| Literature DB >> 24411201 |
Jack U Flanagan1, Graham J Atwell2, Daniel M Heinrich2, Darby G Brooke2, Shevan Silva2, Laurent J M Rigoreau3, Elisabeth Trivier3, Andrew P Turnbull3, Tony Raynham3, Stephen M F Jamieson1, William A Denny4.
Abstract
Inhibitors of the aldo-keto reductase enzyme AKR1C3 are of interest as potential drugs for leukemia and hormone-related cancers. A series of non-carboxylate morpholino(phenylpiperazin-1-yl)methanones were prepared by palladium-catalysed coupling of substituted phenyl or pyridyl bromides with the known morpholino(piperazin-1-yl)methanone, and shown to be potent (IC50∼100nM) and very isoform-selective inhibitors of AKR1C3. Lipophilic electron-withdrawing substituents on the phenyl ring were positive for activity, as was an H-bond acceptor on the other terminal ring, and the ketone moiety (as a urea) was essential. These structure-activity relationships are consistent with an X-ray structure of a representative compound bound in the AKR1C3 active site, which showed H-bonding between the carbonyl oxygen of the drug and Tyr55 and His117 in the 'oxyanion hole' of the enzyme, with the piperazine bridging unit providing the correct twist to allow the terminal benzene ring to occupy the lipophilic pocket and align with Phe311.Entities:
Keywords: AKR; Aldo–keto reductase; COX; Computer aided drug design; Crystal structure; DCM; DIPEA; DMSO; Inhibitor; Morpholylureas; NADPH; NSAID; PBD; Protein Data Bank; TFA; aldo–keto reductase; cyclo-oxygenase; dichloromethane; diisopropylethylamine; dimethyl sulfoxide; nicotinamide adenine dinucleotide phosphate; non-steroidal anti-inflammatory drugs; trifluoroacetic acid
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Year: 2014 PMID: 24411201 DOI: 10.1016/j.bmc.2013.12.050
Source DB: PubMed Journal: Bioorg Med Chem ISSN: 0968-0896 Impact factor: 3.641