Abstract

The long term scientific goal of this proposal is to gain an understanding of how the nitroimidazole sensitizers may enhance the activity of anticancer drugs, and to apply that knowledge in designing novel regimens for the treatment of resistant tumors. Most solid tumors have a significant proportion of hypoxic cells, a consequence of abnormal vascular development in malignant tissue. Hypoxic cells are resistant to both radiation and to chemotherapeutic drugs, especially alkylating agents. A group of xenobiotic-scavenging enzymes, the glutathione-S-transferases (GST's) are expressed at higher levels in cells exposed to hypoxia. 2- Nitroimidazoles have been identified as a class of compounds which in vitro and in vivo restore the sensitivity of hypoxic cells to both radiation and chemotherapy. OF the congeners evaluated to date, SR2508 has the highest therapeutic index of this class of drugs. We hypothesize that the sensitizing action of SR2508 is closely related to its inhibition of GST's and depletion of glutathione. To test these hypotheses, in preclinical models, we will (a) characterize the kinetics of inhibition by SR2508 of GST's using purified enzyme in vitro, and whole cells in culture, under both oxic and hypoxic conditions; (b) define the dose-response and time- course of GST inhibition and glutathione (GSH) depletion by SR2508 in tumors and normal tissues of tumor bearing scid mice; (c) detect and quantify glutathione adducts of SR2508 in tumor and normal tissues. In a series of clinical trials. Ultimately leading to a definitive test of chemosensitization by SR2508, we plan to (a) define the dose and schedule of SR2508 for use in combination with cyclophosphamide at standard doses; (b) describe the combination of SR2508 and cyclophosphamide at high alkylating agent doses in association with autologous bone marrow transplantation. The results of these studies will, it is hoped, clarify aspects of the cellular action of SR2508, and indicate how clinical regimens should be designed to maximize their potential role in therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA049820-01A2
Application #
3194116
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Project Start
1990-06-20
Project End
1993-05-31
Budget Start
1990-06-20
Budget End
1991-05-31
Support Year
1
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Fox Chase Cancer Center
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19111

  Publications

Selvakumaran, Muthu; Amaravadi, Ravi K; Vasilevskaya, Irina A et al. (2013) Autophagy inhibition sensitizes colon cancer cells to antiangiogenic and cytotoxic therapy. Clin Cancer Res 19:2995-3007
Selvakumaran, Muthu; Yao, Kang Shen; Feldman, Michael D et al. (2008) Antitumor effect of the angiogenesis inhibitor bevacizumab is dependent on susceptibility of tumors to hypoxia-induced apoptosis. Biochem Pharmacol 75:627-38
Vasilevskaya, Irina A; Selvakumaran, Muthu; O'Dwyer, Peter J (2008) Disruption of signaling through SEK1 and MKK7 yields differential responses in hypoxic colon cancer cells treated with oxaliplatin. Mol Pharmacol 74:246-54
Rakitina, Tatiana V; Vasilevskaya, Irina A; O'Dwyer, Peter J (2007) Inhibition of G1/S transition potentiates oxaliplatin-induced cell death in colon cancer cell lines. Biochem Pharmacol 73:1715-26
Yao, Kangshen; Shida, Seiichiro; Selvakumaran, Muthu et al. (2005) Macrophage migration inhibitory factor is a determinant of hypoxia-induced apoptosis in colon cancer cell lines. Clin Cancer Res 11:7264-72
Yao, K; Gietema, J A; Shida, S et al. (2005) In vitro hypoxia-conditioned colon cancer cell lines derived from HCT116 and HT29 exhibit altered apoptosis susceptibility and a more angiogenic profile in vivo. Br J Cancer 93:1356-63
Vasilevskaya, Irina A; O'Dwyer, Peter J (2005) 17-Allylamino-17-demethoxygeldanamycin overcomes TRAIL resistance in colon cancer cell lines. Biochem Pharmacol 70:580-9
Vasilevskaya, Irina A; Rakitina, Tatiana V; O'Dwyer, Peter J (2004) Quantitative effects on c-Jun N-terminal protein kinase signaling determine synergistic interaction of cisplatin and 17-allylamino-17-demethoxygeldanamycin in colon cancer cell lines. Mol Pharmacol 65:235-43
Vasilevskaya, Irina A; Rakitina, Tatiana V; O'Dwyer, Peter J (2003) Geldanamycin and its 17-allylamino-17-demethoxy analogue antagonize the action of Cisplatin in human colon adenocarcinoma cells: differential caspase activation as a basis for interaction. Cancer Res 63:3241-6
Rakitina, Tatiana V; Vasilevskaya, Irina A; O'Dwyer, Peter J (2003) Additive interaction of oxaliplatin and 17-allylamino-17-demethoxygeldanamycin in colon cancer cell lines results from inhibition of nuclear factor kappaB signaling. Cancer Res 63:8600-5

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