Abstract

It is the purpose of this study to investigate at a mechanical, hemodynamic and subcellular level the defect in myocardial function as a result of surgically induced glogal ischemia and reperfusion. Since mechanical measures of myocardial function necessitates reperfusion, ischemic injury will be documented by identifying specific subcellular defects (Sarcoplasmic Reticulum Calcium flux and ATPase activity, Myofibrillar ATPase activity and Calcium binding and Sarcolemma Na plus K ion ATPase and Adenylate Cyclase. Based on this information, the first objective of this study will be to design specific protection against ischemic injury. Three possible protective mechanisms will be addressed: 1) Lysosomal stabilization; 2) Sarcolemmal stabilization; and 3) Proton Sequestration. The second objective of this study, based on the preceeding information, will become the definition and characterization of reperfusion injury. This will be accomplished by designing a sophisticated model of reperfusion with internal controls. Reperfusion injury will be characterized as either a primary form of tissue injury or an extension of ischemic injury defined as uneven reperfusion creating localized areas of myocardial oxygen supply to demand imbalance. Mechanical function (dP/dt-max, plus dP/dt, -dP/dt, and isovolumetric LV pressure before and after catecholamine stimulation) will be correlated with coronary hemodynamics (total and regional myocardial flow and coronary vascular resistance) and subcellular function. Any imbalance in reperfusion flow will be documented on both a physiological and anatomic bases. Based on this information, specific protection will be designed to minimize or eliminate reperfusion injury and will include direct coronary vasodilators, modification of the perfusate, platelet inhibition and the new concept of sequential reperfusion. The third objective of this study will then evaluate these findings on the intact myocardium on a hemodynamic, mechanical and subcellular basis and extend the concept of afterload reduction to the post-operative heart.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL024917-06
Application #
3337902
Study Section
Surgery and Bioengineering Study Section (SB)
Project Start
1983-02-01
Project End
1986-01-31
Budget Start
1985-02-01
Budget End
1986-01-31
Support Year
6
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Type
Schools of Medicine
DUNS #
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Kukreja, R C; Loesser, K E; Kearns, A A et al. (1993) Protective effects of histidine during ischemia-reperfusion in isolated perfused rat hearts. Am J Physiol 264:H1370-81
Eich, D M; Nestler, J E; Johnson, D E et al. (1993) Inhibition of accelerated coronary atherosclerosis with dehydroepiandrosterone in the heterotopic rabbit model of cardiac transplantation. Circulation 87:261-9
Okabe, E; Takahashi, S; Norisue, M et al. (1993) The effect of hypochlorous acid and hydrogen peroxide on coronary flow and arrhythmogenesis in myocardial ischemia and reperfusion. Eur J Pharmacol 248:33-9
Vinnikova, A K; Kukreja, R C; Hess, M L (1992) Singlet oxygen-induced inhibition of cardiac sarcolemmal Na+K(+)-ATPase. J Mol Cell Cardiol 24:465-70
Kukreja, R C; Kearns, A A; Zweier, J L et al. (1991) Singlet oxygen interaction with Ca(2+)-ATPase of cardiac sarcoplasmic reticulum. Circ Res 69:1003-14
Loesser, K E; Kukreja, R C; Kazziha, S Y et al. (1991) Oxidative damage to the myocardium: a fundamental mechanism of myocardial injury. Cardioscience 2:199-216
Kukreja, R C; Weaver, A B; Hess, M L (1990) Sarcolemmal Na(+)-K(+)-ATPase: inactivation by neutrophil-derived free radicals and oxidants. Am J Physiol 259:H1330-6
Kukreja, R C; Kontos, H A; Hess, M L (1990) Captopril and enalaprilat do not scavenge the superoxide anion. Am J Cardiol 65:24I-27I
Scott, R B; Wood, H E; Matin, S et al. (1990) Superoxide radical production after phorbol ester stimulation in neutrophils of aged donors. Exp Gerontol 25:523-32
Kontos, H A; Wei, E P; Kukreja, R C et al. (1990) Differences in endothelium-dependent cerebral dilation by bradykinin and acetylcholine. Am J Physiol 258:H1261-6

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