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Arylthioindole inhibitors of tubulin polymerization. 3. Biological evaluation, structure-activity relationships and molecular modeling studies

  1. Author:
    La Regina, G.
    Edler, M. C.
    Brancale, A.
    Kandil, S.
    Coluccia, A.
    Piscitelli, F.
    Hamel, E.
    De Martino, G.
    Matesanz, R.
    Diaz, J. F.
    Scovassi, A. I.
    Prosperi, E.
    Lavecchia, A.
    Novellino, E.
    Artico, M.
    Silvestri, R.

  2. Author Address

    Univ Rome, Dipartimento Studi Farmaceut, Fdn Cenci Bolognetti, Ist Pasteur, I-00185 Rome, Italy. Univ Cardiff Wales, Sch Pharm, Cardiff CF10 3XF, Wales. NIH, Natl Canc Inst, Div Canc Treatment & Diagnosis, Frederick, MD 21702 USA. Univ Naples Federico 2, Dipartimento Chim Farmaceut & Tossicol, I-80131 Naples, Italy. Consejo Nazl Ric, Ctr Invest Biol, E-28040 Madrid, Spain. CNR, Ist Genet Mol, I-27100 Pavia, Italy.;Silvestri, R, Univ Rome, Dipartimento Studi Farmaceut, Fdn Cenci Bolognetti, Ist Pasteur, Piazzale Aldo Moro 5, I-00185 Rome, Italy.;romano.silvestri@uniroma1.it
    1. Year: 2007
    2. Date: Jun
  2. Journal: Journal of Medicinal Chemistry
    1. 50
    2. 12
    3. Pages: 2865-2874
  4. Type of Article: Article
  5. ISSN: 0022-2623
  1. Abstract:

    The new arylthioindole (ATI) derivatives 10, 14-18, and 21-24, which bear a halogen atom or a small size ether group at position 5 of the indole moiety, were compared with the reference compounds colchicine and combretastatin A-4 for biological activity. Derivatives 10, 11, 16, and 21-24 inhibited MCF-7 cell growth with IC50 values < 50 nM. A halogen atom (14-17) at position 5 caused a significant reduction in the free energy of binding of compound to tubulin, with a concomitant reduction in cytotoxicity. In contrast, methyl (21) and methoxy (22) substituents at position 5 caused an increase in cytotoxicity. Compound 16, the most potent antitubulin agent, led to a large increase (56%) in HeLa cells in the G(2)/M phase at 24 h, and at 48 h, 26% of the cells were hyperploid. Molecular modeling studies showed that, despite the absence of the ester moiety present in the previously examined analogues, most of the compounds bind in the colchicine site in the same orientation as the previously studied ATIs. Binding to beta-tubulin involved formation of a hydrogen bond between the indole and Thr179 and positioning of the trimethoxy phenyl group in a hydrophobic pocket near Cys241.

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  2. DOI: 10.1021/jm061479u
  3. View record in Web of ScienceĀ®
  4. WOS: 000247033900011

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