Abstract

Research Project 3. Vesicant-induced Lung Injury Key Personnel: Debra L. Laskin, Ph.D., Distinguished Professor, Rutgers University School of Pharmacy Jeffrey D. Laskin, Ph.D., Professor, Rutgers University School of Public Health Project Summary/Abstract Sulfur mustard (SM) and nitrogen mustard are high priority chemical threats that cause debilitating damage to the respiratory system resulting in both acute and chronic effects. As this is the major cause of morbidity and mortality in exposed victims, it is essential to identify effective strategies to mitigate pulmonary toxicity caused by these vesicants. Our studies are focused on macrophages and inflammatory mediators as key to both acute lung injury and fibrosis induced by vesicants. We discovered that following mustard exposure, distinct subset of macrophages with proinflammatory/ cytotoxic activity (M1) and profibrotic (M2) activity sequentially appear in the lung. Our objective is to elucidate the contribution of these macrophage subsets to mustard-induced lung injury and fibrosis, with the overall goal of identifying new targets for therapeutic intervention. This mechanistic research is essential as macrophages are known to release numerous cytotoxic and profibrotic mediators; thus, targeting only one product or macrophage subset is unlikely to be effective in completely mitigating vesicant-induced lung injury. We hypothesize that M1 macrophages contribute to injury by generating cytotoxic oxidants and TNF?, which cause lung damage and promote lipid oxidation; oxidized lipids and TNF? upregulate macrophage scavenger receptors stimulating lipid uptake and the development of M2 macrophage foam cells, which play a key role in fibrogenesis. To test this hypothesis plans are to (1) elucidate the origin of M1 and M2 inflammatory macrophages responding to vesicant-induced lung injury and mechanisms mediating their accumulation in the lung; (2) Evaluate the role of oxidized lipids and M1 and M2 macrophages in foam cell formation and vesicant- induced fibrosis, and (3) Assess the contribution of TNF? to vesicant-induced acute lung injury and lung fibrosis. An innovative combination of strategies will be used for our studies including lineage tracking, the generation of chimeric mice, adoptive transfer and monocyte/ macrophage depletion. We will also work closely with the Center's Pharmaceutics and Medicinal Chemistry Support Core to refine a microparticle lung drug delivery system designed to specifically target profibotic M2 macrophages and with the Pharmacology and Drug Development Support Core to move one of our lead countermeasures for vesicant-induced lung injury into advanced drug development. Successful completion of our proposed studies will result in a more precise understanding of the specific roles of macrophages in vesicant-induced toxicity, their origin, and mechanisms mediating their accumulation in the lung. This will have significant implications for the development of more efficacious strategies for mitigating mustard-induced lung injury and fibrosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Specialized Center--Cooperative Agreements (U54)
Project #
5U54AR055073-15
Application #
9982785
Study Section
Special Emphasis Panel (ZRG1)
Project Start
Project End
Budget Start
2020-07-01
Budget End
2021-06-30
Support Year
15
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Rbhs-School of Public Health
Department
Type
DUNS #
078795880
City
Piscataway
State
NJ
Country
United States
Zip Code
08854

  Publications

Moretti, Alysha; Li, Qi; Chmielowski, Rebecca et al. (2018) Nanotherapeutics Containing Lithocholic Acid-Based Amphiphilic Scorpion-Like Macromolecules Reduce In Vitro Inflammation in Macrophages: Implications for Atherosclerosis. Nanomaterials (Basel) 8:
Szilagyi, John T; Fussell, Karma C; Wang, Yun et al. (2018) Quinone and nitrofurantoin redox cycling by recombinant cytochrome b5 reductase. Toxicol Appl Pharmacol 359:102-107
Joseph, Laurie B; Composto, Gabriella M; Perez, Roberto M et al. (2018) Sulfur mustard induced mast cell degranulation in mouse skin is inhibited by a novel anti-inflammatory and anticholinergic bifunctional prodrug. Toxicol Lett 293:77-81
Chang, Yoke-Chen; Gordon, Marion K; Gerecke, Donald R (2018) Expression of Laminin 332 in Vesicant Skin Injury and Wound Repair. Clin Dermatol (Wilmington) 2:
Sunil, Vasanthi R; Vayas, Kinal N; Fang, Mingzhu et al. (2017) World Trade Center (WTC) dust exposure in mice is associated with inflammation, oxidative stress and epigenetic changes in the lung. Exp Mol Pathol 102:50-58
Yang, Shaojun; Jan, Yi-Hua; Mishin, Vladimir et al. (2017) Diacetyl/l-Xylulose Reductase Mediates Chemical Redox Cycling in Lung Epithelial Cells. Chem Res Toxicol 30:1406-1418
Venosa, Alessandro; Gow, James G; Hall, LeRoy et al. (2017) Regulation of Nitrogen Mustard-Induced Lung Macrophage Activation by Valproic Acid, a Histone Deacetylase Inhibitor. Toxicol Sci 157:222-234
Francis, Mary; Sun, Richard; Cervelli, Jessica A et al. (2017) Editor's Highlight: Role of Spleen-Derived Macrophages in Ozone-Induced Lung Inflammation and Injury. Toxicol Sci 155:182-195
Chmielowski, Rebecca A; Abdelhamid, Dalia S; Faig, Jonathan J et al. (2017) Athero-inflammatory nanotherapeutics: Ferulic acid-based poly(anhydride-ester) nanoparticles attenuate foam cell formation by regulating macrophage lipogenesis and reactive oxygen species generation. Acta Biomater 57:85-94
Francis, Mary; Groves, Angela M; Sun, Richard et al. (2017) Editor's Highlight: CCR2 Regulates Inflammatory Cell Accumulation in the Lung and Tissue Injury following Ozone Exposure. Toxicol Sci 155:474-484

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