Abstract

Human livers have been transplanted with dramatically increasing success during the past 5 years because of the improved immunosuppression provided by cyclosporin A. But the clinical option of transplantation is often reduced because donor livers can be safely preserved for only 6 to 10 hours. This limited preservation reduces the number of available livers, makes transplant surgery an emergency procedure requiring two surgical teams, and often necessitates operating on some of the sickest surgical patients (viz., liver transplant recipients) during the middle of the night. The proposed research is a comprehensive effort to improve the preservation of donor livers. We will use a dog model to: 1) define optimal conditions for continuous hypothermic perfusion (by examining the effects of perfusion pressures and the effects of administering the perfusate through the hepatic artery or portal vein, or both); 2) develop the ideal perfusate (by examining the roles of electrolyte ratio, oncotic pressure, and osmotic pressure derived from mannitol and raffinose); and 3) test drugs and other agents that minimize liver damage and facilitate the resumption of liver function after revascularization. The investigative agents will include enzyme inhibitors (allopurinol and EHNA), Ca channel blockers (nifedipine, diltiazem, and verapamil), O2-radical scavengers (SOD, catalase, mannitol, and desferrioxamine), membrane stabilizers (chlorpromazine and methylprednisolone) and prostacyclin. We will access cell viability, using an in vitro, tissue-slice model, and determine adenine nucleotide metabolism, O2 consumption, electrolyte transport, tissue edema, and protein synthesis. Cell structure will be assessed from histological analysis and electron microscopy. The viability of an organ and the integrity of its microcirculation will be assessed by orthotopic transplantation and by light and electron microscopic analyses of biopsy specimens. The initial perfusate will be one--which we recently developed for kidney preservation--that contains hydroxyethlstarch as the colloid, and adenosine, gluconate, phosphate, etc. The ultimate objective of this work is a method of clinically preserving donor livers for 48 to 72 hours that can be used in liver transplant programs.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK035143-03
Application #
3233401
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1986-08-01
Project End
1990-07-31
Budget Start
1988-08-01
Budget End
1989-07-31
Support Year
3
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Type
Schools of Medicine
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Mangino, Martin J; Tian, Tao; Ametani, Mary et al. (2008) Cytoskeletal involvement in hypothermic renal preservation injury. Transplantation 85:427-36
Knes, Jane M; Hansen, Thomas N; Gilligan, Barbara et al. (2005) Loss of endothelium-dependent relaxation in abdominal aorta preserved in a co-storage system. Transpl Int 17:699-706
Lindell, Susanne L; Compagnon, Philippe; Mangino, Martin J et al. (2005) UW solution for hypothermic machine perfusion of warm ischemic kidneys. Transplantation 79:1358-61
Mangino, Martin J; Ametani, Mary S; Gilligan, Barbara J et al. (2005) Role of peroxynitrite anion in renal hypothermic preservation injury. Transplantation 80:1455-60
Compagnon, Philippe; Lindell, Susanne; Ametani, Mary S et al. (2005) Ischemic preconditioning and liver tolerance to warm or cold ischemia: experimental studies in large animals. Transplantation 79:1393-400
Mangino, Martin J; Kosieradzki, Maciej; Gilligan, Barbara et al. (2003) The effects of donor brain death on renal function and arachidonic acid metabolism in a large animal model of hypothermic preservation injury. Transplantation 75:1640-7
Compagnon, Philippe; Wang, Hongbing; Lindell, Susanne L et al. (2002) Brain death does not affect hepatic allograft function and survival after orthotopic transplantation in a canine model. Transplantation 73:1218-27
Van der Hoeven, J A; Lindell, S; van Schilfgaarde, R et al. (2001) Donor brain death reduces survival after transplantation in rat livers preserved for 20 hr. Transplantation 72:1632-6
Kim, J S; Southard, J H (2000) Effect of phospholipase A2 inhibitors on the release of arachidonic acid and cell viability in cold-stored hepatocytes. Cryobiology 40:27-35
Southard, J H; Lindell, S; Ametani, M et al. (2000) Kupffer cell activation in liver preservation: cold storage vs machine perfusion. Transplant Proc 32:27-8

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