The long-term objective of the proposed study is to develop strategies of immune depletion and repletion which will facilitate engraftment and be applicable to human organ transplantation. This objective will be achieved by investigating in non-human primates the approaches already proven successful in rodent organ transplant experiments before applying those approaches in human clinical trials. The use of total lymphoid irradiation (TLI) will be refined in the rhesus monkey prior to renal transplantation. TLI will be used alone and in conjunction with drugs, monoclonal antibodies, and adoptively transferred effector T cells to prolong allograft survival and pig-to-monkey xenograft survival. To establish new and innovative strategies to immune modification of sensitized recipients, the alloantibody and xenoantibody responses to heart and liver grafts in rats and kidney grafts in monkeys will be characterized. Methods will include selection of antibody by class and subclass; suppression by monoclonal antibody directed against antibody forming cells, their precursors and the collaborating T-cells; and depletion of allo- or xeno-reactive antibody before transplantation established that the predominant T cell receptor gene rearrangements observed in long-lived T cell lines from human renal allografts also occur in monkeys, then monoclonal antibodies and/or effector T cells directed against these receptors will be used to prevent or treat rejection. Within the time period of the Program Project, the new and promising strategies of immune modification which are proven successful and safe in non-human primates may become the subjects of human clinical investigations.

Project Start
Project End
Budget Start
Budget End
Support Year
6
Fiscal Year
1988
Total Cost
Indirect Cost
Name
Duke University
Department
Type
DUNS #
071723621
City
Durham
State
NC
Country
United States
Zip Code
27705
Kirk, A D; Bollinger, R R; Finn, O J (1995) Rapid, comprehensive analysis of human cytokine mRNA and its application to the study of acute renal allograft rejection. Hum Immunol 43:113-28
Pruitt, S K; Kirk, A D; Bollinger, R R et al. (1994) The effect of soluble complement receptor type 1 on hyperacute rejection of porcine xenografts. Transplantation 57:363-70
Pruitt, S K; Baldwin 3rd, W M; Barth, R N et al. (1993) The effect of xenoreactive antibody and B cell depletion on hyperacute rejection of guinea pig-to-rat cardiac xenografts. Transplantation 56:1318-24
Spurney, R F; Onorato, J J; Ruiz, P et al. (1993) Characterization of glomerular thromboxane receptors in murine lupus nephritis. J Pharmacol Exp Ther 264:584-90
Gravatt, L C; Chaffee, S; Hebert, M E et al. (1993) Efficacy and toxicity of 9-beta-D-arabinofuranosylguanine (araG) as an agent to purge malignant T cells from murine bone marrow: application to an in vivo T-leukemia model. Leukemia 7:1261-7
Kirk, A D; Li, R A; Kinch, M S et al. (1993) The human antiporcine cellular repertoire. In vitro studies of acquired and innate cellular responsiveness. Transplantation 55:924-31
Pruitt, S K; Weinstock, D; Suyemoto, M M et al. (1993) Effect of bursectomy on deposition of natural xenoreactive antibodies and complement within rat cardiac xenografts in the chicken. Transplant Proc 25:435-7
Messina, J P; Gilkeson, G S; Pisetsky, D S (1993) The influence of DNA structure on the in vitro stimulation of murine lymphocytes by natural and synthetic polynucleotide antigens. Cell Immunol 147:148-57
Kirk, A D; Heinle, J S; Mault, J R et al. (1993) Ex vivo characterization of human anti-porcine hyperacute cardiac rejection. Transplantation 56:785-93
Brauer, R B; Baldwin 3rd, W M; Daha, M R et al. (1993) Use of C6-deficient rats to evaluate the mechanism of hyperacute rejection of discordant cardiac xenografts. J Immunol 151:7240-8

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