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  • Discovery of HDAC inhibitors with potent activity against multiple malaria parasite life cycle stages

    Author(s)
    Hansen, Finn K
    Sumanadasa, Subathdrage DM
    Stenzel, Katharina
    Duffy, Sandra
    Meister, Stephan
    Marek, Linda
    Schmetter, Rebekka
    Kuna, Krystina
    Hamacher, Alexandra
    Mordmueller, Benjamin
    Kassack, Matthias U
    Winzeler, Elizabeth A
    Avery, Vicky M
    Andrews, Katherine T
    Kurz, Thomas
    Griffith University Author(s)
    Andrews, Katherine T.
    Duffy, Sandra
    Avery, Vicky M.
    Year published
    2014
    Metadata
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    Abstract
    In this work we investigated the antiplasmodial activity of a series of HDAC inhibitors containing an alkoxyamide connecting-unit linker region. HDAC inhibitor 1a (LMK235), previously shown to be a novel and specific inhibitor of human HDAC4 and 5, was used as a starting point to rapidly construct a mini-library of HDAC inhibitors using a straightforward solid-phase supported synthesis. Several of these novel HDAC inhibitors were found to have potent in vitro activity against asexual stage Plasmodium falciparum malaria parasites. Representative compounds were shown to hyperacetylate P. falciparum histones and to inhibit ...
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    In this work we investigated the antiplasmodial activity of a series of HDAC inhibitors containing an alkoxyamide connecting-unit linker region. HDAC inhibitor 1a (LMK235), previously shown to be a novel and specific inhibitor of human HDAC4 and 5, was used as a starting point to rapidly construct a mini-library of HDAC inhibitors using a straightforward solid-phase supported synthesis. Several of these novel HDAC inhibitors were found to have potent in vitro activity against asexual stage Plasmodium falciparum malaria parasites. Representative compounds were shown to hyperacetylate P. falciparum histones and to inhibit deacetylase activity of recombinant PfHDAC1 and P. falciparum nuclear extracts. All compounds were also screened in vitro for activity against Plasmodium berghei exo-erythrocytic stages and selected compounds were further tested against late stage (IV and V) P. falciparum gametocytes. Of note, some compounds showed nanomolar activity against all three life cycle stages tested (asexual, exo-erythrocytic and gametocyte stages) and several compounds displayed significantly increased parasite selectivity compared to the reference HDAC inhibitor suberoylanilide hydroxamic acid (SAHA). These data suggest that it may be possible to develop HDAC inhibitors that target multiple malaria parasite life cycle stages.
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    Journal Title
    European Journal of Medicinal Chemistry
    Volume
    82
    DOI
    https://doi.org/10.1016/j.ejmech.2014.05.050
    Subject
    Medicinal and biomolecular chemistry
    Medicinal and biomolecular chemistry not elsewhere classified
    Organic chemistry
    Pharmacology and pharmaceutical sciences
    Publication URI
    http://hdl.handle.net/10072/63967
    Collection
    • Journal articles

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