Abstract

The work described in this collaborative research proposal has as its primary aim the development of an understanding of the interaction of the important anticancer drug paclitaxel (Taxol) and the promising anticancer drug epothilone B with their common microtubule receptor, and to use the information derived from this study in the design and development of improved analogs of paclitaxel and possible also epothilone B. The interaction of paxlitaxel and tubulin is believed to be crucial to the anticancer activities of the drugs, and thus knowledge of the details of this interaction will facilitate the design and development of improved analogs. The approach adopted will be to prepare paclitaxel and epothilone B analogs of Virginia Polytechnic Institute and State University that are labeled either with a fluorescent probe or with a stable isotope labeled probe. The fluorescent probes will be used at the State University of New York at Binghamton to elucidate the nature of the paclitaxel-tubulin and epothilone-tubulin interaction through fluorescence spectroscopy, leading to information about the dielectric nature of the fluorophore environment, the fluorophore's accessibility to solvent and the size, shape, and associative behavior of the tubulin macromolecule. The relative orientations of the drugs within the receptor site will be deduced from fluorescence resonance energy transfer measurements. The stable isotope labeled analogs will be analyzed in solid state NMR experiments at Washington University using sophisticated phasing experiments such as double-REDOR NMR to obtain information on key internuclear distances of paclitaxel and of epothilone B bound to microtubules. The information derived from both approaches will be combined with molecular modeling information at SUNY Binghamton to develop a model for the conformation of paclitaxel in the binding site of polymerized tubulin. In addition, the best available information on the likely three-dimensional structure of tubulin will be combined with the paclitaxel model into a combined model for the nature of binding site. These models will then be used as the basis for synthetic efforts designed to prepare analogs that are conformationally restricted so as to mimic the active site conformation. Such analogs are expected to show improved bioactivity as compared with paclitaxel itself. In addition, new analogs of paclitaxel will be prepared by combinatorial chemical methods.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA069571-07
Application #
6512803
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Program Officer
Fu, Yali
Project Start
1996-08-01
Project End
2004-05-31
Budget Start
2002-06-01
Budget End
2003-05-31
Support Year
7
Fiscal Year
2002
Total Cost
$264,693
Indirect Cost

  Institution

Name
Virginia Polytechnic Institute and State University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
003137015
City
Blacksburg
State
VA
Country
United States
Zip Code
24061

  Publications

Ganesh, Thota; Brodie, Peggy J; Banerjee, Abhijit et al. (2014) Synthesis of isotopically labeled epothilones. J Labelled Comp Radiopharm 57:78-81
Kingston, David G I; Snyder, James P (2014) The quest for a simple bioactive analog of paclitaxel as a potential anticancer agent. Acc Chem Res 47:2682-91
Sharma, Shubhada; Lagisetti, Chandraiah; Poliks, Barbara et al. (2013) Dissecting paclitaxel-microtubule association: quantitative assessment of the 2'-OH group. Biochemistry 52:2328-36
Kingston, David G I; Tamarkin, Lawrence; Paciotti, Giulio F (2012) Conformationally Constrained and Nanoparticle Targeted Paclitaxels. Pure Appl Chem 84:1455-1467
Zhan, Weiqiang; Jiang, Yi; Sharma, Shubhada et al. (2011) C6-C8 bridged epothilones: consequences of installing a conformational lock at the edge of the macrocycle. Chemistry 17:14792-804
Zhao, Jielu; Bane, Susan; Snyder, James P et al. (2011) Design and synthesis of simplified taxol analogs based on the T-Taxol bioactive conformation. Bioorg Med Chem 19:7664-78
Dilek, Ozlem; Bane, Susan L (2011) Synthesis and spectroscopic characterization of fluorescent boron dipyrromethene-derived hydrazones. J Fluoresc 21:347-54
Qi, Jun; Blanden, Adam R; Bane, Susan et al. (2011) Design, synthesis and biological evaluation of a simplified fluorescently labeled discodermolide as a molecular probe to study the binding of discodermolide to tubulin. Bioorg Med Chem 19:5247-54
Shanker, Natasha; Dilek, Ozlem; Mukherjee, Kamalika et al. (2011) Aurones: small molecule visible range fluorescent probes suitable for biomacromolecules. J Fluoresc 21:2173-84
Banerjee, Abhijit; Bovenzi, Frank A; Bane, Susan L (2010) High-resolution separation of tubulin monomers on polyacrylamide minigels. Anal Biochem 402:194-6

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