We present a xylosylated
naphthoxyloside carrying a terminal azide
functionality that can be used for conjugation using click chemistry.
We show that this naphthoxyloside serves as a substrate for β4GalT7
and induces the formation of soluble glycosaminoglycan (GAG) chains
with physiologically relevant lengths and sulfation patterns. Finally,
we demonstrate its usefulness by conjugation to the Alexa Fluor 647
and TAMRA fluorophores and coupling to a surface plasmon resonance
chip for interaction studies with the hepatocyte growth factor known
to interact with the GAG heparan sulfate.
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