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Convergent Synthesis and Biological Evaluation of 2-Amino-4-(3 ',4 ',5 '-trimethoxyphenyl)-5-aryl Thiazoles as Microtubule Targeting Agents

  1. Author:
    Romagnoli, R.
    Baraldi, P. G.
    Brancale, A.
    Ricci, A.
    Hamel, E.
    Bortolozzi, R.
    Basso, G.
    Viola, G.
  2. Author Address

    [Romagnoli, R; Baraldi, PG] Univ Ferrara, Dipartimento Sci Farmaceut, I-44100 Ferrara, Italy [Brancale, A; Ricci, A] Cardiff Univ, Welsh Sch Pharm, Cardiff CF10 3NB, S Glam, Wales [Hamel, E] NCI, Screening Technol Branch, Dev Therapeut Program, Div Canc Treatment & Diag,NIH, Frederick, MD 21702 USA [Bortolozzi, R; Basso, G; Viola, G] Univ Padua, Dipartimento Pediat, Lab Oncoematol, I-35131 Padua, Italy;Romagnoli, R (reprint author), Univ Ferrara, Dipartimento Sci Farmaceut, I-44100 Ferrara, Italy;rmr@unife.it giampietro.viola1@unipd.it
    1. Year: 2011
    2. Date: Jul
  1. Journal: Journal of Medicinal Chemistry
    1. 54
    2. 14
    3. Pages: 5144-5153
  2. Type of Article: Article
  3. ISSN: 0022-2623
  1. Abstract:

    Combretastatin A-4, a potent tubulin polymerization inhibitor, caused us to synthesize a novel series of 2-amino-4-(3',4',5'-trimethoxyphenyl)-5-aryl thiazoles with the goal of evaluating the effects of substituents on the phenyl at the 5-position of the thiazole skeleton on biological activities. An ethoxy group at the para-position produced the most active compound in the series, with IC(50) values of 0.03-0.9 nM against five of seven cancer cell lines. The most active compounds retained full activity in multidrug resistant cancer cells and acted through the colchicine site of tubulin. Treated cells were arrested in the G2/M phase of the cell cycle, with cell death proceeding through an apoptotic pathway that was only partially caspase-dependent. Preliminary results suggest that, in addition to cell death by apoptosis, cells were also killed via mitotic catastrophe as an alternative cell death mechanism.

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External Sources

  1. DOI: 10.1021/jm200392p
  2. WOS: 000292892300017

Library Notes

  1. Fiscal Year: FY2010-2011
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