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  • Novel prostaglandin D synthase inhibitors generated by fragment-based drug design.

Novel prostaglandin D synthase inhibitors generated by fragment-based drug design.

Journal of medicinal chemistry (2008-03-18)
Morten Hohwy, Loredana Spadola, Britta Lundquist, Paul Hawtin, Jan Dahmén, Ib Groth-Clausen, Ewa Nilsson, Sofia Persdotter, Karin von Wachenfeldt, Rutger H A Folmer, Karl Edman
ABSTRACT

We describe the discovery of novel inhibitors of prostaglandin D2 synthase (PGDS) through fragment-based lead generation and structure-based drug design. A library of 2500 low-molecular-weight compounds was screened using 2D nuclear magnetic resonance (NMR), leading to the identification of 24 primary hits. Structure determination of protein-ligand complexes with the hits enabled a hit optimization process, whereby we harvested increasingly more potent inhibitors out of our corporate compound collection. Two iterative cycles were carried out, comprising NMR screening, molecular modeling, X-ray crystallography, and in vitro biochemical testing. Six novel high-resolution PGDS complex structures were determined, and 300 hit analogues were tested. This rational drug design procedure culminated in the discovery of 24 compounds with an IC 50 below 1 microM in the in vitro assay. The best inhibitor (IC 50 = 21 nM) is one of the most potent inhibitors of PGDS to date. As such, it may enable new functional in vivo studies of PGDS and the prostaglandin metabolism pathway.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
GST S1-1, Recombinant Human