Abstract

The long-term objectives of our research are to acquire a thorough understanding of the mechanisms of action and of resistance to Taxol, an antitumor agent that is known to be efficacious in the treatment of human cancer. An intense interest in drug development is now concentrated on the epothilones and discodermolide, natural products whose chemical structures are distinct from Taxol but whose mechanisms of action and resistance have similarities, but are definitely not identical, to those of Taxol. Our plan is to dissect the similarities and differences between these three microtubule stabilizing drugs. The epothilones and/or discodermolide may have superior clinical activity compared to Taxol, particularly in tumors resistant to taxanes. An overriding theme of this grant application is the role that low doses of Taxol, the epothilones and discodermolide play in the killing of cancer cells. This emphasis on low drug dosage is a new focus for our laboratory that developed as it became clear that Taxol was responsible for cell death at low doses of drug that did not block cells in mitosis. There are undoubtedly diverse pathways by which low doses of Taxol kill cancer cells. The availability of preclinical data is essential and must contribute to the decision to move drugs into clinical trials.
The specific aims of this proposal are to: 1. Determine the mechanism(s) by which cells treated with low concentrations of Taxol escape the spindle checkpoint. HeLa cells will be transfected with MAD2, a checkpoint component, to determine if its overexpression can rescue from cell death, those cells that escape from the mitotic checkpoint. The relationship between overexpression of the protein CENP-E, a component of the mitotic checkpoint, and drug resistance will also be investigated. 2. Examine the contribution of p53-dependent apoptosis to cytotoxicity caused by low concentrations of Taxol. Determine if aberrant mitosis leads to p53-dependent apoptosis. DNA microarrays will be used to survey and compare gene expression profiles of A549 cells treated with different concentrations of microtubule stabilizing drugs. 3. Investigate how the expression level and the phosphorylation status of the microtubule regulatory proteins stathmin and MAP4 in cancer cells relate to differential sensitivity to microtubule-stabilizing agents, and how these agents affect the expression profile of these proteins.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA083185-05
Application #
6619166
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Fu, Yali
Project Start
1999-07-06
Project End
2007-04-30
Budget Start
2003-05-23
Budget End
2004-04-30
Support Year
5
Fiscal Year
2003
Total Cost
$370,690
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Pharmacology
Type
Schools of Medicine
DUNS #
071036636
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Wang, Yihong; Sparano, Joseph A; Fineberg, Susan et al. (2013) High expression of class III ?-tubulin predicts good response to neoadjuvant taxane and doxorubicin/cyclophosphamide-based chemotherapy in estrogen receptor-negative breast cancer. Clin Breast Cancer 13:103-8
Xiao, Hui; Wang, Hui; Zhang, Xuechun et al. (2012) Structural evidence for cooperative microtubule stabilization by Taxol and the endogenous dynamics regulator MAP4. ACS Chem Biol 7:744-52
Yang, Chia-Ping Huang; Liu, Lingling; Ikui, Amy E et al. (2010) The interaction between mitotic checkpoint proteins, CENP-E and BubR1, is diminished in epothilone B-resistant A549 cells. Cell Cycle 9:1207-13
Devred, Francois; Tsvetkov, Philipp O; Barbier, Pascale et al. (2008) Stathmin/Op18 is a novel mediator of vinblastine activity. FEBS Lett 582:2484-8
Sun, Liang; Geng, Xudong; Geney, Raphael et al. (2008) Design, synthesis, and biological evaluation of novel C14-C3'BzN-linked macrocyclic taxoids. J Org Chem 73:9584-93
Ojima, Iwao; Chen, Jin; Sun, Liang et al. (2008) Design, synthesis, and biological evaluation of new-generation taxoids. J Med Chem 51:3203-21
Legrier, Marie-Emmanuelle; Yang, Chia-Ping Huang; Yan, Han-Guang et al. (2007) Targeting protein translation in human non small cell lung cancer via combined MEK and mammalian target of rapamycin suppression. Cancer Res 67:11300-8
Wiesen, Kenneth M; Xia, Shujun; Yang, Chia-Ping Huang et al. (2007) Wild-type class I beta-tubulin sensitizes Taxol-resistant breast adenocarcinoma cells harboring a beta-tubulin mutation. Cancer Lett 257:227-35
Huang, Gloria S; Lopez-Barcons, Lluis; Freeze, B Scott et al. (2006) Potentiation of taxol efficacy and by discodermolide in ovarian carcinoma xenograft-bearing mice. Clin Cancer Res 12:298-304
Xiao, Hui; Verdier-Pinard, Pascal; Fernandez-Fuentes, Narcis et al. (2006) Insights into the mechanism of microtubule stabilization by Taxol. Proc Natl Acad Sci U S A 103:10166-73

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