Author:
Giguère Denis,St-Gelais Jacob
Abstract
AbstractSmall-molecule galectin inhibitors are useful research tools that could also be used as potential drug candidates. In that context, GB1107, a monosaccharidic galectin inhibitor, was shown to be an orally active galectin-3 antagonist that inhibits lung adenocarcinoma growth. Herein, a protecting-group-free synthesis of GB1107, along with other analogues is described. Starting from inexpensive levoglucosan, a Payne rearrangement/azidation process was used as key step. Finally, the use of a log P determination method based on 19F NMR spectroscopy was explored to assess the lipophilicity of galectin inhibitors.
Funder
Natural Sciences and Engineering Research Council of Canada
Université Laval
Subject
Organic Chemistry,Catalysis
Cited by
3 articles.
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