Abstract

This Program Project application combines the different expertise of four collaborating laboratories to perform research on the radiation sensitizing and bioreductive activity in cancer of novel compounds including bifunctional and other nitroheterocyclic agents, fused pyrazine mono-N- oxides and quinonoid analogs of mitomycin C. The four projects which comprise this application and their general objectives are: Project 1. Identification and Evaluation of Bioreductive Drugs. The broad aim of this project is to optimize the selection and development of novel bioreductive drugs that may be used as clinical radiation sensitizers and hypoxia-selective drugs for use in chemotherapy. Project 2. Microenvironments and Effectiveness of Bioreductive Drugs in Spheroids. Multicellular tumor spheroids of human and rodent cell lines will be used to assess structure-activity relationships for cytotoxicity and chemosensitization, and the role of cell microenvironments. Project 3. Efficacy and Mechanisms of Bioreductive Drugs as Chemosensitizing Agents. The central goal of this project is to determine the effectiveness and mechanisms of action of these bioreductive drugs as in vitro and in vivo hypoxic cell cytotoxins or chemopotentiating agents. Project 4. Mechanisms of Oncogenic Transformation by Bioreductive Drugs. The basic aim is to elucidate the mechanisms and factors that determine oncogenicity and provide input to identify the ideal physico-chemical properties of a bioreductive drug. Information provided by the experiments in these four projects will be integrated to guide the development of a new generation of bioreductive drugs for application in the treatment and diagnosis of cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA055165-03
Application #
2096375
Study Section
Special Emphasis Panel (SRC (G2))
Project Start
1992-09-30
Project End
1996-09-29
Budget Start
1994-09-30
Budget End
1995-09-29
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Sri International
Department
Type
DUNS #
City
Menlo Park
State
CA
Country
United States
Zip Code
94025

  Publications

Phillips, R M; Naylor, M A; Jaffar, M et al. (1999) Bioreductive activation of a series of indolequinones by human DT-diaphorase: structure-activity relationships. J Med Chem 42:4071-80
Siemann, D W; Hinchman, C A (1998) Potentiation of cisplatin activity by the bioreductive agent tirapazamine. Radiother Oncol 47:215-20
Jaffar, M; Naylor, M A; Robertson, N et al. (1998) 5-substituted analogues of 3-hydroxymethyl-5-aziridinyl-1-methyl-2-[1H-indole-4,7-dione]prop-2-en- 1-ol (EO9, NSC 382459) and their regioisomers as hypoxia-selective agents: structure-cytotoxicity in vitro. Anticancer Drug Des 13:105-23
Dachs, G U; Patterson, A V; Firth, J D et al. (1997) Targeting gene expression to hypoxic tumor cells. Nat Med 3:515-20
Butler, S A; Wood, P J; Cole, S et al. (1997) Enhancement of bioreductive drug toxicity in murine tumours by inhibition of the activity of nitric oxide synthase. Br J Cancer 76:438-44
Patterson, A V; Saunders, M P; Chinje, E C et al. (1997) Overexpression of human NADPH:cytochrome c (P450) reductase confers enhanced sensitivity to both tirapazamine (SR 4233) and RSU 1069. Br J Cancer 76:1338-47
Naylor, M A; Jaffar, M; Nolan, J et al. (1997) 2-Cyclopropylindoloquinones and their analogues as bioreductively activated antitumor agents: structure-activity in vitro and efficacy in vivo. J Med Chem 40:2335-46
Moody, C J; Roffey, J R; Stephens, M A et al. (1997) Synthesis and cytotoxic activity of indolyl thiazoles. Anticancer Drugs 8:489-99
Siemann, D W (1996) The in situ tumour response to combinations of cyclophosphamide and tirapazamine. Br J Cancer Suppl 27:S65-9
Barham, H M; Inglis, R; Chinje, E C et al. (1996) Development and validation of a spectrophotometric assay for measuring the activity of NADH: cytochrome b5 reductase in human tumour cells. Br J Cancer 74:1188-93

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