This paper describes the discovery of glycosyl acceptor analogs as potent and selective inhibitors of α-1, 3-and β-1, 4-galactosyltransferases. Incorporation of an appropriate aromatic group to the aglycon position of the enzyme's acceptors results in a strong inhibition, representing the first and most potent small uncharged molecules as selective inhibitors of these two enzymes and thus providing a new strategy for the development of ...
