Residue Asn 204 in the glucose binding site of hexokinase IV was mutated, in two separate experiments, to either Ala or Asp. The Asn → Ala mutant had a K_M nearly 50-fold greater than the wild-type enzyme, and the Asn → Asp mutant had a 140-fold greater K_M value than the wild-type enzyme. These mutations impact the intermolecular interactions between the enzyme and the glucose substrate.

The amide functional group of the Asn side chain can form                                                             with the hydroxyl groups of the glucose substrate and can potentially function as either a                                                            . The methyl group of Ala cannot participate in hydrogen bond formation, which explains the                                                             in glucose affinity as indicated by the higher K_M for the mutant enzyme. The side chain of Asp could potentially serve as a                                                            , but the higher K_M value for this mutant indicates that the substrate binds even                                                             than when the hydrogen bonding is abolished at this site. This indicates that the —NH₂ group of the Asn side chain functions as a hydrogen bond donor when interacting with the —OH groups of the glucose substrate and that this interaction is vitally important for substrate binding.