Abstract

Whole organ transplantation remains the only clinically effective method of treating both acute liver failure an specific genetic defects of liver function which result in liver failure. However, there are several factors which limit the application of live transplantation in the treatment of liver insufficiency. These include: limited donor availability, inability to obtain an organ at the time when it is urgently needed, need for life- long immunosuppression and high cost. The purpose of our proposed work is to use isolated normal hepatocytes to: A. Develop Novel Methods of Cell Transplantation. B. Develop A Bioartificial Liver (BAL). Cell Transplantation. Isolated hepatocytes will be sued primarily to treat specific genetic liver defects. In these instances, correction of the defect results in normal liver function. Potential advantages of use of isolated hepatocyte transplantation include: a. cell cryopreservation, b. in vitro cell manipulation to either decrease immunogenicity or correct genetic defects using gene transfer technology cells from single donor can be used to treat multiple recipients, and d. simple technique at potentially low cost. In the past five years we have carried out studies which resulted in the development of successful methods of intraperitoneal transplantation and we plan to continue these studies and specifically address two major limitations of this technique: a. lack of long-term function and b. need for immunosuppression. In addition, we will specifically study hepatocyte transfection in vitro, examining the fate and stability of transfected hepatocytes following transplantation and in vivo by developing techniques of in situ hepatocyte transfection. Bioartificial Liver. The BAL will be used primarily to treat acute liver failure. In the past five years we have developed and tested a BAL system which utilizes microcarrier-attached normal hepatocytes on the outer surface of a hollow-fiber bioreactor. We plan to continue working with this system to define its effectiveness and characteristics, to improve its function and, in addition, develop and test other novel BAL systems. The major limitation of these systems remains inadequate tissue availability. We will thus work towards developing a BAL which utilizes xenogeneic hepatocytes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK038763-06
Application #
3238253
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1986-09-01
Project End
1995-08-31
Budget Start
1991-09-01
Budget End
1992-08-31
Support Year
6
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Detry, O; Arkadopoulos, N; Ting, P et al. (1999) Intracranial pressure during liver transplantation for fulminant hepatic failure. Transplantation 67:767-70
Detry, O; Arkadopoulos, N; Ting, P et al. (1999) Clinical use of a bioartificial liver in the treatment of acetaminophen-induced fulminant hepatic failure. Am Surg 65:934-8
Watanabe, F D; Arnaout, W S; Ting, P et al. (1999) Artificial liver. Transplant Proc 31:371-3
Arkadopoulos, N; Detry, O; Rozga, J et al. (1998) Liver assist systems: state of the art. Int J Artif Organs 21:781-7
Hunter, S J; Garvey, W T (1998) Insulin action and insulin resistance: diseases involving defects in insulin receptors, signal transduction, and the glucose transport effector system. Am J Med 105:331-45
Ljubimova, J Y; Petrovic, L M; Wilson, S E et al. (1997) Expression of HGF, its receptor c-met, c-myc, and albumin in cirrhotic and neoplastic human liver tissue. J Histochem Cytochem 45:79-87
Watanabe, F D; Mullon, C J; Hewitt, W R et al. (1997) Clinical experience with a bioartificial liver in the treatment of severe liver failure. A phase I clinical trial. Ann Surg 225:484-91; discussion 491-4
Ljubimova, J Y; Petrovic, L M; Arkadopoulos, N et al. (1997) Lack of hepatocyte growth factor receptor (c-met) gene expression in fulminant hepatic failure livers before transplantation. Dig Dis Sci 42:1675-80
Chen, S; Eguchi, S; Watanabe, F et al. (1996) Hepatic support strategies. Transplant Proc 28:2036-8
Eguchi, S; Rozga, J; Lebow, L T et al. (1996) Treatment of hypercholesterolemia in the Watanabe rabbit using allogeneic hepatocellular transplantation under a regeneration stimulus. Transplantation 62:588-93

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