Abstract

Multiple drug resistance (MDR) refers to the fact that tumor cells can display a broad cross-resistance to a variety of """"""""natural product"""""""" compounds of widely differing structure and mechanism of action. One type of MDR (Pgp-MDR) has been characterized by decreased drug accumulation and overexpression of the gene coding for a large membrane glycoprotein, termed, Pgp. We have developed progressively-VM-26-resistant human leukemic cell lines (CEM/Vm-1 and CEM/VM-1-5) with an """"""""atypical"""""""" pattern of cross-resistance and cellular pharmacology. These cells retain sensitivity to the Vinca alkaloids, are not impaired in their transport of drugs, and do not overexpress the pgp gene. There is now considerable evidence that """"""""atypical-MDR"""""""" (at-MDR) is due to an alteration in the activity of the essential nuclear enzyme, topoisomerase II, an unique and important target for many anticancer agents. Whether this alteration is a consequence of a mutation in the gene coding for topoisomerase II or in a gene that modulates it is not clear. The long-term objective of the proposed work is to determine the molecular basis of at-MDR. To accomplish this goal, five specific aims will be addressed.
The first aim i s to purify and characterize the topoisomerase II protein from at-MDR cells.
A second aim i s to characterize the topoisomerase II mRNA and its regulation in the at-MDR cells using a topoisomerase II-specific nucleotide probe.
The third aim i s to identify specific mutations in the at-MDR topoisomerase II mRNA using nuclease mapping techniques and cDNA sequence determinations.
The fourth aim i s to confirm that any identified alterations in the at-MDR topoisomerase II are indeed responsible for the expression of the at-MDR phenotype. Finally, if the topoisomerase II mRNA and enzyme is unaltered in the resistant cells, the fifth aim is to characterize by biochemical and molecular procedures the nature of the altered modulator of topoisomerase II. Characterization of mutations in the at-MDR cells that are responsible for the alterations in topoisomerase II activity will yield information about the interaction of clinically important drugs with the critical enzyme, may provide information pertinent to the mechanism of action of topoisomerase II, and may provide insights into the design of new drugs and therapeutic modalities to overcome this form of resistance.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA047941-03
Application #
3191769
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Project Start
1989-04-10
Project End
1992-03-31
Budget Start
1991-04-01
Budget End
1992-03-31
Support Year
3
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
St. Jude Children's Research Hospital
Department
Type
DUNS #
067717892
City
Memphis
State
TN
Country
United States
Zip Code
38105

  Publications

Joshi, Ashish A; Wu, Zhong; Reed, Robin F et al. (2003) Nuclear factor-Y binding to the topoisomerase IIalpha promoter is inhibited by both the p53 tumor suppressor and anticancer drugs. Mol Pharmacol 63:359-67
Lothstein, L; Suttle, D P; Roaten, J B et al. (2000) Catalytic inhibition of DNA topoisomerase II by N-benzyladriamycin (AD 288). Biochem Pharmacol 60:1621-8
Chen, G; Templeton, D; Suttle, D P et al. (1999) Ras stimulates DNA topoisomerase II alpha through MEK: a link between oncogenic signaling and a therapeutic target. Oncogene 18:7149-60
Wang, Q; Zambetti, G P; Suttle, D P (1997) Inhibition of DNA topoisomerase II alpha gene expression by the p53 tumor suppressor. Mol Cell Biol 17:389-97
Beck, W T; Danks, M K; Wolverton, J S et al. (1994) Resistance of mammalian tumor cells to inhibitors of DNA topoisomerase II. Adv Pharmacol 29B:145-69
Beck, W T; Danks, M K; Wolverton, J S et al. (1993) Altered DNA topoisomerase II in multidrug resistance. Cytotechnology 11:115-9
Danks, M K; Warmoth, M R; Friche, E et al. (1993) Single-strand conformational polymorphism analysis of the M(r) 170,000 isozyme of DNA topoisomerase II in human tumor cells. Cancer Res 53:1373-9
Bugg, B Y; Danks, M K; Beck, W T et al. (1991) Expression of a mutant DNA topoisomerase II in CCRF-CEM human leukemic cells selected for resistance to teniposide. Proc Natl Acad Sci U S A 88:7654-8
Friche, E; Danks, M K; Schmidt, C A et al. (1991) Decreased DNA topoisomerase II in daunorubicin-resistant Ehrlich ascites tumor cells. Cancer Res 51:4213-8
Beck, W T; Danks, M K (1991) Mechanisms of resistance to drugs that inhibit DNA topoisomerases. Semin Cancer Biol 2:235-44

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