Abstract

The long-term goal of this application is to elucidate the role of oxidative stress in the biological effects of DEPs in the respiratory tract. We hypothesize that generation of oxidative stress by organic chemicals in DEPs (DEP xenobiotics) initiates a stratified pulmonary response that commences with the: 1) activation of the ARE pathway, which transitions to 2) excitation of inflammation and 3) cell injury in the lung, with all three responses being critical to enhancement of asthma. To elucidate how DEP chemicals interact with oxidative stress pathways in the lung, we will employ a very sensitive system for analyzing oxidative stress by oxidative xenobiotics, including those in DEP. This pathway, which utilizes the transcription factor Nrf2, induces the expression of the oxidative stress enzyme, HO-1 via AREs. HO-1, in turn, has potent antioxidant, anti-inflammatory and anti-apoptotic effects in the lung.
In Specific Aim 1, we will test the hypothesis that the effect of DEP on HO-1 expression in vitro is mediated by redox cycling DEP chemicals that operate via Nrf2 and AREs in the promoter of that gene. We will test the effect of HO-1 for its ability to protect epithelial cells and macrophages against the oxidative stress effects of DEP, using drugs that modulate HO-1 expression or HO-1 activity.
In Specific Aim 2 we will test the hypothesis that the pro-inflammatory and pro-allergic effects of DEP in the murine lung are related to oxidative stress and can be modified by modulating HO-1 expression through genetic or pharmacological means. This will be accomplished by testing intratracheal DEP instillation on HO-1 expression, along with other markers for oxidative stress, inflammation and apoptosis. We will also determine whether pharmacological modification of HO-1 activity and transgenic HO-1 overexpression influence the adjuvant effects of DEP in the murine asthma model. We will use the same model, in collaboration with Project 4, to determine the effects of Nrf2 knockout on the pro-oxidative and allergic/inflammatory effects of DEP.
In Specific Aim 3, we will test the hypothesis that interference in HO-1 expression by a known poly-(GT) polymorphism in the human HO-1 gene enhances the pro-allergic effects of DEP in humans. This will be accomplished in collaboration with Projects 1 and 3, and will involve genotyping and intranasal DEP challenge followed nasal lavage and studying the parameters for oxidative stress and allergic inflammation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI050495-02
Application #
6663327
Study Section
Special Emphasis Panel (ZAI1)
Project Start
2002-09-01
Project End
2003-06-30
Budget Start
Budget End
Support Year
2
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
DUNS #
119132785
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Riedl, Marc A; Saxon, Andrew; Diaz-Sanchez, David (2009) Oral sulforaphane increases Phase II antioxidant enzymes in the human upper airway. Clin Immunol 130:244-51
Schroder, Nicolas W J; Crother, Timothy R; Naiki, Yoshikazu et al. (2008) Innate immune responses during respiratory tract infection with a bacterial pathogen induce allergic airway sensitization. J Allergy Clin Immunol 122:595-602.e5
Xia, Tian; Kovochich, Michael; Nel, Andre E (2007) Impairment of mitochondrial function by particulate matter (PM) and their toxic components: implications for PM-induced cardiovascular and lung disease. Front Biosci 12:1238-46
Gilliland, Frank D; Li, Yu-Fen; Gong Jr, Henry et al. (2006) Glutathione s-transferases M1 and P1 prevent aggravation of allergic responses by secondhand smoke. Am J Respir Crit Care Med 174:1335-41
Nel, Andre; Xia, Tian; Madler, Lutz et al. (2006) Toxic potential of materials at the nanolevel. Science 311:622-7
Wan, Junxiang; Diaz-Sanchez, David (2006) Phase II enzymes induction blocks the enhanced IgE production in B cells by diesel exhaust particles. J Immunol 177:3477-83
Riedl, Marc A; Landaw, Elliot M; Saxon, Andrew et al. (2005) Initial high-dose nasal allergen exposure prevents allergic sensitization to a neoantigen. J Immunol 174:7440-5
Xiao, Gary Guishan; Nel, Andre E; Loo, Joseph A (2005) Nitrotyrosine-modified proteins and oxidative stress induced by diesel exhaust particles. Electrophoresis 26:280-92
Xia, Tian; Korge, Paavo; Weiss, James N et al. (2004) Quinones and aromatic chemical compounds in particulate matter induce mitochondrial dysfunction: implications for ultrafine particle toxicity. Environ Health Perspect 112:1347-58
Finkelman, Fred D; Yang, Mingyan; Orekhova, Tatyana et al. (2004) Diesel exhaust particles suppress in vivo IFN-gamma production by inhibiting cytokine effects on NK and NKT cells. J Immunol 172:3808-13

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