Abstract

Cardiopulmonary bypass (CPB) leads to profound alterations in the coagulation and immune systems, resulting in clinical complications including bleeding, thrombosis, and reperfusion injury. As demonstrated under the prior aegis of this grant, the cellular components of the two systems do not operate independently but rather directly interact to affect mutual function, as well as interacting with soluble mediators. The underlying hypothesis is that CPB leads to dynamic alterations in plateIet- Ieukocyte-endothelial cell adhesive nd functional interactions contributing to pathophysiologic events. Published articles have shown that (1) platelets are activated in vivo by CPB with resultant selective changes in adhesive ligands on the platelet surface membrane; (2) these changes are more profound in specific patient subpopulations, e.g., pediatric cyanotic congenital heart disease patients; (3) this activation leads to formation of in vivo circulating platelet leukocyte (plt-wbc) conjugates and, in temporal parallel, upregulation of the leukocyte adhesive receptor CD1 1 b on wbc; (4) pharmacologic agents such as acadesine modulate these changes; (5) adhesion of activated platelets to wbc is mediated by platelet P- seIectin while resting platelet binding is mediated by a different receptor; (6) an in vitro whole blood model shows a dynamic interplay of plt-plt homotypic adhesion versus plt-wbc heterotypic adhesion as well as dynamic alterations in plt-wbc adhesion over time that mimic he in vivo physiology; (7) aspirin does not block platelet o-granule release and consequent P-selectin expression and function. Ongoing studies show that (1) platelet adhesion results in a wbc signal transduction event ([Ca+2] flux); (2) activated platelet adhesion to monocytes results in functional tissue actor upregulation; (3) fibrinolytic protease inhibitors alter plt- wbc activation in an ex vivo """"""""closed loop"""""""" CPB model; (4) other clinical conditions - pre-eclampsia and cocaine abuse - mimic part of the pathophysiology of CPB, as does platelet transfusion. Specific questions for the next proposed grant period are: (1) what are the quantitative and functional changes in (a) platelet and (b) leukocyte adhesion receptors and in plt-wbc conjugate formation during clinical CPB?; (2) what are the in vitro and in vivo functional consequences of wbc adhesion, including (a) early signal transduction events such as [Ca +2] flux and (b) late effector events such as oxidative burst, CD1 1 /CD11/CD18 upregulation, and tissue factor expression; what are the molecules on the plt and wbc surface membranes that mediate these events?; (3) what are the mechanisms underlying these changes in CPB?; what physiological and pharmacological mediators alter these parameters?; what is the role of the endothelium and of shear stress in these interactions? The long term goals are to (1) describe he pathobiology of CPB, (2) understand the normal molecular mechanisms underlying this biology, and (3) determine potential therapeutic interventions to abrogate clinical complications of the procedure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL047193-05
Application #
2223487
Study Section
Surgery and Bioengineering Study Section (SB)
Project Start
1991-08-01
Project End
1998-05-31
Budget Start
1995-06-01
Budget End
1996-05-31
Support Year
5
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Pathology
Type
Schools of Medicine
DUNS #
082359691
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Rinder, Christine S; Smith, Michael J; Rinder, Henry M et al. (2007) Leukocyte effects of C5a-receptor blockade during simulated extracorporeal circulation. Ann Thorac Surg 83:146-52
Mathew, Joseph P; Rinder, Henry M; Smith, Brian R et al. (2006) Transcerebral platelet activation after aortic cross-clamp release is linked to neurocognitive decline. Ann Thorac Surg 81:1644-9
Rinder, Christine S; Rinder, Henry M; Smith, Michael J et al. (2006) Antithrombin reduces monocyte and neutrophil CD11b up regulation in addition to blocking platelet activation during extracorporeal circulation. Transfusion 46:1130-7
Fontes, Manuel L; Mathew, Joseph P; Rinder, Henry M et al. (2005) Atrial fibrillation after cardiac surgery/cardiopulmonary bypass is associated with monocyte activation. Anesth Analg 101:17-23, table of contents
Kosten, Thomas R; Tucker, Karen; Gottschalk, P Christopher et al. (2004) Platelet abnormalities associated with cerebral perfusion defects in cocaine dependence. Biol Psychiatry 55:91-7
Greilich, Philip E; Brouse, Chad F; Rinder, Christine S et al. (2004) Effects of epsilon-aminocaproic acid and aprotinin on leukocyte-platelet adhesion in patients undergoing cardiac surgery. Anesthesiology 100:225-33
Patel, Parag B; Pfau, Steven E; Cleman, Michael W et al. (2004) Comparison of coronary artery specific leukocyte-platelet conjugate formation in unstable versus stable angina pectoris. Am J Cardiol 93:410-3
Angelopoulou, Maria K; Rinder, Henry; Wang, Chao et al. (2004) A preclinical xenotransplantation animal model to assess human hematopoietic stem cell engraftment. Transfusion 44:555-66
Esposito, Claire J; Popescu, Wanda M; Rinder, Henry M et al. (2003) Increased leukocyte-platelet adhesion in patients with graft occlusion after peripheral vascular surgery. Thromb Haemost 90:1128-34
Rinder, Henry M; Snyder, Edward L; Tracey, Jayne B et al. (2003) Reversibility of severe metabolic stress in stored platelets after in vitro plasma rescue or in vivo transfusion: restoration of secretory function and maintenance of platelet survival. Transfusion 43:1230-7

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