Abstract

The goal of these studies is to induce long-term specific unresponsiveness to allografts without the need for chronic immunosuppression. A well- studied protocol, treatment of recipients with a short course of antilymphocyte serum (ALS) and donor bone marrow cells (BMC), has promise in this regard, but only a small percentage of grafts are retained long- term. We have recently observed that if the ALS/BMC, skin- or islet cell- grafted mice are exposed to donor strain neonatal tissue, the length of graft survival is considerably increased. Not only do neonatal grafts survive longer that adult grafts, but if adult-grafted animals are co- transplanted with neonatal tissue, the length of adult graft survival is increased. Additionally, it appears that a more profound state of immunological unresponsiveness is induced by exposure to neonatal, rather than adult, alloantigen. We propose to investigate the mechanisms by which neonatal skin allografts and adult allografts co-transplanted with neonatal donor strain tissue enjoy prolonged survival in ALS-BMS treated mice. Cells recovered from animals bearing long-term surviving grafts will be tested in vivo and in vitro for immunological reactivity. Also, the response of cells from naive animals to neonatal and neonatal plus adult alloantigen will be analyzed in vitro. Immunohistochemical analysis of the development of immunoregulatory cells in the transplanted skin will be carried out, and such cells isolated, to determine their contribution to the induction of unresponsiveness. In a pilot experiment in which a short course of therapy with cyclosporin A has been added to the treatment protocol, strikingly improved survival of neonatal skin allografts has been observed (>80% of grafts have survive >180 d). Therefore, this combined treatment will be extended to attempt to prolong survival of adult grafts co-transplanted with neonatal tissue, and to strongly incompatible recipient/donor combinations, including xenogeneic combinations. Cells that preferentially activate suppressor pathways are known to be present in adult tissues and can be recovered by fractionation, or their activity can be """"""""unmasked"""""""" by UV-irradiation of the tissue. Therefore, we will attempt to use such adult-donor derived cells to simulate the immunoregulatory effects of neonatal tissue. The understanding which we will gain of the immunoregulatory potential of neonatal alloantigen should lead to the ability to induce specific, long-term unresponsiveness to allografts from adult donors, and ultimately to application to human transplantation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
3R01AI029650-05S1
Application #
2327167
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Project Start
1990-04-01
Project End
1999-08-31
Budget Start
1994-04-01
Budget End
1999-08-31
Support Year
5
Fiscal Year
1996
Total Cost
Indirect Cost

  Institution

Name
Northeastern University
Department
Other Health Professions
Type
Schools of Allied Health Profes
DUNS #
039318308
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

De Fazio, S R; Gozzo, J J (2000) Role of graft interleukin-10 expression in the tolerogenicity of neonatal skin allografts. Transplantation 70:1371-7
Masli, S; De Fazio, S R; Gozzo, J J (2000) Requirement for early donor cell chimerism during prolonged survival of murine skin allografts. Transplantation 69:1667-75
Gozzo, J; De Fazio, S (1999) Role of graft cytokine expression in the tolerogenicity of neonatal skin allografts. Transplant Proc 31:813
Gozzo, J; Masli, S; De Fazio, S (1999) Extension of graft survival with pulsed administration of donor dendritic cells. Transplant Proc 31:1196
Markees, T G; Jamshidi, F; De Fazio, S R et al. (1996) Association between epidermal interleukin-10 secretion and the ability of cotransplanted skin from neonatal donors to prolong adult allograft survival. Transplantation 61:111-5
De Fazio, S R; Plowey, J M; Hartner, W C et al. (1996) Late adjunctive therapy with single doses of rapamycin in skin-allografted mice treated with antilymphocyte serum and donor bone marrow cells. Transpl Immunol 4:105-12
Markees, T G; De Fazio, S R; Gozzo, J J (1994) Tolerogenic behavior of skin allografts from neonatal mice. Transplantation 58:1008-14
De Fazio, S R; Gozzo, J J (1994) Prolongation of skin allograft survival by cotransplantation of ultraviolet B-irradiated skin. Transplantation 58:1044-7
Jamshidi, F; De Fazio, S R; Gozzo, J J (1993) Allograft and xenograft unresponsiveness induced by transplantation of neonatal skin. Transplantation 56:135-8
Markees, T G; De Fazio, S R; Gozzo, J J (1992) Prolonged adult skin allograft survival as a result of cotransplantation with neonatal tissue. The requirement for antigen sharing between graft and cotransplant. Transplantation 54:955-8

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