• Title of article

    α-Substituted norstatines as the transition-state mimic in inhibitors of multiple digestive vacuole malaria aspartic proteases Original Research Article

  • Author/Authors

    Kristina M. Orrling، نويسنده , , Melissa R. Marzahn، نويسنده , , Hugo Gutiérrez-de-Ter?n، نويسنده , , Johan ?qvist، نويسنده , , Ben M. Dunn، نويسنده , , Mats Larhed، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2009
  • Pages
    17
  • From page
    5933
  • To page
    5949
  • Abstract
    The impact of moving the P1 side-chain from the β-position to the α-position in norstatine-containing plasmepsin inhibitors was investigated, generating two new classes of tertiary alcohol-comprising α-benzylnorstatines and α-phenylnorstatines. Twelve α-substituted norstatines were designed, synthesized and evaluated for their inhibitory potencies against plasmepsin II and the plasmepsin IV orthologues (PM4) present in the digestive vacuole of all four Plasmodium species causing malaria in man. New synthetic routes were developed for producing the desired α-substituted norstatines as pure stereoisomers. The best compounds provided Ki values in the nanomolar range for all PM4, with a best value of 110 nM in PM4 from Plasmodium ovale. In addition, excellent selectivity over the closely related human aspartic protease Cathepsin D was achieved. The loss of affinity to Plasmodium falciparum PM4, which was experienced upon the move of the P1 substituent, was rationalized by the calculation of inhibitor–protein binding affinities using the linear interaction energy method (LIE).
  • Keywords
    Plasmepsin , Inhibitors , Microwave-assisted synthesis , Linear interaction energy mehtod , molecular dynamics , malaria
  • Journal title
    Bioorganic and Medicinal Chemistry
  • Serial Year
    2009
  • Journal title
    Bioorganic and Medicinal Chemistry
  • Record number

    1306261