Abstract

Taxol and the Vinca alkaloids are highly effective cancer chemotherapeutic drugs. Their primary targets in tumor cells appear to be dynamic spindle microtubules required for proper segregation of chromosomes to the daughter cells at mitosis. Despite considerable knowledge gained recently about how taxol and Vinca alkaloids act to inhibit mitotic progression by suppression of spindle microtubule dynamics, their precise mechanisms of action and the reasons that tumor cells are resistant or sensitive to the drugs are far from understood. It is hypothesized that a) the tubulin isotype composition of the microtubules in tumor cells, the composition of microtubule-associated mitotic regulatory proteins, and mutated forms of tubulin may all be important determinants of sensitivity to antimitotic drugs, and b) that microtubule-targeted antitumor drugs inhibit proliferation of, and kill, tumor cells in several ways, not only by suppressing spindle microtubule dynamics and disrupting mitotic spindle function, but by binding to tubulin components of the centrosomes (spindle poles), which could lead to aberrant spindle function and aberrant cytokinesis. To test these hypotheses, the following experimental aims are proposed: 1) To determine to what extent the beta-tubulin isotype composition, tubulin mutations, and regulatory microtubule-associated proteins (MCAK, stathmin, and survivin) affect the resistance of cells to these drugs. 2) To elucidate the mechanistic relationship between altered expression of mitotic regulatory proteins (using RNAi), suppression of mitotic spindle microtubule and centromere dynamics, inhibition of tumor cell proliferation and cytokinesis, induction of aneuploidy and cell killing by microtubule-targeted drugs, and 3) To elucidate the interactions between microtubule-targeted drugs and centrosomal tubulins and their effects on tumor cell proliferation and killing. The binding of radiolabeled taxol or vinblastine to purified centrosomal tubulins, the effects of antimitotic drugs on the organization of gamma-, delta-, and epsilon-tubulins by light, electron and confocal microscopy of fixed and living cells, on the nucleation of microtubules at centrosomes, and on centriolar migration prior to cytokinesis will be determined. The results will elucidate mechanisms and predict possible clinical efficacy of combination therapies directed at modulating mitotic microtubule regulatory proteins in combination with taxanes and Vinca alkaloids.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA057291-13
Application #
6931095
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Fu, Yali
Project Start
1992-09-18
Project End
2008-06-30
Budget Start
2005-09-01
Budget End
2006-06-30
Support Year
13
Fiscal Year
2005
Total Cost
$310,905
Indirect Cost

  Institution

Name
University of California Santa Barbara
Department
Type
Organized Research Units
DUNS #
094878394
City
Santa Barbara
State
CA
Country
United States
Zip Code
93106

  Publications

Kamath, Kathy; Smiyun, Greg; Wilson, Leslie et al. (2014) Mechanisms of inhibition of endothelial cell migration by taxanes. Cytoskeleton (Hoboken) 71:46-60
Hinow, Peter; Rezania, Vahid; Lopus, Manu et al. (2011) Modeling the effects of drug binding on the dynamic instability of microtubules. Phys Biol 8:056004
Balasubramani, Manimalha; Nakao, Chitose; Uechi, Guy T et al. (2011) Characterization and detection of cellular and proteomic alterations in stable stathmin-overexpressing, taxol-resistant BT549 breast cancer cells using offgel IEF/PAGE difference gel electrophoresis. Mutat Res 722:154-64
Kiris, Erkan; Ventimiglia, Donovan; Sargin, Mehmet E et al. (2011) Combinatorial Tau pseudophosphorylation: markedly different regulatory effects on microtubule assembly and dynamic instability than the sum of the individual parts. J Biol Chem 286:14257-70
Oroudjev, Emin; Lopus, Manu; Wilson, Leslie et al. (2010) Maytansinoid-antibody conjugates induce mitotic arrest by suppressing microtubule dynamic instability. Mol Cancer Ther 9:2700-13
Gan, Pei Pei; McCarroll, Joshua A; Po'uha, Sela T et al. (2010) Microtubule dynamics, mitotic arrest, and apoptosis: drug-induced differential effects of betaIII-tubulin. Mol Cancer Ther 9:1339-48
Lopus, Manu; Oroudjev, Emin; Wilson, Leslie et al. (2010) Maytansine and cellular metabolites of antibody-maytansinoid conjugates strongly suppress microtubule dynamics by binding to microtubules. Mol Cancer Ther 9:2689-99
Smith, Jennifer A; Jordan, Mary Ann (2010) Determination of drug binding to microtubules in vitro. Methods Cell Biol 95:289-99
Smith, Jennifer A; Wilson, Leslie; Azarenko, Olga et al. (2010) Eribulin binds at microtubule ends to a single site on tubulin to suppress dynamic instability. Biochemistry 49:1331-7
Kamath, Kathy; Oroudjev, Emin; Jordan, Mary Ann (2010) Determination of microtubule dynamic instability in living cells. Methods Cell Biol 97:1-14

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