Abstract

Diffuse alveolar damage (DAD) of ARDS is a stereotypic response to a variety of etiologies. At post-mortem, DAD represents a continuum of overlapping phases of injury that may lead to formation of intra-alveolar granulation tissue/fibrosis. These findings are also present in ARDS patients that survive after prolonged mechanical ventilation and exposure to high FIO/2; as a significant proportion of these patients have compromised pulmonary function at one year. Angiogenesis represents a mechanism that supports intra-alveolar mesenchymal cellular proliferation and deposition of extracellular matrix in DAD. However, the specific angiogenic factors that promote angiogenesis during DAD remain to be fully elucidated. The CXC chemokines are unique are unique cytokines that can behave as either potent promoters (angiogenic factors) or inhibitors (angiostatic factors) of angiogenesis. We hypothesize that the pathogenesis of intra-alveolar angiogenesis/fibrosis associated with DAD is due to an imbalance of over-expression of angiogenic, as compared to angiostatic members of the CXC chemokine family. This paradigm of biological imbalance will favor net angiogenesis leading to intra-alveolar fibrosis and impaired lung function of ARDS patients. In the proposal, we will test this postulate by addressing the following questions: 1) Do specific cytokine networks and exposure to hyperoxia (oxidant stress) result in a preponderance of angiogenic CXC chemokines that leads to augmented intra-alveolar angiogenesis/fibrosis? 2) What is the molecular mechanism(s) for hyperoxia-induced over-expression of angiogenic CXC chemokines from human lung microvascular endothelial cells, and can gene transfer of an angiostatic CXC chemokines from human lung microvascular endothelial cells, and can gene transfer of an angiostatic CXC chemokine gene shift this imbalance and reduce the angiogenic potential of these cells? 3) Can gene transfer of an angiostatic CXC chemokine gene in vivo lead to attenuation of angiogenesis and fibrosis and an animal model of DAD? 4) Does an imbalance of over-expression of angiogenic, as compared to angiostatic CXC chemokines correlate with clinical evidence of angiogenesis/fibrosis and long-term impairment of pulmonary function in ARDS patients? Techniques employed in this application will include: a variety of molecular, immunological, cellular, bioassay, and animal models of DAD. The elucidation of the pathobiology of the imbalance of angiogenic, as compared to angiostatic CXC chemokines will permit the development of novel and targeted therapy aimed specifically at attenuation intra-alveolar angiogenesis/fibrosis, leading to improved preservation of lung function in ARDS.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Specialized Center (P50)
Project #
5P50HL060289-04
Application #
6565083
Study Section
Project Start
2001-12-01
Project End
2002-11-30
Budget Start
Budget End
Support Year
4
Fiscal Year
2002
Total Cost
$282,412
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Bosmann, Markus; Grailer, Jamison J; Ruemmler, Robert et al. (2013) Extracellular histones are essential effectors of C5aR- and C5L2-mediated tissue damage and inflammation in acute lung injury. FASEB J 27:5010-21
Moss, Marc; Standiford, Theodore J (2011) Leptin in fibroproliferative acute respiratory distress syndrome: not just a satiety factor. Am J Respir Crit Care Med 183:1443-4
Smith, Monica R; Gangireddy, Srinivasa R; Narala, Venkata R et al. (2010) Curcumin inhibits fibrosis-related effects in IPF fibroblasts and in mice following bleomycin-induced lung injury. Am J Physiol Lung Cell Mol Physiol 298:L616-25
Keshamouni, Venkateshwar G; Jagtap, Pratik; Michailidis, George et al. (2009) Temporal quantitative proteomics by iTRAQ 2D-LC-MS/MS and corresponding mRNA expression analysis identify post-transcriptional modulation of actin-cytoskeleton regulators during TGF-beta-Induced epithelial-mesenchymal transition. J Proteome Res 8:35-47
Reddy, Raju C; Srirangam, Anjaiah; Reddy, Kaunteya et al. (2008) Chemotherapeutic drugs induce PPAR-gamma expression and show sequence-specific synergy with PPAR-gamma ligands in inhibition of non-small cell lung cancer. Neoplasia 10:597-603
Reddy, Raju C; Narala, Venkata R; Keshamouni, Venkateshwar G et al. (2008) Sepsis-induced inhibition of neutrophil chemotaxis is mediated by activation of peroxisome proliferator-activated receptor-{gamma}. Blood 112:4250-8
Milam, Jami E; Keshamouni, Venkateshwar G; Phan, Sem H et al. (2008) PPAR-gamma agonists inhibit profibrotic phenotypes in human lung fibroblasts and bleomycin-induced pulmonary fibrosis. Am J Physiol Lung Cell Mol Physiol 294:L891-901
Gomperts, Brigitte N; Belperio, John A; Fishbein, Michael C et al. (2007) Keratinocyte growth factor improves repair in the injured tracheal epithelium. Am J Respir Cell Mol Biol 37:48-56
Keshamouni, Venkateshwar G; Michailidis, George; Grasso, Catherine S et al. (2006) Differential protein expression profiling by iTRAQ-2DLC-MS/MS of lung cancer cells undergoing epithelial-mesenchymal transition reveals a migratory/invasive phenotype. J Proteome Res 5:1143-54
Gomperts, Brigitte N; Belperio, John A; Rao, P Nagesh et al. (2006) Circulating progenitor epithelial cells traffic via CXCR4/CXCL12 in response to airway injury. J Immunol 176:1916-27

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