Abstract

The proposed research will delineate the effects of removing or inhibiting tumor-induced T suppressor (Ts) cells on the in vitro activation of tumor-reactive lymphocytes in mice and humans. Using the P815 tumor model in which we have been studying Ts effects, Ts cells from tumor-bearing hosts (TBH) whose ability to respond to their tumors has begun to decline, will be removed or inhibited by in vivo treatment with cyclophosphamide (CYP), irradiation, or cimetidine or by in vitro treatment with 4- hydroperoxycyclophosphamine (4HpCY) or cimetidine. We will first determine whether these manipulations increase the generation of CTL and subsequently, whether they will increase the in vitro expansion of tumor-reactive cells in interleukin-2- supplemented cultures. We will also test whether depletion of Lyt2+ or L3T4+ T-cell subsets improves the propagation of T cells with helper or lytic functions, respectively, respectively. Murine tumor-reactive T cells expanded in vitro after Ts depletion will then be tested for in vivo efficacy in early TBHs and in our adjuvant model (TBH mice with systemic metastases and in whom Ts activity has become dominant). The adoptive transfer of these T cells will be combined with anti-Ts treatments of the host and exogenous IL-2. In our preliminary studies of the in vitro immune responses of cells from draining lymph nodes (DLN) breast cancer patients, there is considerable variability among DLNs from each patient, and the proliferative response can be significantly increased by removal of Leu-7+ cells. In the proposed research, we will determine the effect of eliminating or inhibiting Ts cells on the in vitro proliferation and expansion of tumor-reactive lymphocytes from breast cancer patients' DLN (obtained at the time of surgery). Ts cells will be removed on the basis of phenotypic markers (Leu-7, OKM1, CD8 antigens and Fc receptors) or inhibited by in vitro incubation with 4-HpCY. Propagation of cytolytic and T helper cells will also be studied. For both the murine and human lymphocytes, we will also determine whether Ts-depleted tumor-reactive T cells can be propagated by stimulation with tumor antigen or phorbol dibutyrate + ionomycin and IL-2, as we have done for normal mouse and human killer lymphocytes. Thus, by combining abrogation of Ts function with activation and expansion of tumor-reactive T cells and testing in vivo efficacy in a relevant mouse model, the research proposed should lead to improved strategies of adoptive immunotherapy for cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA048075-02
Application #
3192024
Study Section
(SRC)
Project Start
1988-08-15
Project End
1991-07-31
Budget Start
1989-08-01
Budget End
1990-07-31
Support Year
2
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Type
Overall Medical
DUNS #
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Miller, Catriona H T; Graham, Laura; Bear, Harry D (2010) Phenotype, functions and fate of adoptively transferred tumor draining lymphocytes activated ex vivo in mice with an aggressive weakly immunogenic mammary carcinoma. BMC Immunol 11:54
Chin, Cynthia S; Miller, Catriona H T; Graham, Laura et al. (2004) Bryostatin 1/ionomycin (B/I) ex vivo stimulation preferentially activates L-selectinlow tumor-sensitized lymphocytes. Int Immunol 16:1283-94
Parviz, Maryam; Chin, Cynthia S; Graham, Laura J et al. (2003) Successful adoptive immunotherapy with vaccine-sensitized T cells, despite no effect with vaccination alone in a weakly immunogenic tumor model. Cancer Immunol Immunother 52:739-50
Chin, Cynthia S; Bear, Harry D (2002) Sentinel node mapping identifies vaccine-draining lymph nodes with tumor-specific immunological activity. Ann Surg Oncol 9:94-103
Chin, C S; Graham, L J; Hamad, G G et al. (2001) Bryostatin/ionomycin-activated T cells mediate regression of established tumors. J Surg Res 98:108-15
Kos, F J; Cornell, D L; Lipke, A B et al. (2000) Protective role of IL-2 during activation of T cells with bryostatin 1. Int J Immunopharmacol 22:645-52
Kos, F J; Bear, H D (1998) Involvement of protein kinase C-delta in CD28-triggered cytotoxicity mediated by a human leukaemic cell line YT. Immunology 94:575-9
Baldwin, N G; Rice, C D; Tuttle, T M et al. (1997) Ex vivo expansion of tumor-draining lymph node cells using compounds which activate intracellular signal transduction. I. Characterization and in vivo anti-tumor activity of glioma-sensitized lymphocytes. J Neurooncol 32:19-28
Rice, C D; Baldwin, N G; Biron, R T et al. (1997) Ex vivo expansion of tumor-draining lymph node cells using compounds which activate intracellular signal transduction. II. Cytokine production and in vivo efficacy of glioma-sensitized lymphocytes. J Neurooncol 32:29-38
Merchant, R E; Baldwin, N G; Rice, C D et al. (1997) Adoptive immunotherapy of malignant glioma using tumor-sensitized T lymphocytes. Neurol Res 19:145-52

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