Ligand compatibility of salacinol-type α-glucosidase inhibitors toward the GH31 family.
Fumihiro IshikawaAiko HiranoYuuto YoshimoriKana NishidaShinya NakamuraKatsuki TakashimaShinsuke MarumotoKiyofumi NinomiyaIsao NakanishiWeijia XieToshio MorikawaOsamu MuraokaGenzoh TanabePublished in: RSC advances (2021)
We show that salacinol-type α-glucosidase inhibitors are ligand-compatible with the GH 31 family. Salacinol and its 3'- O -benzylated analogs inhibit human lysosomal α-glucosidase at submicromolar levels. Simple structure-activity relationship studies reveal that the salacinol side-chain stereochemistry significantly influences binding to GH31 α-glucosidases.