Abstract

The Problem: Particulates within air pollution are associated with significant morbidity and mortality at commonly encountered ambient concentrations. The biologic basis for their health effects is unknown, but the same epidemiologic studies which reveal particle effects also offer an important clue. Harmful health effects occur most notably among individuals with pre-existing respiratory disease, e.g. chronic bronchitis and asthma, indicating a heightened sensitivity to particle effects within inflammed lungs. Experimentally, we have found that inhalation exposure of animals to """"""""real-world"""""""" concentrated ambient particulates (CAPs) prepared via a novel technology causes toxic effects--but only in animals with pre-existing pulmonary inflammation (asthma, SO2, bronchitis), and not in healthy controls. Hypothesis: The central thesis of this proposal is that pre-existing pulmonary disease alters or """"""""primes"""""""" the lung's response to inhaled ambient particles, resulting in increased inflammation and health effects. We further postulate that oxidative stress mediated by particulate components is a central mechanism for increased production of inflammatory mediators by """"""""primed"""""""" lung cells. Experimental Plan:
In specific Aim #1 we will measure in vitro the production of reactive oxygen species, nitric oxide and cyrokines in response to uptake of CAPs by lung marcophages or epithelial cells with or without """"""""priming"""""""" by inflammatory mediators (LPS, TNF). We will test our hypothesis regarding oxidant mechanisms of CAPs effects by: 1) measuring oxidant stress in primed and normal lung cells after uptake of CAPs (oxidation of intracellular reporter DCFH; lipid peroxidation); 2) analyzing oxidant components (e.g. SiO2, Fe) in samples of CAPs that vary in inflammatory effects; 3) testing the ability of antioxidants to block cellular responses.
In specific Aim #2 we will characterize in vivo the effects of inhaled concentrated ambient particulates (CAPs) on pre-existing inflammatory lung disease using a mouse asthma model. We will test our hypotheses by inhalation exposure of normal and """"""""asthmatic"""""""" mice to CAPs, measuring both lung lavage markers of cellular inflammation (total cells, number of eosinophils, cytokine levels) and physiologic tests of airway bronchoconstriction. To complete our study of mechanisms in vivo, we will also measure the effects of antioxidant intervention, both pharmacologic and through use of genetically altered mice. Significance: The proposed studies will determine mechanisms for the effect of air pollution particulates. Such informaiton is critical to public health management of this problem.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Program Projects (P01)
Project #
5P01ES008129-04
Application #
6336516
Study Section
Project Start
2000-06-01
Project End
2001-05-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
4
Fiscal Year
2000
Total Cost
$316,040
Indirect Cost

  Institution

Name
Harvard University
Department
Type
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Wu, Muzo; Gibbons, John G; DeLoid, Glen M et al. (2017) Immunomodulators targeting MARCO expression improve resistance to postinfluenza bacterial pneumonia. Am J Physiol Lung Cell Mol Physiol 313:L138-L153
Bartoli, Carlo R; Nadar, Menaka M; Godleski, John J (2010) Capsule thickness correlates with vascular density and blood flow within foreign-body capsules surrounding surgically implanted subcutaneous devices. Artif Organs 34:857-61
Rhoden, Claudia Ramos; Lawrence, Joy; Godleski, John J et al. (2004) N-acetylcysteine prevents lung inflammation after short-term inhalation exposure to concentrated ambient particles. Toxicol Sci 79:296-303
Pope 3rd, C Arden; Burnett, Richard T; Thurston, George D et al. (2004) Cardiovascular mortality and long-term exposure to particulate air pollution: epidemiological evidence of general pathophysiological pathways of disease. Circulation 109:71-7
Ning, Yaoyu; Tao, Florence; Qin, Guozhong et al. (2004) Particle-epithelial interaction: effect of priming and bystander neutrophils on interleukin-8 release. Am J Respir Cell Mol Biol 30:744-50
Wellenius, Gregory A; Coull, Brent A; Godleski, John J et al. (2003) Inhalation of concentrated ambient air particles exacerbates myocardial ischemia in conscious dogs. Environ Health Perspect 111:402-8
Savage, Sara T; Lawrence, Joy; Katz, Tracy et al. (2003) Does the Harvard/U.S. Environmental Protection Agency Ambient Particle Concentrator change the toxic potential of particles? J Air Waste Manag Assoc 53:1088-97
Saldiva, Paulo H N; Clarke, Robert W; Coull, Brent A et al. (2002) Lung inflammation induced by concentrated ambient air particles is related to particle composition. Am J Respir Crit Care Med 165:1610-7
Batalha, Joao R F; Saldiva, Paulo H N; Clarke, Robert W et al. (2002) Concentrated ambient air particles induce vasoconstriction of small pulmonary arteries in rats. Environ Health Perspect 110:1191-7
Tao, Florence; Kobzik, Lester (2002) Lung macrophage-epithelial cell interactions amplify particle-mediated cytokine release. Am J Respir Cell Mol Biol 26:499-505

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