PLoS Neglected Tropical Diseases (Jan 2015)

Structural and Functional Characterization of the Enantiomers of the Antischistosomal Drug Oxamniquine.

  • Alexander B Taylor,
  • Livia Pica-Mattoccia,
  • Chiara M Polcaro,
  • Enrica Donati,
  • Xiaohang Cao,
  • Annalisa Basso,
  • Alessandra Guidi,
  • Anastasia R Rugel,
  • Stephen P Holloway,
  • Timothy J C Anderson,
  • P John Hart,
  • Donato Cioli,
  • Philip T LoVerde

DOI
https://doi.org/10.1371/journal.pntd.0004132
Journal volume & issue
Vol. 9, no. 10
p. e0004132

Abstract

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For over two decades, a racemic mixture of oxamniquine (OXA) was administered to patients infected by Schistosoma mansoni, but whether one or both enantiomers exert antischistosomal activity was unknown. Recently, a ~30 kDa S. mansoni sulfotransferase (SmSULT) was identified as the target of OXA action.Here, we separate the OXA enantiomers using chromatographic methods and assign their optical activities as dextrorotary [(+)-OXA] or levorotary [(-)-OXA]. Crystal structures of the parasite enzyme in complex with optically pure (+)-OXA and (-)-OXA) reveal their absolute configurations as S- and R-, respectively. When tested in vitro, S-OXA demonstrated the bulk of schistosomicidal activity, while R-OXA had antischistosomal effects when present at relatively high concentrations. Crystal structures R-OXA•SmSULT and S-OXA•SmSULT complexes reveal similarities in the modes of OXA binding, but only the S-OXA enantiomer is observed in the structure of the enzyme exposed to racemic OXA.Together the data suggest the higher schistosomicidal activity of S-OXA is correlated with its ability to outcompete R-OXA binding the sulfotransferase active site. These findings have important implications for the design, syntheses, and dosing of new OXA-based antischistosomal compounds.