Abstract

Respiratory failure remains a major cause of mortality in the trauma patient. The combination of an episode of shock and tissue damage followed by sepsis, frequently results in a severe form of acute lung injury; the injury from both sepsis and trauma appearing to be greater in both frequency and in severity from that due to sepsis alone. The major characteristics of this lung injury in man and animals remains that of pulmonary artery hypertension and increased protein permeability leading to pulmonary edema. We have recently demonstrated that increased transvascular fluid flux seen after hemorrhagic shock alone is basically that produced by the shock and resuscitation induced hypoproteinemia. We now want to define the mechanism of injury of the other components, namely sepsis and the effect of soft tissue damage on the sepsis injury. Recent findings indicate that three factors are involved: (1) the cyclooxygenase products of arachidonic acid with the role of the lipoxygenase products still undetermined, (2) products released from sequestered neutrophils, specifically oxygen radicals, and (3) platelets possibly via serotonin release. We plan to implement physiological, immunological and biochemical methods already being used by the four established investigators to define this relationship. The animal model will continue to be the unanesthetized sheep with lung and soft tissue lymph fistulae using lymph flow and protein content to reflect QF and protein permeability and the content of mediators in lymph to reflect that released by or into the lung or from a focus of tissue damage. The septic episode will initially be endotoxin while a bacterial sepsis model is being developed. Tissue trauma will be produced by a full thickness burn (anesthetic to the animal). Neutrophil chemotactic factors, complement being one, and factors activating neutrophils to release O2 radicals, will be characterized as will the role of the pulmonary macrophage in initiating the process. Cyclooxygenase products will continue to be monitored as well as lipoxygenase products (initially by selective inhibition until an assay is available). The relationship of serotonin to the above will be determined. The role of oxygen radicals will be studied by monitoring the degree of lipid peroxidation present in lung tissue and its correlation with physiologic injury. Treatment modalities can be pursued once the mechanism of injury is better defined.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL030068-03
Application #
3341131
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1982-07-01
Project End
1986-11-30
Budget Start
1984-12-01
Budget End
1985-11-30
Support Year
3
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Beth Israel Deaconess Medical Center
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code

  Publications

Chan, E D; Riches, D W; White, C W (2001) Redox paradox: effect of N-acetylcysteine and serum on oxidation reduction-sensitive mitogen-activated protein kinase signaling pathways. Am J Respir Cell Mol Biol 24:627-32
Hokanson, J E; Krauss, R M; Albers, J J et al. (1995) LDL physical and chemical properties in familial combined hyperlipidemia. Arterioscler Thromb Vasc Biol 15:452-9
Demling, R H; LaLonde, C; Goad, M E (1989) Effect of ibuprofen on the pulmonary and systemic response to repeated doses of endotoxin. Surgery 105:421-9
Demling, R; LaLonde, C (1989) Relationship between lung injury and lung lipid peroxidation caused by recurrent endotoxemia. Am Rev Respir Dis 139:1118-24
Nishide, T; Tollefson, J H; Albers, J J (1989) Inhibition of lipid transfer by a unique high density lipoprotein subclass containing an inhibitor protein. J Lipid Res 30:149-58
Tollefson, J H; Ravnik, S; Albers, J J (1988) Isolation and characterization of a phospholipid transfer protein (LTP-II) from human plasma. J Lipid Res 29:1593-602
Seekamp, A; Lalonde, C; Zhu, D G et al. (1988) Catalase prevents prostanoid release and lung lipid peroxidation after endotoxemia in sheep. J Appl Physiol 65:1210-6
Lalonde, C; Demling, R H; Goad, M E (1988) Tissue inflammation without bacteria produces increased oxygen consumption and distant organ lipid peroxidation. Surgery 104:49-56
Demling, R H; Katz, A; Lalonde, C et al. (1987) The immediate effect of burn wound excision on pulmonary function in sheep: the role of prostanoids, oxygen radicals, and chemoattractants. Surgery 101:44-55
Demling, R H (1987) Pulmonary edema: current concepts of pathophysiology, clinical significance, and methods of measurement. World J Surg 11:147-53

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