| Literature DB >> 22213563 |
Daniel Schwizer1, John T Patton, Brian Cutting, Martin Smieško, Beatrice Wagner, Ako Kato, Céline Weckerle, Florian P C Binder, Said Rabbani, Oliver Schwardt, John L Magnani, Beat Ernst.
Abstract
A new class of N-acetyl-D-glucosamine (GlcNAc) mimics for E-selectin antagonists was designed and synthesized. The mimic consists of a cyclohexane ring substituted with alkyl substituents adjacent to the linking position of the fucose moiety. Incorporation into E-selectin antagonists led to the test compounds 8 and the 2'-benzoylated analogues 21, which exhibit affinities in the low micromolar range. By using saturation transfer difference (STD)-NMR it could be shown that the increase in affinity does not result from an additional hydrophobic contact of the alkyl substituent with the target protein E-selectin, but rather from a steric effect stabilizing the antagonist in its bioactive conformation. The loss of affinity found for antagonists 10 and 35 containing a methyl substituent in a remote position (and therefore unable to support to the stabilization of the core) further supports this hypothesis. Finally, when a GlcNAc mimetic containing two methyl substituents (52 and 53) was used, in which one methyl was positioned adjacent to the fucose linking position and the other was in a remote position, the affinity was regained.Entities:
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Year: 2011 PMID: 22213563 DOI: 10.1002/chem.201102884
Source DB: PubMed Journal: Chemistry ISSN: 0947-6539 Impact factor: 5.236