Abstract

In order to facilitate analysis of the complex immune response to cancer cells, a well-defined tumor model system has been established in our group. In this model the mouse renal cancer Renca, transfected with the viral protein hemagglutinin (Renca-HA) as a surrogate tumor antigen, is used. The transfer of the viral HA gene provides a tumor that is much more immunogenic, due to response by CD 8 cytotoxic T cells of the mouse to the viral protein. In addition transgenic mice have been generated where the T cell receptor (TCR) transgene specifically recognizes a single dominant peptide of the viral HA protein (TCR-HA), thus allowing for this antigen-specific T cell population to be accurately followed and monitored in vivo. These mice have been crossed onto strains which lack some of the cytotoxic effector molecules of T cells such as perforin and FasL important for killing tumor cells in vitro. Adoptive transfer of activated CD 8 T cells from these various novel mouse strains (developed in our group) to wild type mice bearing the Renca-HA tumors shows that T cell production of the effector protein FasL is crucial for rejection of Renca-HA cells in vivo, whereas the cytotoxic pathway using perforin is dispensable. The reason for the dominance of the FasL pathway may be that it is more efficiently triggered under conditions where levels of tumor antigen (HA) are very low resulting in a weak signal to the antitumor T cells. This may more accurately model the normal situation in vivo, where responses to tumor antigens are probably much weaker than response to viral antigens. Therefore our conclusions from this mouse model of renal cancer are that the FasL killing pathway may be more important than was previously thought for tumor destruction in vivo. The role of this cytotoxic FasL pathway for killing human renal cancer cells is under further investigation. This tumor model system has also proven useful for a detailed analysis of how drugs affect a CD8 T cell response, at either the generation of the response or the effector phase of the response could be used together with immunotherapy. This is due to the practical consideration that the development of the specific immune response to a single peptide from HA can be easily followed in vivo using the appropriate reagents in this model system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC010012-13
Application #
7732959
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
13
Fiscal Year
2008
Total Cost
$300,175
Indirect Cost

  Institution

Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Sun, Kai; Li, Minghui; Sayers, Thomas J et al. (2008) Differential effects of donor T-cell cytokines on outcome with continuous bortezomib administration after allogeneic bone marrow transplantation. Blood 112:1522-9
Cretney, Erika; Shanker, Anil; Yagita, Hideo et al. (2006) TNF-related apoptosis-inducing ligand as a therapeutic agent in autoimmunity and cancer. Immunol Cell Biol 84:87-98
Sayers, Thomas J; Murphy, William J (2006) Combining proteasome inhibition with TNF-related apoptosis-inducing ligand (Apo2L/TRAIL) for cancer therapy. Cancer Immunol Immunother 55:76-84
Khan, Tahira; Stauffer, Jimmy K; Williams, Rebecca et al. (2006) Proteasome inhibition to maximize the apoptotic potential of cytokine therapy for murine neuroblastoma tumors. J Immunol 176:6302-12
Sun, Kai; Wilkins, Danice E C; Anver, Miriam R et al. (2005) Differential effects of proteasome inhibition by bortezomib on murine acute graft-versus-host disease (GVHD): delayed administration of bortezomib results in increased GVHD-dependent gastrointestinal toxicity. Blood 106:3293-9
Brooks, Alan D; Sayers, Thomas J (2005) Reduction of the antiapoptotic protein cFLIP enhances the susceptibility of human renal cancer cells to TRAIL apoptosis. Cancer Immunol Immunother 54:499-505
Sedelies, Karin A; Sayers, Thomas J; Edwards, Kirsten M et al. (2004) Discordant regulation of granzyme H and granzyme B expression in human lymphocytes. J Biol Chem 279:26581-7
Sun, Kai; Welniak, Lisbeth A; Panoskaltsis-Mortari, Angela et al. (2004) Inhibition of acute graft-versus-host disease with retention of graft-versus-tumor effects by the proteasome inhibitor bortezomib. Proc Natl Acad Sci U S A 101:8120-5
Takeda, Kazuyoshi; Yamaguchi, Noriko; Akiba, Hisaya et al. (2004) Induction of tumor-specific T cell immunity by anti-DR5 antibody therapy. J Exp Med 199:437-48
Smyth, Mark J; Swann, Jeremy; Kelly, Janice M et al. (2004) NKG2D recognition and perforin effector function mediate effective cytokine immunotherapy of cancer. J Exp Med 200:1325-35

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