Abstract

Active specific immunotherapy is an attractive strategy for patients with prostate cancer because this tumor is slow growing, potentially allowing time to augment host responses. Moreover, the available treatment options are limited to surgery and hormonal intervention with most tumors eventually becoming hormonal refractory. The studies proposed in this application are focused on generating host immune responses to prostate tumor cells and, in particular to prostate specific ,antigen (PSA), and to prostate specific membrane antigen (PSMA). As PSA and PSMA are immunogenic, produced by the majority of prostate cancer cells, and nearly exclusively expressed by prostate cells, they represent attractive targets separately and together for active specific immunotherapy of prostate cancer. Our approach is to use CD64 (FcyRI) targeted fusion proteins (FP) to deliver PSA and/or PSMA specifically to CD64 on antigen presenting cells (APC). Our previous studies, and those of other workers, have shown that targeting antigen via similar FPs significantly improves antigen presentation. In addition, FPs (H22xPSA) incorporating PSA and the humanized Fab portion of anti-CD64 could target CD64 expressing cells to process and present peptides in association with MHC class I for killing by cytolytic T lymphocytes specific for PSA peptides. Based on these findings, we propose studies in this application that would establish a coherent strategy for a phase I clinical trial to treat prostate cancer patients with metastatic disease. In particular, we would: 1) Evaluate the efficiency and extent to which targeting the tumor associated antigens PSA and PSMA to antigen presenting cells modulates MHC class I and II restricted T cell responses. We would develop FP constructed with anti-CD64 and whole tumor protein, and evaluate their ability to target appropriate processing and presentation by APC for generation of anti-tumor Th1 and CTL responses, and the relative efficiency and extent to which different FP target processing and presentation in association with MHC class I and/or Il; 2) Evaluate the mechanisms associated with enhanced processing and presentation resulting from targeting prostate antigens to FcyRI on antigen presenting cells, including the effects on antigen presenting cells, and in particular DC (i) of cytokines that enhance FcyRI expression and induce antigen presenting cell differentiation and maturation; (ii) of ligating CD40; and (iii) on the pathway of antigen presentation in association with MHC class 1; and 3) Using a murine model of human prostate cancer in mice transgenic for human FcyRI, we would examine the effects of targeting prostate antigens to FcyRI alone and in conjunction with immune modulators to determine the requirements for, and mechanisms of, induction of the most robust Th1 and CTL immune response to PSA and to PSMA and the extent to which this targeted vaccine approach is effective.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Exploratory Grants (P20)
Project #
1P20RR016437-01
Application #
6553628
Study Section
Special Emphasis Panel (ZRR1)
Project Start
2001-09-30
Project End
2006-08-31
Budget Start
Budget End
Support Year
1
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
Dartmouth College
Department
Type
DUNS #
041027822
City
Hanover
State
NH
Country
United States
Zip Code
03755

  Publications

Parker, Zachary M; Pasieka, Tracy Jo; Parker, George A et al. (2016) Immune- and Nonimmune-Compartment-Specific Interferon Responses Are Critical Determinants of Herpes Simplex Virus-Induced Generalized Infections and Acute Liver Failure. J Virol 90:10789-10799
Allegrezza, Michael J; Rutkowski, Melanie R; Stephen, Tom L et al. (2016) Trametinib Drives T-cell-Dependent Control of KRAS-Mutated Tumors by Inhibiting Pathological Myelopoiesis. Cancer Res 76:6253-6265
Rosato, Pamela C; Katzenell, Sarah; Pesola, Jean M et al. (2016) Neuronal IFN signaling is dispensable for the establishment of HSV-1 latency. Virology 497:323-327
O'Connor, Megan A; Vella, Jennifer L; Green, William R (2016) Reciprocal relationship of T regulatory cells and monocytic myeloid-derived suppressor cells in LP-BM5 murine retrovirus-induced immunodeficiency. J Gen Virol 97:509-22
Yeager, Mark P; Pioli, Patricia A; Collins, Jane et al. (2016) Glucocorticoids enhance the in vivo migratory response of human monocytes. Brain Behav Immun 54:86-94
Ball, Michael S; Shipman, Emilie P; Kim, Hyunjung et al. (2016) CDDO-Me Redirects Activation of Breast Tumor Associated Macrophages. PLoS One 11:e0149600
Katzenell, Sarah; Leib, David A (2016) Herpes Simplex Virus and Interferon Signaling Induce Novel Autophagic Clusters in Sensory Neurons. J Virol 90:4706-4719
Patankar, Yash R; Mabaera, Rodwell; Berwin, Brent (2015) Differential ASC requirements reveal a key role for neutrophils and a noncanonical IL-1? response to Pseudomonas aeruginosa. Am J Physiol Lung Cell Mol Physiol 309:L902-13
Parker, Zachary M; Murphy, Aisling A; Leib, David A (2015) Role of the DNA Sensor STING in Protection from Lethal Infection following Corneal and Intracerebral Challenge with Herpes Simplex Virus 1. J Virol 89:11080-91
Rosato, Pamela C; Leib, David A (2015) Neuronal Interferon Signaling Is Required for Protection against Herpes Simplex Virus Replication and Pathogenesis. PLoS Pathog 11:e1005028

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