Abstract

This application proposes the establishment of a National Cooperative Drug Development Group (NCDDG) in response to RFA 87-CA-25 from the National Cancer Institute. The focus of this NCDDG will be on the development of a novel group of chimeric toxins for the treatment of specific leukemias and lymphomas. These chimeric toxins are genetically assembled from cDNAs, or synthetic genes encoding cell specific growth factors which are fused in correct translational reading frame to a truncated diphtheria toxin structural gene. We have shown that the resulting toxin-related/growth factor fusion proteins that are expressed from the chimeric toxin genes retain both the immunologic determinants and the biologic function of their component parts. For example, the chimeric toxin assembled from interleukin-2 and a truncated form of diphtheria toxin is specifically targeted towards and intoxicates only those eukaryotic cells which bear high affinity receptors for the T-cell growth factor IL-2. As such, we are using the cell specificity of growth factors to deliver the cytotoxic activity of diphtheria toxin fragment A to the cytosol of target cells. In these instances, elongation factor 2 within th cytosol of target cells is ADP-ribosylated, and the resulting inhibition of protein synthesis causes target cell death. We have shown that all HTLV-I infected, transformed human T-cell lines which bear the high affinity IL-2 receptor, so far tested, are killed by pico molar concentrations of IL-2-toxin; whereas receptor negative cells are resistant to the action of this chimeric toxin. In the present proposal, the NCDDG will develop variants of IL-2-toxin with the long term goal of creating new biologicals for the treatment of IL-2 receptor bearing leukemias and lymphomas. We shall investigate structural/functional relationships of the chimeric toxins, their biology with respect to the IL-2 receptor on both normal and malignant cells, and their biology in vivo. Further, we shall examine the distribution and induction of high affinity IL-2 receptors on neoplastic cells from patients with leukemia/lymphoma. In addition, we shall create a new chimeric toxin based on interleukin-4, study the action of IL-4-toxin both in vitro and in vivo, and examine the distribution of the IL-4 receptor on cells from patients with leukemia / lymphoma. It is envisioned that these studies will result in a new class of highly specific and potent biologicals for the treatment of selected leukemias and lymphomas.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01CA048626-02
Application #
3549233
Study Section
(SRC)
Project Start
1988-09-30
Project End
1993-07-31
Budget Start
1989-08-01
Budget End
1990-07-31
Support Year
2
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Boston University
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02118

  Publications

vanderSpek, Johanna C; Sutherland, John A; Gill, Brian M et al. (2002) Structure function analysis of interleukin 7: requirement for an aromatic ring at position 143 of helix D. Cytokine 17:227-33
Gorgun, Gullu; van der Spek, Johanna; Cosenza, Larry et al. (2002) Altered biological activity associated with C-terminal modifications of IL-7. Cytokine 20:17-22
Sweeney, E B; Foss, F M; Murphy, J R et al. (1998) Interleukin 7 (IL-7) receptor-specific cell killing by DAB389 IL-7: a novel agent for the elimination of IL-7 receptor positive cells. Bioconjug Chem 9:201-7
Kelley, V R; Strom, T B (1995) A paradigm 1994: the allograft response. Blood Purif 13:199-205
Jean, L F; Waters, C A; Keemy, D et al. (1993) Site-directed and deletion mutational analysis of the receptor binding domain of the interleukin-6 receptor targeted fusion toxin DAB389-IL-6. Protein Eng 6:305-11
Kelley, V R; Singer, G G (1993) The antigen presentation function of renal tubular epithelial cells. Exp Nephrol 1:102-11
vanderSpek, J C; Mindell, J A; Finkelstein, A et al. (1993) Structure/function analysis of the transmembrane domain of DAB389-interleukin-2, an interleukin-2 receptor-targeted fusion toxin. The amphipathic helical region of the transmembrane domain is essential for the efficient delivery of the catalytic domain to J Biol Chem 268:12077-82
Maslinski, W; Remillard, B; Tsudo, M et al. (1993) Interleukin-2 receptor signal transduction: translocation of active serine-threonine kinase Raf-1 from IL-2 receptor into cytosol depends on IL-2-induced tyrosine kinase activation. Transplant Proc 25:109-10
Jevnikar, A M; Singer, G G; Coffman, T et al. (1993) Transgenic tubular cell expression of class II is insufficient to initiate immune renal injury. J Am Soc Nephrol 3:1972-7
Bloom, R D; Florquin, S; Singer, G G et al. (1993) Colony stimulating factor-1 in the induction of lupus nephritis. Kidney Int 43:1000-9

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