Abstract

The overall goal of this proposal is to develop strategies to eliminate lymphomas through the infusion of lymphocytes transduced with retroviral vectors containing the interleukin-I (IL-1) or interleukin-2 (IL-2) gene. The basic premise of these studies is that a defective immunosurveillance system leads to the occurrence of lymphomas. lnfusional therapy with exogenous IL-1 or IL-2 alone may be an inadequate means of producing an anti-lymphoma effect due to a failure of achieving sufficient local concentrations of lymphokines at the site of the tumor. Transduced lymphocytes with known cytolytic function against murine or human lymphoma cells represent a means of bypassing the need to infuse large quantities of potentially cytotoxic lymphokines. Therefore, we propose to utilize retroviral vectors which are capable of transducing human or mouse T-lymphocytes and producing IL-1 or IL-2 in vitro and in vivo. We will focus on identification of which T-cell subpopulations are capable of being transduced by these retroviral vectors. In addition, we will investigate the use of the herpesvirus thymidine kinase gene as a suicide marker to be used in instances in which the transduced lymphocytes become autonomously proliferating. Once we have obtained transduced lymphocyte populations, we will infuse human lymphocytes into severe combined immunodeficiency (SCID) mice or murine cells into normal mice. We will examine the persistence of these cell populations as well as the continued expression of these transduced lymphocytes and their tumorigenic potential. We will drive these lymphocytes in vivo with exogenous IL-1 and/or IL-2 as a means of promoting their persistence. Finally, we will examine the ability of these transduced lymphocyte populations to mediate an anti-lymphoma effect. Using SCID mice and human lymphoma cell lines or fresh lymphoma tissue, we will assess the potential benefit of transduced lymphocyte populations as in vivo cellular immunotherapy. A parallel study using murine lymphomas in normal or immunosuppressed mice will allow us to examine the effect of cellular immunotherapy in a setting in which the full species specific lymphohemopoietic system is intact. These data will be used in conjunction with the preclinical and clinical studies of immunotherapy for lymphoma to cumulatively design the most effective and safe adjunctive therapy for the elimination of lymphoma in the context of autologous bone marrow transplantation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA021737-19
Application #
5206949
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
19
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Flynn, Catherine M; Hirsch, Betsy; Defor, Todd et al. (2007) Reduced intensity compared with high dose conditioning for allotransplantation in acute myeloid leukemia and myelodysplastic syndrome: a comparative clinical analysis. Am J Hematol 82:867-72
Orchard, Paul J; Blazar, Bruce R; Wagner, John et al. (2007) Hematopoietic cell therapy for metabolic disease. J Pediatr 151:340-6
Grewal, Satkiran S; Barker, Juliet N; Davies, Stella M et al. (2003) Unrelated donor hematopoietic cell transplantation: marrow or umbilical cord blood? Blood 101:4233-44
Wagner, John E; Barker, Juliet N; DeFor, Todd E et al. (2002) Transplantation of unrelated donor umbilical cord blood in 102 patients with malignant and nonmalignant diseases: influence of CD34 cell dose and HLA disparity on treatment-related mortality and survival. Blood 100:1611-8
Sladek, Norman E (2002) Leukemic cell insensitivity to cyclophosphamide and other oxazaphosphorines mediated by aldehyde dehydrogenase(s). Cancer Treat Res 112:161-75
Browne, P V; Weisdorf, D J; DeFor, T et al. (2000) Response to thalidomide therapy in refractory chronic graft-versus-host disease. Bone Marrow Transplant 26:865-9
Delforge, M; Boogaerts, M A; McGlave, P B et al. (1999) BCR/ABL- CD34(+)HLA-DR- progenitor cells in early chronic phase, but not in more advanced phases, of chronic myelogenous leukemia are polyclonal. Blood 93:284-92
Warwick, A B; Mertens, A C; Shu, X O et al. (1998) Outcomes following mechanical ventilation in children undergoing bone marrow transplantation. Bone Marrow Transplant 22:787-94
Katsanis, E; Weisdorf, D J; Miller, J S (1998) Activated peripheral blood mononuclear cells from patients receiving subcutaneous interleukin-2 following autologous stem cell transplantation prolong survival of SCID mice bearing human lymphoma. Bone Marrow Transplant 22:185-91
Arns da Cunha, C; Weisdorf, D; Shu, X O et al. (1998) Early gram-positive bacteremia in BMT recipients: impact of three different approaches to antimicrobial prophylaxis. Bone Marrow Transplant 21:173-80

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