Identification of an Allosteric Binding Site on Human Lysosomal Alpha-Galactosidase Opens the Way to New Pharmacological Chaperones for Fabry Disease
Academic Article
Publication Date:
2016
abstract:
Personalized therapies are required for Fabry disease due to its large phenotypic spectrum and numerous different genotypes. In principle, missense mutations that do not affect the active site could be rescued with pharmacological chaperones. At present pharmacological chaperones for Fabry disease bind the active site and couple a stabilizing effect, which is required, to an inhibitory effect, which is deleterious. By in silico docking we identified an allosteric hot-spot for ligand binding where a drug-like compound, 2,6-dithiopurine, binds preferentially. 2,6-dithiopurine stabilizes lysosomal alpha-galactosidase in vitro and rescues a mutant that is not responsive to a mono-therapy with previously described pharmacological chaperones, 1-deoxygalactonojirimycin and galactose in a cell based assay. Copyright: CC BY
Iris type:
01.01 Articolo in rivista
Keywords:
Fabry disease; pharmacological chaperones; lysosomal alpha-galactosidase; allosteric site; Dithiopurine; Biochemistry; Medicine; Cell Biology; Pharmacology; Evolutionary Biology; Chemical sciences; Biological Sciences; Infectious diseases; Chaperone; Human Lysosomal Alpha-Galactosidase Opens; Ligand Binding; silico docking; Missense Mutations; dithiopurine; Fabry disease bind; Fabry Disease Personalized therapies; 1- deoxygalactonojirimycin; lysosomal alpha-galactosidase; Allosteric Binding Site; phenotypic spectrum; allosteric hot-spot; New Pharmacological Chaperones; drug-like compound; Fabry Disease; Site; Fabry disease; Fabry disease; pharmacological chaperone
List of contributors:
Andreotti, Giuseppina
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