Abstract

The UWCCC Biotherapy Program has a long interest of integrating clinical biotherapy trials with preclinical and clinical immunological observations, focusing on the role of immunotherapy in the treatment of cancer patients. Our recent approaches have centered around increasing anti-tumor activity by endogenous tumor reactive T cells by delivering BRM genes using a novel particle mediated gene transfer (PMGT) technology. Using this technology, we have demonstrated that we can induce effective antitumor immunity by inserting the cDNA for genes such as IL-12, GM-CSF, or IFN-gamma into tumor cells or peritumor epidermal tissues. Building upon these observations, we propose four years of clinical trials testing the hypothesis that vaccines consisting of BRM-gene transfer, using the PMGT technology, can be safety administered and will result in effective antitumor immunity. Specifically, during these four years, we will perform four clinical trials to: A-1 and A-2: Determine whether gene transfer of GM-CSF cDNA, by PMGT technology, will result in local transgenic production of GM-CSF and a local inflammatory response sufficient to stimulate a systemic antitumor immune response; and to evaluate and compare the safety, toxicities and biological effects of ex vivo PMGT of GM-CSF cDNA to tumor cells, and in vivo PMGT of GM-CSF cDNA to nontransformed tumor vaccination sites (years 1 and 2): B: Examine and compare the effects of ex vivo, or in situ gene transfer of IL-12 cDNA on local transgenic production of IL-12, and the generation of both a local and systemic antitumor immune response (years 2 and 3); C: Determine and compare the safety, toxicity and biological activity of two different dose levels of c-DNA for MART-1 either alone or in combination with two different dose levels of cDNA for B7-1 and or IFN- gamma (years 3 and 4). In close collaboration with Programs II and IV, detailed biological endpoints on each of the clinical trials will be evaluated to determine the effects of gene therapy on local and systemic transgene expression, and to characterize the local and systemic immune response. These trials will result in a deeper understanding of the biological and clinical effects of a novel method of gene delivery for vaccine treatment of patients with cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01CA061498-06
Application #
6102939
Study Section
Project Start
1998-09-01
Project End
1999-08-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
6
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Type
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Cassaday, Ryan D; Sondel, Paul M; King, David M et al. (2007) A phase I study of immunization using particle-mediated epidermal delivery of genes for gp100 and GM-CSF into uninvolved skin of melanoma patients. Clin Cancer Res 13:540-9
Mahvi, D M; Shi, F-S; Yang, N-S et al. (2002) Immunization by particle-mediated transfer of the granulocyte-macrophage colony-stimulating factor gene into autologous tumor cells in melanoma or sarcoma patients: report of a phase I/IB study. Hum Gene Ther 13:1711-21
Rakhmilevich, A L; Imboden, M; Hao, Z et al. (2001) Effective particle-mediated vaccination against mouse melanoma by coadministration of plasmid DNA encoding Gp100 and granulocyte-macrophage colony-stimulating factor. Clin Cancer Res 7:952-61
Sondel, P M; Hank, J A (2001) Antibody-directed, effector cell-mediated tumor destruction. Hematol Oncol Clin North Am 15:703-21
Rakhmilevich, A L; Janssen, K; Hao, Z et al. (2000) Interleukin-12 gene therapy of a weakly immunogenic mouse mammary carcinoma results in reduction of spontaneous lung metastases via a T-cell-independent mechanism. Cancer Gene Ther 7:826-38
Hank, J A; Surfus, J; Gan, J et al. (1999) Distinct clinical and laboratory activity of two recombinant interleukin-2 preparations. Clin Cancer Res 5:281-9
Hank, J A; Albertini, M R; Sondel, P M (1999) Monoclonal antibodies, cytokines and fusion proteins in the treatment of malignant disease. Cancer Chemother Biol Response Modif 18:210-22
Surfus, J E; Hank, J A; Oosterwijk, E et al. (1996) Anti-renal-cell carcinoma chimeric antibody G250 facilitates antibody-dependent cellular cytotoxicity with in vitro and in vivo interleukin-2-activated effectors. J Immunother Emphasis Tumor Immunol 19:184-91
Helfand, S C; Hank, J A; Gan, J et al. (1996) Lysis of human tumor cell lines by canine complement plus monoclonal antiganglioside antibodies or natural canine xenoantibodies. Cell Immunol 167:99-107
Helfand, S C; Modiano, J F; Moore, P F et al. (1995) Functional interleukin-2 receptors are expressed on natural killer-like leukemic cells from a dog with cutaneous lymphoma. Blood 86:636-45

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