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Fucosyltransferase-specific inhibition via next generation of fucose mimetics.

Kyle C MartinJacopo TricomiFrancisco CorzanaAna García-GarcíaLaura Ceballos-LaitaThomas HicksSerena MonacoJesus AnguloRamon Hurtado GuerreroBarbara RichichiRobert Sackstein
Published in: Chemical communications (Cambridge, England) (2021)
The ability to custom-modify cell surface glycans holds great promise for treatment of a variety of diseases. We propose a glycomimetic of l-fucose that markedly inhibits the creation of sLeX by FTVI and FTVII, but has no effect on creation of LeX by FTIX. Our findings thus indicate that selective suppression of sLex display can be achieved, and STD-NMR studies surprisingly reveal that the mimetic does not compete with GDP-fucose at the enzymatic binding site.
Keyphrases
  • cell surface
  • high resolution
  • hydrogen peroxide
  • genome wide
  • big data
  • combination therapy
  • machine learning
  • dna methylation
  • replacement therapy