Abstract

The overall goal of the proposed studies in this project is to determine how radioimmunotherapy (RAIT) can be used together with chemotherapy to improve anti-tumor responses of colonic and pancreatic cancer and to establish biological principles that will guide the optimal combined use of these two therapeutic modalities. Studies will be done primarily on three colonic cancer lines (GW-39, LS174T, HT-29) and on one pancreatic line (CaPan-1) that vary in their sensitivity to RAIT and chemotherapy. Studies will be performed on tumors grown s.c., as well as in micrometastatic and orthotopic models. The GW-39 xenograft will be used as both a subcutaneous (sc) model and as an intrapulmonary micrometastatic model. The LS174T and HT-29 lines will be used as both sc and liver metastasis models. The responsiveness to RAIT or to chemotherapy alone of all 3 colonic sc models has already been determined. GW-39 is a good responder to RAIT and a moderate responder to chemotherapy. LS174T is a good responder to RAIT and a poor responder to chemotherapy and HT-29 exhibits a moderate response to each treatment. The well characterized sc xenograft and orthotopic models of CaPan-1 will be used. All four lines have already been used to evaluate antigen (Ag) expression, antibody (MAb) targeting, and growth kinetics in nude mice. Radiolabeled MN-14 anti-carcinoembryonic antigen (CEA) and PAM4 (anti-MUC-1 epitope) will be used for these studies. Chemotherapy will be done with 5-fluorouracil (5-FU) alone for pancreatic cancer and with 5-FU+leucovorin (LV) for colonic tumors. Four major aims will be examined: [1] the optimal approach for using chemotherapy and RAIT together will be examined, [2] the importance of (a) in vitro chemo- and radiosensitivity, and (b) in vivo chemo- and radiosensitivity (intratumor pH and pO2) on tumor responsiveness to chemotherapy and RAIT will be examined, [3] the expression of antigen, intratumor pH and pO2, and targetability and responsiveness of whole tumor that survive either RAIT, chemotherapy or the combination therapy will be determined, and [4] the deposition of antibody or cytotoxic drug as function of vascularization. tumor size and viability will be assessed using video image analysis of colonic and pancreatic xenograft sections, treated with a single cycle or multiple cycles of chemo- or radioantibody therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA054425-08
Application #
6300386
Study Section
Project Start
2000-02-15
Project End
2003-01-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
8
Fiscal Year
2000
Total Cost
$292,374
Indirect Cost

  Institution

Name
Center for Molecular Medicine/Immunology
Department
Type
DUNS #
City
Belleville
State
NJ
Country
United States
Zip Code
07950

  Publications

Cardillo, Thomas M; Karacay, Habibe; Goldenberg, David M et al. (2004) Improved targeting of pancreatic cancer: experimental studies of a new bispecific antibody, pretargeting enhancement system for immunoscintigraphy. Clin Cancer Res 10:3552-61
Gold, David V; Modrak, David E; Schutsky, Keith et al. (2004) Combined 90Yttrium-DOTA-labeled PAM4 antibody radioimmunotherapy and gemcitabine radiosensitization for the treatment of a human pancreatic cancer xenograft. Int J Cancer 109:618-26
Gold, David V; Schutsky, Keith; Modrak, David et al. (2003) Low-dose radioimmunotherapy ((90)Y-PAM4) combined with gemcitabine for the treatment of experimental pancreatic cancer. Clin Cancer Res 9:3929S-37S
Reddy, P K; Gold, D V; Cardillo, T M et al. (2003) Interferon-gamma upregulates MUC1 expression in haematopoietic and epithelial cancer cell lines, an effect associated with MUC1 mRNA induction. Eur J Cancer 39:397-404
Cardillo, Thomas M; Blumenthal, Rosalyn; Ying, Zhiliang et al. (2002) Combined gemcitabine and radioimmunotherapy for the treatment of pancreatic cancer. Int J Cancer 97:386-92
Hajjar, George; Sharkey, Robert M; Burton, Jack et al. (2002) Phase I radioimmunotherapy trial with iodine-131--labeled humanized MN-14 anti-carcinoembryonic antigen monoclonal antibody in patients with metastatic gastrointestinal and colorectal cancer. Clin Colorectal Cancer 2:31-42
Modrak, David E; Rodriguez, Marisol D; Goldenberg, David M et al. (2002) Sphingomyelin enhances chemotherapy efficacy and increases apoptosis in human colonic tumor xenografts. Int J Oncol 20:379-84
O'Hara, J A; Blumenthal, R D; Grinberg, O Y et al. (2001) Response to radioimmunotherapy correlates with tumor pO2 measured by EPR oximetry in human tumor xenografts. Radiat Res 155:466-73
Gold, D V; Cardillo, T M (2001) Monoclonal antibody G47 engineered to be reactive with colorectal tumor mucin. Hybrid Hybridomics 20:343-50
Gold, D V; Cardillo, T; Goldenberg, D M et al. (2001) Localization of pancreatic cancer with radiolabeled monoclonal antibody PAM4. Crit Rev Oncol Hematol 39:147-54

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