1. Academic Validation
  2. Inhibition of L-fucokinase from rat liver by L-fucose analogues in vitro

Inhibition of L-fucokinase from rat liver by L-fucose analogues in vitro

  • J Enzyme Inhib. 1997 Feb;11(4):265-73. doi: 10.3109/14756369709027655.
R Zeitler 1 S Danneschewski T Lindhorst J Thiem W Reutter
Affiliations

Affiliation

  • 1 Institut für Molekularbiologie und Biochemie der Freien Universität Berlin, Germany.
Abstract

By investigating the effects of more than 15 different L-fucose analogues on the activity of L-fucokinase (EC 2.7.1.52) from rat liver in vitro, certain structural requirements for potent inhibition of this Enzyme were established. Of the novel compounds, 4,6-dideoxy-L-xylo-hexopyranose (4) and methyl 4,6-dideoxy-4-iodo-L-glucopyranose (9) were found to be competitive inhibitors with Ki-values of 0.5 mM and 5.0 mM respectively. Thus 4,6-dideoxy-L-xylo-hexopyranose is a better inhibitor of L-fucokinase than methyl-alpha-L-fucoside (1). Uptake of L-fucose into rat hepatoma cells is reduced by 52% in the presence of the deoxy derivative (4), leading to a decrease of 45% in the incorporation of L-fucose into total cellular glycoproteins.

Figures
Products