Abstract

Despite growing successes associated with whole organ liver transplantation, surgical risks and complications contribute significantly to patient morbidity and mortality. Hepatocyte transplantation could be used to treat acute liver failure and liver-based metabolic diseases and would avoid surgical intervention and its associated risks. A potential alternative to the transplantation of primary hepatocytes would be the use of a clonal cell line. An hepatocyte cell line would provide the advantages of availability, uniformity and sterility and could be grown in unlimited quantity and at far less cost compared to isolated primary hepatocytes. This proposal will examine whether hepatocytes can be conditionally immortalized and engineered to be non-tumorigenic when transplanted in to recipients for the treatment of liver-based metabolic diseases and liver failure. To test this hypothesis eukaryotic expression vectors will be constructed which control expression of the SV40 large T antigen at the level of both transcription and translation. Vectors will contain inducible promoters and operator/repressor sequences. Primary hepatocytes will then be immortalized by transfection with these constructs and cells will be characterized at the permissive and non-permissive conditions for gene expression to determine their level of differentiated function. Regulation of gene transcription and translocation under the various conditions will be evaluated by measuring SV40 T antigen mRNA and protein production and cell growth will be assessed in vitro and following transplantation in immunodeficient mice. In order to provide one more way to protect against possible abnormal cell growth in recipients, conditionally immortalized cells will be transduced to express a suicide gene. Introduction of the Herpes Simplex Virus - thymidine kinase gene will provide a way of eliminating the transplanted cells if desired by treatment with gancyclovir. Conditionally immortalized hepatocytes will then be transplanted into Nagase aalbuminemic rats and rats with ammonium acetate inducible hepatic coma to assess the ability of these cells to correct deficiencies in liver function in vivo. In summary, these studies will determine whether conditionally immortalized hepatocyte cell lines can be engineered to be non-tumorigenic and safe for use in the treatment of metabolic and global liver deficiencies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK048794-04
Application #
2905688
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Doo, Edward
Project Start
1996-08-01
Project End
2001-07-31
Budget Start
1999-08-01
Budget End
2000-07-31
Support Year
4
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Nebraska Medical Center
Department
Surgery
Type
Schools of Medicine
DUNS #
City
Omaha
State
NE
Country
United States
Zip Code
68198

  Publications

Nishikawa, Taichiro; Bell, Aaron; Brooks, Jenna M et al. (2015) Resetting the transcription factor network reverses terminal chronic hepatic failure. J Clin Invest 125:1533-44
Chen, Yong; Li, Yanfeng; Wang, Xia et al. (2015) Amelioration of Hyperbilirubinemia in Gunn Rats after Transplantation of Human Induced Pluripotent Stem Cell-Derived Hepatocytes. Stem Cell Reports 5:22-30
Hansel, Marc C; Gramignoli, Roberto; Blake, William et al. (2014) Increased reprogramming of human fetal hepatocytes compared with adult hepatocytes in feeder-free conditions. Cell Transplant 23:27-38
Fox, Ira J; Daley, George Q; Goldman, Steven A et al. (2014) Stem cell therapy. Use of differentiated pluripotent stem cells as replacement therapy for treating disease. Science 345:1247391
Yannam, Govardhana Rao; Han, Bing; Setoyama, Kentaro et al. (2014) A nonhuman primate model of human radiation-induced venocclusive liver disease and hepatocyte injury. Int J Radiat Oncol Biol Phys 88:404-411
Bhatia, Sangeeta N; Underhill, Gregory H; Zaret, Kenneth S et al. (2014) Cell and tissue engineering for liver disease. Sci Transl Med 6:245sr2
Nishikawa, Taichiro; Bellance, Nadège; Damm, Aaron et al. (2014) A switch in the source of ATP production and a loss in capacity to perform glycolysis are hallmarks of hepatocyte failure in advance liver disease. J Hepatol 60:1203-11
Fox, Ira J; Duncan, Stephen A (2013) Engineering liver tissue from induced pluripotent stem cells: a first step in generating new organs for transplantation? Hepatology 58:2198-201
Liu, Liping; Yannam, Govardhana Rao; Nishikawa, Taichiro et al. (2012) The microenvironment in hepatocyte regeneration and function in rats with advanced cirrhosis. Hepatology 55:1529-39
Soto-Gutierrez, Alejandro; Tafaleng, Edgar; Kelly, Victoria et al. (2011) Modeling and therapy of human liver diseases using induced pluripotent stem cells: how far have we come? Hepatology 53:708-11

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