Towards 20,20-difluorinated bryostatin: synthesis and biological evaluation of C17,C27-fragments

Paul R. Mears, Steven Hoekman, Claire E. Rye, Fiona P. Bailey, Dominic P. Byrne, Patrick A. Eyers, Eric J. Thomas

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    Abstract

    Bryostatins with modified C17–C27 fragments have not been widely studied. The synthesis of 20,20-difluorinated analogues was therefore investigated. Such substitution would inhibit dehydration involving the C19-hydroxyl group and stabilise the ring-closed hemiacetal tautomers. Following preliminary studies, allyldifluorination was used to prepare difluorinated alkenols. Oxidation followed by stereoselective Wittig reactions of the resulting α,α-difluorinated ketones gave (E)-α,β-unsaturated esters that were taken through to complete syntheses of 2-hydroxytetrahydropyrans corresponding to C17–C27 fragments of 20,20-difluorinated bryostatin. These compounds showed modest binding to protein kinase Cα isozyme. Attempts were also undertaken to synthesise macrocyclic 20,20-difluorinated analogues. During preliminary studies, allyldifluorination was carried out using a 2-alkyl-3-bromo-1,1-difluoropropene.
    Original languageEnglish
    Pages (from-to)1487-1505
    JournalOrganic & biomolecular chemistry
    Volume17
    Issue number6
    Early online date16 Jan 2019
    DOIs
    Publication statusPublished - 2019

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