过敏黏液。
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