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Synthesis of Epothilones a and B in Solid and Solution Phase

  1. Author:
    Nicolaou, K. C.
    Winssinger, N.
    Pastor, J.
    Ninkovic, S.
    Sarabia, F.
    He, Y.
    Vourloumis, D.
    Yang, Z.
    Li, T.
    Giannakakou, P.
    Hamel, E.
  2. Author Address

    Nicolaou KC SCRIPPS CLIN & RES INST DEPT CHEM 10550 N TORREY PINES RD LA JOLLA, CA 92037 USA SCRIPPS CLIN & RES INST SKAGGS INST CHEM BIOL LA JOLLA, CA 92037 USA UNIV CALIF SAN DIEGO DEPT CHEM & BIOCHEM LA JOLLA, CA 92093 USA NCI MED BRANCH DCS NIH BETHESDA, MD 20892 USA NCI LAB DRUG DISCOVERY RES & DEV DEV THERAPEUT PROGRAM DCTDC FREDERICK CANC RES & DEV CTR FREDERICK, MD 21702 USA
    1. Year: 1997
  1. Journal: Nature
    1. 387
    2. 6630
    3. Pages: 268-272
  2. Type of Article: Article
  1. Abstract:

    Epothilones A and B, two compounds that have been recently isolated(1) from myxobacterium Sorangium cellulosum strain 90, have generated intense interest(2-16) among chemists, biologists and clinicians erring to the structural complexity, unusual mechanism of interaction with microtubules and anticancer potential of these molecules. Like taxol* (refs 17, 18), they exhibit cytotoxicity against tumour cells by inducing microtubule assembly and stabilization(3,4), even in taxol-resistant cell lines. Following the structural elucidation of these molecules by X-ray crystallography in 1996(1), several syntheses of epothilones A (refs 12-16) and B (ref. 19) have been reported, indicative of the potential importance of these molecules in the cancer field. Here we report the first solid-phase synthesis of epothilone A, the total synthesis of epothilone B, and the generation of a small epothilone library. The solid-phase synthesis applied here to epothilone A could open up new possibilities in natural-product synthesis and, together with solution-phase synthesis of other epothilones, paves the way for the generation of large combinatorial libraries of these important molecules for biological screening. [References: 33]

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