Abstract

Murine tumor models have contributed much to our understanding of immune rejection processes and afford an opportunity for rapidly monitoring the in vivo therapeutic effects of cancer vaccines, adoptively transferred T cells (ATC), and bone marrow transplantation (BMT). We have shown that murine tumor lysate- pulsed dendritic cells (TP-DC) can elicit tumor-specific CD4+ and CD8+ T cell reactivities in vitro and in vivo. This observation has been made in a variety of histologically-distinct murine tumors, including sarcoma, carcinoma, and melanoma. We have also shown that syngeneic hosts can be effectively immunized in vivo to reject aggressive, weakly-immunogenic sarcomas, a breast carcinoma, and a poorly-immunogenic subline of the B16 melanoma by immunization with TP-DC, which is dependent upon host-derived CD8+ and, to a lesser extent, CD4+ T cells. TP-DC treatments could also result in regression of well-established s.c. and lung metastases, which could be further enhanced by the systemic administration of low-dose IL-2. The experimental studies outlined in this renewal application are designed to continue our successful preclinical efforts to generate more potent immunization strategies against cancer based on potent antigen- presenting dendritic cells. We will now extend our efforts on novel approaches to use TP-DC in the setting of BMT. The rationale for doing so is based on the accepted dogma that certain preparative regimens for BMT can debulk tumor load, that it can reduce tumor-induced immunosuppression, and that antigen- pulsed DC may potently """"""""educate"""""""" the developing T cell lineage to tumor-associated antigens post-BMT. The effects of TP-DC immunization on the antitumor immune response will be evaluated in the setting of BMT and the developing lymphomyeloid system upon reconstitution. We propose the following Specific Aims: 1. To determine the therapeutic efficacy of the combination of tumor-pulsed dendritic cell immunizations, recombinant cytokine administration, and BMT in mice with solid tumors; 2. To analyze the specificity, function, and repertoire of the host T cell response induced by tumor-pulsed dendritic cell immunization; 3. To determine the therapeutic efficacy of ex vivo expanded antitumor effector T cells in tumor-bearing mice with BMT and tumor-pulsed dendritic cell immunizations. The range of therapeutic strategies will be tested and compared in settings of minimal residual disease and advanced disease. The overall goal of our research effort will be to develop and optimize a new strategy that combines BMT with TP-DC vaccines, recombinant cytokines, and ATC transfer for the treatment of cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA071669-07
Application #
6633199
Study Section
Special Emphasis Panel (ZRG1-ET-1 (01))
Program Officer
Yovandich, Jason L
Project Start
1996-08-01
Project End
2003-12-31
Budget Start
2003-06-01
Budget End
2003-12-31
Support Year
7
Fiscal Year
2003
Total Cost
$336,674
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Surgery
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Komine, Hiroshi; Kuhn, Lisa; Matsushita, Norimasa et al. (2013) Examination of MARCO activity on dendritic cell phenotype and function using a gene knockout mouse. PLoS One 8:e67795
Matsushita, Norimasa; Komine, Hiroshi; Grolleau-Julius, Annabelle et al. (2010) Targeting MARCO can lead to enhanced dendritic cell motility and anti-melanoma activity. Cancer Immunol Immunother 59:875-84
Koike, Nobusada; Pilon-Thomas, Shari; Mule, James J (2008) Nonmyeloablative chemotherapy followed by T-cell adoptive transfer and dendritic cell-based vaccination results in rejection of established melanoma. J Immunother 31:402-12
Pilon-Thomas, Shari; Verhaegen, Monique; Kuhn, Lisa et al. (2006) Induction of anti-tumor immunity by vaccination with dendritic cells pulsed with anti-CD44 IgG opsonized tumor cells. Cancer Immunol Immunother 55:1238-46
Pilon-Thomas, Shari; Li, Wenbin; Briggs, Jon J et al. (2006) Immunostimulatory effects of CpG-ODN upon dendritic cell-based immunotherapy in a murine melanoma model. J Immunother 29:381-7
Asavaroengchai, W; Kotera, Y; Koike, N et al. (2004) Augmentation of antitumor immune responses after adoptive transfer of bone marrow derived from donors immunized with tumor lysate-pulsed dendritic cells. Biol Blood Marrow Transplant 10:524-33
Terando, Alicia; Roessler, Blake; Mule, James J (2004) Chemokine gene modification of human dendritic cell-based tumor vaccines using a recombinant adenoviral vector. Cancer Gene Ther 11:165-73
Grolleau, Annabelle; Misek, David E; Kuick, Rork et al. (2003) Inducible expression of macrophage receptor Marco by dendritic cells following phagocytic uptake of dead cells uncovered by oligonucleotide arrays. J Immunol 171:2879-88
Asavaroengchai, W; Kotera, Y; Mule, J J (2002) Tumor lysate-pulsed dendritic cells can elicit an effective antitumor immune response during early lymphoid recovery. Proc Natl Acad Sci U S A 99:931-6
Candido, K A; Shimizu, K; McLaughlin, J C et al. (2001) Local administration of dendritic cells inhibits established breast tumor growth: implications for apoptosis-inducing agents. Cancer Res 61:228-36

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