Abstract

Diabetes is now considered a prime risk actor for cardiovascular disease, particularly ischemic heart disease. The risks for myocardial infarction, reinfarction, ischemic heart failure, stroke and the associated mortalities are all significantly increased in diabetes. The pathobiology underlying the excessive and severe ischemic heart disease in diabetes is unclear. Myocardial ischemia-reperfusion (I'R)injury involves both early and late phases. In the early phase, the initial deposition of leukocytes amplifies cardiac injury via an acute inflammatory response. The initial step in acute inflammation is leukocyte, particularly PMN, deposition in the coronary microcirculation. It is not clear how PMNs initially accumulate in the microcirculation, but recent studies suggest that this step is amplified in the diabetic heart following ischemia. Once accumulated, the PMNs activate and produce oxygen free radicals, causing further damage to the vasculature and myocytes. Following ischemia, if PMN deposition is excessive in the diabetic coronary microcirculation an(LIor if diabetic PMNs are hyper-responsive to cytokines released from ischemic tissue, then the severity of leukocytemediated reperfusion injury may be excessive as well. In this project, we will test the hypothesis that diabetes causes alterations in both the blood and the coronary blood vessels. These alterations set the stage for an excessive leukocyte-mediated reperfusion injury in the diabetic heart. If so, then pharmacologically blocking early PMN-mediated inflammation will reduce reperfusion injury and improve the recovery of myocardial contractile function. We will first investigate specific mechanisms, suspected to cause the excessive blood-coronary microvessel interactions observed in diabetes. We will then compare leukocyte adhesion protein characteristics and the """"""""reactivity"""""""" of PMNs to stimulation in Type I and Type II diabetic animals and in patients with Type II diabetes. We will determine if platelets and plasma complement, modulate leukocyte function and leukocyte reactivity in diabetes. The therapeutic potential of limiting leukocyte-mediated inflammation in diabetes will be evaluated. Those pharmacologic agents and antibodies that prove to attenuate the early PMN-mediated response will be tested for efficacy to improve the recovery of myocardial contractile function in the diabetic. The lessons learned from these studies will aid in developing improved therapies to reduce the excessive ischemic heart disease observed in diabetes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL058859-01
Application #
2389123
Study Section
Cardiovascular and Pulmonary Research A Study Section (CVA)
Project Start
1997-08-01
Project End
2002-07-31
Budget Start
1997-08-01
Budget End
1998-07-31
Support Year
1
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Arizona
Department
Surgery
Type
Schools of Medicine
DUNS #
City
Tucson
State
AZ
Country
United States
Zip Code
85721

  Publications

Dokken, B B; La Bonte, L R; Davis-Gorman, G et al. (2011) Glucagon-like peptide-1 (GLP-1), immediately prior to reperfusion, decreases neutrophil activation and reduces myocardial infarct size in rodents. Horm Metab Res 43:300-5
La Bonte, Laura R; Dokken, Betsy; Davis-Gorman, Grace et al. (2009) The mannose-binding lectin pathway is a significant contributor to reperfusion injury in the type 2 diabetic heart. Diab Vasc Dis Res 6:172-80
La Bonte, Laura R; Davis-Gorman, Grace; Stahl, Gregory L et al. (2008) Complement inhibition reduces injury in the type 2 diabetic heart following ischemia and reperfusion. Am J Physiol Heart Circ Physiol 294:H1282-90
Maes, Melissa L; Davidson, Lisa B; McDonagh, Paul F et al. (2007) Comparison of sample fixation and the use of LDS-751 or anti-CD45 for leukocyte identification in mouse whole blood for flow cytometry. J Immunol Methods 319:79-86
Ritter, Leslie S; Stempel, Karl M; Coull, Bruce M et al. (2005) Leukocyte-platelet aggregates in rat peripheral blood after ischemic stroke and reperfusion. Biol Res Nurs 6:281-8
Le Guyader, Alexandre; Davis-Gorman, Grace; Copeland, Jack G et al. (2004) A flow cytometric method for determining the binding of coagulation factor X to monocytes in whole human blood. J Immunol Methods 292:207-15
Cohen, Zoe; Wilson, Jonathan; Ritter, Leslie et al. (2004) Caspase inhibition decreases both platelet phosphatidylserine exposure and aggregation: caspase inhibition of platelets. Thromb Res 113:387-93
Tuttle, Hillary A; Davis-Gorman, Grace; Goldman, Steve et al. (2004) Proinflammatory cytokines are increased in type 2 diabetic women with cardiovascular disease. J Diabetes Complications 18:343-51
McDonagh, Paul F; Hokama, Jason Y; Gale, Stephen C et al. (2003) Chronic expression of platelet adhesion proteins is associated with severe ischemic heart disease in type 2 diabetic patients: Chronic platelet activation in diabetic heart patients. J Diabetes Complications 17:269-78
Gale, S C; Hokama, J Y; Ritter, L S et al. (2001) Pentoxifylline reduces coronary leukocyte accumulation early in reperfusion after cold ischemia. Ann Thorac Surg 71:1305-11

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