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Discovery of a novel antitumor benzolactone enamide class that selectively inhibits mammalian vacuolar-type (H+)-ATPases

  1. Author:
    Boyd, M. R.
    Farina, C.
    Belfiore, P.
    Gagliardi, S.
    Kim, J. W.
    Hayakawa, Y.
    Beutler, J. A.
    McKee, T. C.
    Bowman, B. J.
    Bowman, E. J.

  2. Author Address

    NCI, Frederick Canc Res & Dev Ctr, Lab Nat Prod, Div Basic Sci, Bldg 1052, Rm 121, Frederick, MD 21702 USA. NCI, Frederick Canc Res & Dev Ctr, Lab Nat Prod, Div Basic Sci, Frederick, MD 21702 USA. SmithKline Beecham SpA, Milan, Italy. Univ Tokyo, Inst Mol & Cellular Biosci, Bunkyo Ku, Tokyo, Japan. SAIC Frederick, Frederick, MD USA. Univ Calif Santa Cruz, Dept Biol, Santa Cruz, CA 95064 USA. Boyd MR NCI, Frederick Canc Res & Dev Ctr, Lab Nat Prod, Div Basic Sci, Bldg 1052, Rm 121, Frederick, MD 21702 USA.
    1. Year: 2001
  2. Journal: Journal of Pharmacology and Experimental Therapeutics
    1. 297
    2. 1
    3. Pages: 114-120
  4. Type of Article: Article
  1. Abstract:

    A series of naturally occurring compounds reported recently by multiple laboratories defines a new small-molecule class sharing a unique benzolactone enamide core structure and diverse biological actions, including inhibition of growth of tumor cells and oncogene-transformed cell lines. Here we show that representative members of this class, including salicylihalamide A, lobatamides A-F, and oximidines I and II inhibit mammalian vacuolar-type (H+)-ATPases (V-ATPases) with unprecedented selectivity. Data derived from the NCl 60-cell antitumor screen critically predicted the V-ATPase molecular target, while specific biochemical assays provided confirmation and further illumination. The compounds potently blocked representative V-ATPases from human kidney, liver, and osteoclastic giant-cell tumor of bone but were essentially inactive against V-ATPases of Neurospora crassa and Saccharomyces cerevisiae and other membrane ATPases. Essential regulation of pH in cytoplasmic, intraorganellar, and local extracellular spaces is provided by V-ATPases, which are ubiquitously distributed among eukaryotic cells and tissues. The most potent and selective V-ATPase inhibitors heretofore known were the bafilomycins and concanamycins, which do not discriminate between mammalian and nonmammalian V-ATPases. Numerous physiological processes are mediated by V-ATPases, and aberrant V-ATPase functions are implicated in many different human diseases. Previous efforts to develop therapeutic pharmacological modulators of V-ATPases have been frustrated by a lack of synthetically tractable and biologically selective leads. Therefore, availability of the unique benzolactone enamide inhibitor class may enable further elucidation of functional and architectural features of mammalian versus nonmammalian V-ATPase isoforms and provide new opportunities for targeting V-ATPase-mediated processes implicated in diverse pathophysiological phenomena, including cancer.

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