Abstract

The inflammatory process, stimulated by reperfusion following tissue ischemia, leads to local injury. With sufficiently large regions and times of ischemia, sizable quantities of mediators gain entry into the vasculature and lead to remote organ failure accompanied by prominent leukosequestration. This study of reperfusion injury will test the postulates that; (1) in the ischemic region, endothelial phenotype changes with the appearance of neoantigens, causing the deposition of immune complexes and activation of the classical complement pathway; (2) local injury via the terminal C5b-9 complex is permitted by loss of membrane complement regulatory proteins as well as the appearance of a scaffolding to strengthen complement binding to the cell membrane; (3) the scaffolding is thought to be provided by the adhesion glycoprotein P selectin which contains 9 short consensus repeats homologous with other complement binding proteins; (4) remote pulmonary injury is dependent upon binding of C3 components to an altered endothelium. This complement fragment works in synergy with neutrophils. Reoxygenation and reperfusion experiments will be conducted in endothelial cell cultures, ex-vivo blood vessels as well as in intact mice, rats, human volunteers, patients undergoing thoracoabdominal aneurysmectomy and femoral-popliteal bypass surgery. Assays will include the detection of membrane bound immune complexes, complement fragments, complement regulatory proteins as well as cell bound and soluble P-selectin. A variety of reagents will be employed to study mechanisms of injury, including monoclonal antibodies to proteins as well as genetically engineered materials: peptides homologous with selectin complementarily determining regions; soluble P-selectin, soluble counter receptor of P-selectin including sialyl Lewis and P-selectin glycoprotein ligand-1. Measurement techniques include immunohistochemistry, flow cytometry as well as standard methods for muscle and lung permeability using 125I-albumin, myeloperoxidase for neutrophil sequestration and the hemolytic red cell assay for classical and alternative complement activation. The data generated should provide an understanding of the putative functions of P selectin in leukocyte-endothelial adhesion as well as in complement binding.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Specialized Center (P50)
Project #
5P50GM052585-02
Application #
5212280
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Sadeghipour, Hamed; Torabi, Radbeh; Gottschall, James et al. (2017) Blockade of IgM-Mediated Inflammation Alters Wound Progression in a Swine Model of Partial-Thickness Burn. J Burn Care Res 38:148-160
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Houde, Martin; Jamain, Marc-David; Labonte, Julie et al. (2013) Pivotal role of mouse mast cell protease 4 in the conversion and pressor properties of Big-endothelin-1. J Pharmacol Exp Ther 346:31-7
Gurish, Michael F; Austen, K Frank (2012) Developmental origin and functional specialization of mast cell subsets. Immunity 37:25-33
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Afnan, Jalil; Ahmadi-Yazdi, Cyrus; Sheu, Eric G et al. (2010) Inhibition of rat gut reperfusion injury with an agent developed for the mouse. Evidence that amplification of injury by innate immunity is conserved between two animal species. Am J Physiol Regul Integr Comp Physiol 298:R1675-81
Haas, Michael S; Alicot, Elisabeth M; Schuerpf, Franziska et al. (2010) Blockade of self-reactive IgM significantly reduces injury in a murine model of acute myocardial infarction. Cardiovasc Res 87:618-27

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