Abstract

Gastric aspiration is a major risk factor for the development of ARDS, and also places the patient in jeopardy of secondary bacterial pneumonia. The major objective is to examine cellular mechanisms that increase the risks of these diseases. Although aspiration-induced host changes are poorly understood, this laboratory has demonstrated a likely role for TNF-alpha, IL-1-beta, MIP-2, MCP-1, and toxic inflammatory chemical mediators including proteinases, oxidants, and nitric oxide (NO) in the pathogenesis of the secondary lung injuries. The applicants hypothesize that increased susceptibility results from acid-induced, cytokine-mediated """"""""priming"""""""" of leukocytes. They have demonstrated that """"""""priming"""""""" enhances release of oxidants, NO, and proteinases following an additional sustained insult. They predict that oxidants and NO can subsequently augment cytokine progression and accelerate the shift to monocytic recruitment, thereby increasing lung injury and mortality.
Aims #1 and #2 will focus on mechanism(s) involved in """"""""priming"""""""" and Aim #3 will evaluate the effects of """"""""priming"""""""" on susceptibility of the host to bacterial infection.
Aim #1 will assess: a) recruitment and turnover of the MO population following acid (ACID), small non-acidified particle (SNAP), or combined acid small particulate (CASP) aspiration and b) in vivo TNFalpha and/or IL-1beta, or MCP-1 neutralization on the ability to reverse alterations in ex vivo MO expression of cytokines, iNOS, and MO toxic products. The investigators predict that CASP aspiration will augment the progression of the cytokine response to a more rapid expression of MCP-1 and MO influx with enhanced effector activity.
Aim #2 will examine the role of superoxide, H2O2 and/or NO to the CASP-induced synergistic lung injury and increased mortality by examining the proinflammatory cytokine cascade and leukocyte influx following: a) selective inhibition of superoxide, H2O2, or NO generation, before or following CASP aspiration, or b) hyperoxia-induced generation of oxidants and/or NO following ACID aspiration. They postulate that increased H2O2 and NO generation will augment the progression of proinflammatory cytokines and accelerate the appearance of MCP-1-mediated monocyte recruitment. Finally, in Aim #3 they will examine cytokine expression, lung inflammatory cell influx, bacterial clearance, lung injury, and mortality following gastric aspiration. The investigators anticipate that aspiration will increase the lung injury to bacterial challenge by initially enhancing the inflammatory injury, but eventually impairing TNFalpha, IL-1beta, and/or MIP-2 production, thereby decreasing bacterial clearance. These studies may uncover mechanisms on which to base therapeutic strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL048889-05
Application #
6389235
Study Section
Special Emphasis Panel (ZRG1-SSS-W (25))
Program Officer
Harabin, Andrea L
Project Start
1996-07-01
Project End
2004-07-31
Budget Start
2001-08-01
Budget End
2002-07-31
Support Year
5
Fiscal Year
2001
Total Cost
$309,257
Indirect Cost

  Institution

Name
State University of New York at Buffalo
Department
Anesthesiology
Type
Schools of Medicine
DUNS #
038633251
City
Buffalo
State
NY
Country
United States
Zip Code
14260

  Publications

Sayej, Wael N; Knight Iii, Paul R; Guo, Weidun Alan et al. (2016) Advanced Glycation End Products Induce Obesity and Hepatosteatosis in CD-1 Wild-Type Mice. Biomed Res Int 2016:7867852
MacDonald, Brian A; Chakravarthy, Krishnan V; Davidson, Bruce A et al. (2015) Halothane modulates the type i interferon response to influenza and minimizes the risk of secondary bacterial pneumonia through maintenance of neutrophil recruitment in an animal model. Anesthesiology 123:590-602
Gerard, Elizabeth; Spengler, Robert N; Bonoiu, Adela C et al. (2015) Chronic constriction injury-induced nociception is relieved by nanomedicine-mediated decrease of rat hippocampal tumor necrosis factor. Pain 156:1320-33
Smit, Peter J; Guo, Weidun A; Davidson, Bruce A et al. (2014) Dietary advanced glycation end-products, its pulmonary receptor, and high mobility group box 1 in aspiration lung injury. J Surg Res 191:214-23
Marks, Laura R; Davidson, Bruce A; Knight, Paul R et al. (2013) Interkingdom signaling induces Streptococcus pneumoniae biofilm dispersion and transition from asymptomatic colonization to disease. MBio 4:
Grimm, Melissa J; Vethanayagam, R Robert; Almyroudis, Nikolaos G et al. (2013) Monocyte- and macrophage-targeted NADPH oxidase mediates antifungal host defense and regulation of acute inflammation in mice. J Immunol 190:4175-84
Davidson, Bruce A; Vethanayagam, R Robert; Grimm, Melissa J et al. (2013) NADPH oxidase and Nrf2 regulate gastric aspiration-induced inflammation and acute lung injury. J Immunol 190:1714-24
Fernandez, Stanley F; Fung, Christopher; Helinski, Jadwiga D et al. (2013) Low pH environmental stress inhibits LPS and LTA-stimulated proinflammatory cytokine production in rat alveolar macrophages. Biomed Res Int 2013:742184
Lakshminrusimha, Satyan; Suresh, Madathilparambil V; Knight, Paul R et al. (2013) Role of pulmonary artery reactivity and nitric oxide in injury and inflammation following lung contusion. Shock 39:278-85
Davidson, Bruce A; Alluri, Ravi (2013) Gastric Aspiration Models. Bio Protoc 3:

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