Abstract

Interleukin-12 (IL-12) is a heterodimeric cytokine originally defined by its ability to induce the maturation of cytolytic lymphocytes and by its capacity to effectively synergize with IL-2 in the induction of cytolytic activity. IL-12 activates NK cells, facilitates the generation of antigen-specific cytolytic T lymphocytes (CTL), maintains tumor infiltrating lymphocytes (TIL) in culture, and induces the secretion of high levels of IFN-tau (required early in the immune response) from both T cells and NK cells in vitro and in vivo. While IL-02 may promote similar functions, IL-12 is effective at 10-1000 fold lower molar concentrations than IL-2. Since IL-12 is (apparently) secreted exclusively by professional antigen presenting cells (APC); monocytes and B cells) and IL-12 receptors are expressed selectively on activated T lymphocytes and NK cells, it appears that IL-12 is well-suited to drive the expansion and maturation of the two most prevalent anti-tumor effector cells localized within tumor lesions (T cells and NK cells). Based on our previous and current observations using in vivo murine models, we believe that IL-12 is an ideal candidate for use in the immunotherapy of cancer. In particular, we believe that IL-12 therapy will be optimally effective when administered through gene transfer in a paracrine (local) manner, either alone or in conjunction with additional costimulator molecule gene therapy. As a basis for future IL-12 clinical trials we propose the following specific aims: l. ESTABLISH EFFICIENT POLYCISTRONIC GENE TRANSFER SYSTEMS FOR PRODUCING TRANSFECTANTS SECRETING BIOLOGICALLY ACTIVE IL-12 AND EXPRESSING T-12 COSTIMULATORY MOLECULES (i.e. IL-2, B7.1, B7.2). Tumor cells, fibroblasts, and antigen presenting cells (dendritic cells or the RMA-S cell line) will be transduced with novel retroviral vectors., 2. EXAMINE THE ABILITY OF PARACRINE SECRETION OF IL-12, ALONE OR IN CONJUNCTION WITH COEXPRESSED COSTIMULATORY MOLECULES, TO ENHANCE ANTI- TUMOR IMMUNE RESPONSES IN VIVO. Engineered tumors or engineered fibroblasts admixed with tumor will be evaluated for their capacity to elicit anti-tumor immunity in vivo., 3. EXAMINE THE ADJUVANTICITY OF IL-12 ENGINEERED ANTIGEN PRESENTING CELLS IN PROMOTING ANTI-TUMOR CELLULAR IMMUNE RESPONSES. Engineered antigen presenting cells (dendritic cells or RMA-S) will be evaluated for their capacity to elicit tumor peptide- specific CTL in vitro and in vivo., 4. DEVELOP CLINICAL TRIALS UTILIZING IL-12 GENE THERAPY. We will develop vectors encoding IL-12 or costimulator molecules for clinical trials in the Human Gene Therapy Applications Laboratory (Core D) and prepare a clinical protocol based on the results obtained in Specific Aims 1-3.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
3P01CA068067-04S1
Application #
6217458
Study Section
Project Start
1998-05-01
Project End
2001-11-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
4
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Type
DUNS #
053785812
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

DeMarco, Richard A; Fink, Mitchell P; Lotze, Michael T (2005) Monocytes promote natural killer cell interferon gamma production in response to the endogenous danger signal HMGB1. Mol Immunol 42:433-44
Witham, Timothy F; Villa, Lorissa; Yang, Tianbing et al. (2003) Expression of a soluble transforming growth factor-beta (TGFbeta) receptor reduces tumorigenicity by regulating natural killer (NK) cell activity against 9L gliosarcoma in vivo. J Neurooncol 64:63-9
Son, Young-Ik; Dallal, Ramsey M; Lotze, Michael T (2003) Combined treatment with interleukin-18 and low-dose interleukin-2 induced regression of a murine sarcoma and memory response. J Immunother 26:234-40
Tatsumi, Tomohide; Gambotto, Andrea; Robbins, Paul D et al. (2002) Interleukin 18 gene transfer expands the repertoire of antitumor Th1-type immunity elicited by dendritic cell-based vaccines in association with enhanced therapeutic efficacy. Cancer Res 62:5853-8
Yang, Tianbing; Witham, Timothy F; Villa, Lorissa et al. (2002) Glioma-associated hyaluronan induces apoptosis in dendritic cells via inducible nitric oxide synthase: implications for the use of dendritic cells for therapy of gliomas. Cancer Res 62:2583-91
Son, Y I; Dallal, R M; Mailliard, R B et al. (2001) Interleukin-18 (IL-18) synergizes with IL-2 to enhance cytotoxicity, interferon-gamma production, and expansion of natural killer cells. Cancer Res 61:884-8
Okada, H; Attanucci, J; Giezeman-Smits, K M et al. (2001) Immunization with an antigen identified by cytokine tumor vaccine-assisted SEREX (CAS) suppressed growth of the rat 9L glioma in vivo. Cancer Res 61:2625-31
Son, Y I; Mailliard, R B; Watkins, S C et al. (2001) Dendritic cells pulsed with apoptotic squamous cell carcinoma have anti-tumor effects when combined with interleukin-2. Laryngoscope 111:1472-8
Okada, H; Villa, L; Attanucci, J et al. (2001) Cytokine gene therapy of gliomas: effective induction of therapeutic immunity to intracranial tumors by peripheral immunization with interleukin-4 transduced glioma cells. Gene Ther 8:1157-66
Hiroishi, K; Tuting, T; Lotze, M T (2000) IFN-alpha-expressing tumor cells enhance generation and promote survival of tumor-specific CTLs. J Immunol 164:567-72

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