Abstract

The long term scientific goal of this proposal is to gain an understanding of the molecular mechanisms which underlie the phenotypic expression of drug resistance. Many cancer patients fail to benefit from potentially effective chemotherapy because their tumors are either intrinsically resistant or acquire resistance following exposure to sub-curative drug concentrations. Nitrogen mustards and nitrosoureas are two classes of bifunctional alkylating agents with distinct mechanisms of action. Both are useful in the clinical management of a number of malignancies, although resistant tumor cells frequently repopulate a tumor following partial response. By using nitrogen mustard resistant rat and human tumor cell lines and by analysing primary human biopsy material, the role of drug detoxification in the expression of the resistant phenotype will be assessed. Glutathione-S-transferase (GST) isoenzymes are important in xenobiotic metabolism and preliminary indications are that both quantitative and qualitative differences exist in nitrogen mustard resistant tumor cells. Because of this, a number of biochemical and molecular studies with GST are planned. These include, (a) glutathione affinity column chromatography purification and full biochemical and immunological characterization of the multiple GST isoenzymes in resistant and sensitive tumor cells. (b) Sub- cellular compartmentalization of GST isoenzymes and the relevance of such distribution to nitrogen mustard metabolism. (c) Synthesis of GST isoenzyme cDNA and subsequent evaluation of transcriptional control under conditions of selective drug exposure. (d) Drug combination studies in vitro and in vivo using pertinent GST inhibitors with nitrogen mustards in an effort to increase tumor cell kill. Such studies should establish if increased GST activity and/or the presence of novel GST isoenzymes are a consequence of specific nitrogen mustard pretreatment or are an overt cellular response to a stress environment. Concomitant to the GST analyses, O6-alkyl guanine transferase (Mer phenotype) and glutathione reductase activity will be assessed in both cell lines and biopsy material to determine the potential link between nitrogen mustard resistance and nitrosourea collateral sensitivity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA043830-05
Application #
3186207
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Project Start
1985-12-01
Project End
1992-03-31
Budget Start
1990-04-01
Budget End
1991-03-31
Support Year
5
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

Clapper, M L; Kuzmich, S; Seestaller, L M et al. (1993) Time course of glutathione S-transferase elevation in Walker mammary carcinoma cells following chlorambucil exposure. Biochem Pharmacol 45:683-90
Kuzmich, S; Vanderveer, L A; Walsh, E S et al. (1992) Increased levels of glutathione S-transferase pi transcript as a mechanism of resistance to ethacrynic acid. Biochem J 281 ( Pt 1):219-24
Clapper, M L; Hoffman, S J; Carp, N et al. (1991) Contribution of patient history to the glutathione S-transferase activity of human lung, breast and colon tissue. Carcinogenesis 12:1957-61
Clapper, M L; Hoffman, S J; Tew, K D (1991) Glutathione S-transferases in normal and malignant human colon tissue. Biochim Biophys Acta 1096:209-16
Morris, D I; Speicher, L A; Ruoho, A E et al. (1991) Interaction of forskolin with the P-glycoprotein multidrug transporter. Biochemistry 30:8371-9
Kuzmich, S; Vanderveer, L A; Tew, K D (1991) Evidence for a glycoconjugate form of glutathione S-transferase pI. Int J Pept Protein Res 37:565-71
Ranganathan, S; Tew, K D (1991) Immunohistochemical localization of glutathione S-transferases alpha, mu, and pi in normal tissue and carcinomas from human colon. Carcinogenesis 12:2383-7
Nakagawa, K; Saijo, N; Tsuchida, S et al. (1990) Glutathione-S-transferase pi as a determinant of drug resistance in transfectant cell lines. J Biol Chem 265:4296-301
Schisselbauer, J C; Silber, R; Papadopoulos, E et al. (1990) Characterization of glutathione S-transferase expression in lymphocytes from chronic lymphocytic leukemia patients. Cancer Res 50:3562-8
Clapper, M L; Tew, K D (1989) Identification of a glutathione S-transferase associated with microsomes of tumor cells resistant to nitrogen mustards. Biochem Pharmacol 38:1915-21

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