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Chemoenzymatic synthesis of GDP-L-fucose and the Lewis X glycan derivatives.

Proceedings of the National Academy of Sciences of the United States of America (2009-10-07)
Wei Wang, Tianshun Hu, Patrick A Frantom, Tianqing Zheng, Brian Gerwe, David Soriano Del Amo, Sarah Garret, Ronald D Seidel, Peng Wu
ANOTACE

Lewis X (Le(x))-containing glycans play important roles in numerous cellular processes. However, the absence of robust, facile, and cost-effective methods for the synthesis of Le(x) and its structurally related analogs has severely hampered the elucidation of the specific functions of these glycan epitopes. Here we demonstrate that chemically defined guanidine 5'-diphosphate-beta-l-fucose (GDP-fucose), the universal fucosyl donor, the Le(x) trisaccharide, and their C-5 substituted derivatives can be synthesized on preparative scales, using a chemoenzymatic approach. This method exploits l-fucokinase/GDP-fucose pyrophosphorylase (FKP), a bifunctional enzyme isolated from Bacteroides fragilis 9343, which converts l-fucose into GDP-fucose via a fucose-1-phosphate (Fuc-1-P) intermediate. Combining the activities of FKP and a Helicobacter pylori alpha1,3 fucosyltransferase, we prepared a library of Le(x) trisaccharide glycans bearing a wide variety of functional groups at the fucose C-5 position. These neoglycoconjugates will be invaluable tools for studying Le(x)-mediated biological processes.

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Sigma-Aldrich
Guanosine 5′-diphospho-β-L-fucose sodium salt, ≥85%