Mirror‐Image Packing Provides a Molecular Basis for the Nanomolar Equipotency of Enantiomers of an Experimental Herbicide

نویسندگان

  • Claudine Bisson
  • K Linda Britton
  • Svetlana E Sedelnikova
  • H Fiona Rodgers
  • Thomas C Eadsforth
  • Russell C Viner
  • Tim R Hawkes
  • Patrick J Baker
  • David W Rice
چکیده

Programs of drug discovery generally exploit one enantiomer of a chiral compound for lead development following the principle that enantiomer recognition is central to biological specificity. However, chiral promiscuity has been identified for a number of enzyme families, which have shown that mirror-image packing can enable opposite enantiomers to be accommodated in an enzyme's active site. Reported here is a series of crystallographic studies of complexes between an enzyme and a potent experimental herbicide whose chiral center forms an essential part of the inhibitor pharmacophore. Initial studies with a racemate at 1.85 Å resolution failed to identify the chirality of the bound inhibitor, however, by extending the resolution to 1.1 Å and by analyzing high-resolution complexes with the enantiopure compounds, we determined that both enantiomers make equivalent pseudosymmetric interactions in the active site, thus mimicking an achiral reaction intermediate.

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عنوان ژورنال:

دوره 55  شماره 

صفحات  -

تاریخ انتشار 2016