Abstract

The focus of our efforts is to use a molecular understanding of immune function to develop safe and consistently effective immune based treatments for patients whose cancers are not currently treatable with traditional approaches such as chemotherapy, radiation and surgery. Our approach is to create mouse models to enable us to understand the basic immunology of the tumor-host interaction and to develop and pre-clinically test new treatments for patients. Data obtained from clinical trials based on experimental approaches are then used to generate new hypotheses, which are explored in the laboratory. We have now identified and cloned the mouse homologs of human tumor associated antigens and used these in the creation of recombinant and synthetic anticancer vaccines, including recombinant viruses, """"""""naked"""""""" DNA immunogens, proteins and peptides. We have optimized the functions of a variety of vaccines and learned how stimulate anti-tumor immune responses in animal models and in patients with cancer. One consequence of successful tumor immunotherapy with the T cell growth factor, interleukin-2 can be vitiligo, the patchy and usually permanent loss of pigment from the skin. We have successfully developed a mouse model for vitiligo, in which we can prevent the growth of an experimental mouse melanoma. Despite considerable advances in our understanding of the molecular basis of immune-tumor interactions, we are not yet able to consistently destroy tumor cells in patients with melanoma. We have learned that merely increasing T cell precursor frequency can be insufficient to induce anti-tumor immune responses. In order to understand how to improve therapeutic effectiveness of experimental anti-tumor vaccines we have employed mice that are transgenic for human MHC molecules (such as HLA-A2 and HLA-DR4). We also use mice that are knocked out for the antigens that we are targeting, enabling us to assess the roles for immunological tolerance to these antigens. Most recently, we have created mice that are transgenic for T cell receptors, and these mice make it possible for us to study tumor-specific T cells in a variety of activation states. In the immediate future, we plan to focus our research efforts on extending efforts to develop effective therapeutic cancer vaccines, including alphavirus replicase-based vectors for research and clinical use. Experimental vaccines will be used to explore issues surrounding the function (and non-function) of T cells that are elicited by experimental vaccines including the tolerance and apoptosis of anti-tumor T cells. An increased understanding at the molecular level of T cell activation, function and death has led us to genetically manipulate T cell function using transgenic mice. Ongoing research efforts include the conferring of new specificities to T cells (eg. insertion of new T cell receptors), enhancing the expression of pro-survival genes (eg. bcl-2) in anti-tumor T cells, knocking out negative regulators of T cell function (eg. CTLA-4), and genetically interfering with apoptotic pathways (eg. Fas-FasL)

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Division of Clinical Sciences - NCI (NCI)
Type
Intramural Research (Z01)
Project #
1Z01SC006670-10
Application #
6756287
Study Section
Surgery (SURG)
Project Start
Project End
Budget Start
Budget End
Support Year
10
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
Clinical Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Cortes, Lizette M; Mattapallil, Mary J; Silver, Phyllis B et al. (2008) Repertoire analysis and new pathogenic epitopes of IRBP in C57BL/6 (H-2b) and B10.RIII (H-2r) mice. Invest Ophthalmol Vis Sci 49:1946-56
Manjili, Masoud H; Kmieciak, Maciej; Keeler, Johanna (2006) Comment on ""Tumor progression can occur despite the induction of very high levels of self/tumor antigen-specific CD8+ T cells in patients with melanoma"". J Immunol 176:4511; author reply 4511-2
Zhao, Yangbing; Zheng, Zhili; Cohen, Cyrille J et al. (2006) High-efficiency transfection of primary human and mouse T lymphocytes using RNA electroporation. Mol Ther 13:151-9
Gattinoni, Luca; Klebanoff, Christopher A; Palmer, Douglas C et al. (2005) Acquisition of full effector function in vitro paradoxically impairs the in vivo antitumor efficacy of adoptively transferred CD8+ T cells. J Clin Invest 115:1616-26
Antony, Paul Andrew; Restifo, Nicholas P (2005) CD4+CD25+ T regulatory cells, immunotherapy of cancer, and interleukin-2. J Immunother 28:120-8
Chang, Chien-Chung; Campoli, Michael; Restifo, Nicholas P et al. (2005) Immune selection of hot-spot beta 2-microglobulin gene mutations, HLA-A2 allospecificity loss, and antigen-processing machinery component down-regulation in melanoma cells derived from recurrent metastases following immunotherapy. J Immunol 174:1462-71
Zeng, Rong; Spolski, Rosanne; Finkelstein, Steven E et al. (2005) Synergy of IL-21 and IL-15 in regulating CD8+ T cell expansion and function. J Exp Med 201:139-48
Restifo, Nicholas P; Rosenberg, Steven A (2005) Use of standard criteria for assessment of cancer vaccines. Lancet Oncol 6:3-4
Klebanoff, Christopher A; Gattinoni, Luca; Torabi-Parizi, Parizad et al. (2005) Central memory self/tumor-reactive CD8+ T cells confer superior antitumor immunity compared with effector memory T cells. Proc Natl Acad Sci U S A 102:9571-6
Charo, Jehad; Finkelstein, Steven E; Grewal, Navrose et al. (2005) Bcl-2 overexpression enhances tumor-specific T-cell survival. Cancer Res 65:2001-8

Showing the most recent 10 out of 23 publications