Abstract

The goal of this proposal is to develop improved marrow transplant preparative regimens for the treatment of malignant and nonmalignant diseases of the marrow. Marrow transplantation is a widely used form of therapy for diseases of the marrow; over 5,000 transplants were performed last year alone. The success of transplantation, as currently used, is limited primarily by inadequacies of the preparative regimens which are often incapable of eradicating the marrow-based disease, yet are frequently associated with severe or fatal nonhematopoietic toxicities. This project will explore whether improved preparative regimens can be developed by using radiotherapy targeted specifically to the marrow. Two approaches to targeting marrow will be taken. One approach is to use radionuclides linked to antibodies reactive with antigens expressed on cells of marrow origin. The second approach is to use radionuclides linked to boneseeking agents as a way of delivering radiotherapy specifically to the marrow cavity. A canine model will be used to explore these two approaches. For the antibody studies, initial experiments will involve murine monoclonal antibodies specifically reactive with canine myeloid cells labeled with trace amounts of radionuclide, administered intravenously to normal dogs. Using external gamma camera imaging and organ biopsies, specific experiments will determine the biodistribution over time of the radiolabeled antibody, and will explore those factors which influence biodistribution, including antibody dose, form, amount of antigen on target cells, mass of targeted cells, deiodination (in the case of radioiodinated antibody), and the use of alternative radionuclides. The actual radiobiologic effects of radiolabeled antibodies will be determined by labeling a nonbinding antibody and a specific antimyeloid antibody with high levels of activity and determining the effects of these reagents in dogs given no transplant support to determine the marrow ablative effects of these reagents, autologous transplant support to determine nonhematopoietic dose-limiting toxicities, or allogeneic transplantation to determine the immunosuppressive effects of these reagents. A similar series of experiments will be performed using an energetic beta emitter (166Ho) linked to the bone-seeking aminophosphonic acid EDTMP. Again using a canine model, the biodistribution of 166Ho-EDTMP will be determined and the actual radiobiologic effects of 166Ho-EDTMP will be measured by administering the agent to normal dogs given no marrow support, autologous marrow, or allogeneic marrow.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA018105-16
Application #
3164831
Study Section
Experimental Immunology Study Section (EI)
Project Start
1986-03-01
Project End
1996-02-28
Budget Start
1991-03-01
Budget End
1992-02-29
Support Year
16
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Fred Hutchinson Cancer Research Center
Department
Type
DUNS #
075524595
City
Seattle
State
WA
Country
United States
Zip Code
98109

  Publications

Garrido, S M; Appelbaum, F R; Willman, C L et al. (2001) Acute myeloid leukemia cells are protected from spontaneous and drug-induced apoptosis by direct contact with a human bone marrow stromal cell line (HS-5). Exp Hematol 29:448-57
Garrido, S M; Cooper, J J; Appelbaum, F R et al. (2001) Blasts from elderly acute myeloid leukemia patients are characterized by low levels of culture- and drug-induced apoptosis. Leuk Res 25:23-32
Garrido, S M; Willman, C; Appelbaum, F R et al. (2000) Three-color versus four-color multiparameter cell cycle analyses of primary acute myeloid leukemia samples. Cytometry 42:83-94
Banker, D E; Radich, J; Becker, A et al. (1998) The t(8;21) translocation is not consistently associated with high Bcl-2 expression in de novo acute myeloid leukemias of adults. Clin Cancer Res 4:3051-62
Banker, D E; Groudine, M; Willman, C L et al. (1998) Cell cycle perturbations in acute myeloid leukemia samples following in vitro exposures to therapeutic agents. Leuk Res 22:221-39
Banker, D E; Groudine, M; Norwood, T et al. (1997) Measurement of spontaneous and therapeutic agent-induced apoptosis with BCL-2 protein expression in acute myeloid leukemia. Blood 89:243-55
Francisco, L V; Langston, A A; Mellersh, C S et al. (1996) A class of highly polymorphic tetranucleotide repeats for canine genetic mapping. Mamm Genome 7:359-62
Hong, D S; Huss, R; Beckham, C et al. (1995) Major histocompatibility complex class II-mediated inhibition of hemopoiesis in vitro and in vivo is abrogated by c-kit ligand. Transplant Proc 27:642-3
Huss, R; Hong, D S; Beckham, C et al. (1995) Ultrastructural localization of stem cell factor in canine marrow-derived stromal cells. Exp Hematol 23:33-40
Storb, R; Raff, R F; Appelbaum, F R et al. (1994) Fractionated versus single-dose total body irradiation at low and high dose rates to condition canine littermates for DLA-identical marrow grafts. Blood 83:3384-9

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