Conformationally-Locked N-Glycosides with Selective β-Glucosidase Inhibitory Activity: Identification of a New Non-Iminosugar-Type Pharmacological Chaperone for Gaucher Disease

被引:42
作者
Castilla, Javier [1 ]
Risquez, Rocio [2 ]
Cruz, Deysi [1 ]
Higaki, Katsumi [3 ]
Nanba, Eiji [3 ]
Ohno, Kousaku [4 ]
Suzuki, Yoshiyuki [5 ]
Diaz, Yolanda [1 ]
Ortiz Mellet, Carmen [2 ]
Garcia Fernandez, Jose M. [6 ]
Castillon, Sergio [1 ]
机构
[1] Univ Rovira & Virgili, Dept Quim Analit & Quim Organ, Tarragona 43007, Spain
[2] Univ Seville, Fac Quim, Dept Quim Organ, E-41012 Seville, Spain
[3] Tottori Univ, Fac Med, Res Ctr Biosci & Technol, Div Funct Gen, Yonago, Tottori 6838503, Japan
[4] Tottori Univ, Fac Med, Insitute Neurol Sci, Div Child Neurol, Yonago, Tottori 6838504, Japan
[5] Int Univ Hlth & Welf, Grad Sch, Otawara 3248501, Japan
[6] Univ Seville, CSIC, IIQ, Seville 41092, Spain
基金
日本科学技术振兴机构;
关键词
BIOLOGICAL EVALUATION; DERIVATIVES; ENZYME; THERAPY; POTENT; GLYCOMIMETICS; PROSPECTS; MECHANISM; ANALOGS; DESIGN;
D O I
10.1021/jm3006178
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
A series of conformationally locked N-glycosides having a cis-1,2-fused pyranose-1,3-oxazoline-2-thione structure and bearing different substituents at the exocyclic sulfur has been prepared. The polyhydroxylated bicyclic system was built in only three steps by treatment of the corresponding readily available 1,2-anhydrosugar with KSCN using TiO(TFA)(2) as catalyst, followed by S-alkylation and acetyl deprotection. In vitro screening against several glycosidase enzymes showed highly specific inhibition of mammalian beta-glucosidase with a marked dependence of the potency upon the nature of the exocyclic substituent. The most potent representative, bearing an S-(omega-hydroxyhexadecyl) substituent, was further assayed as inhibitor of the human lysosomal beta-glucocerebrosidase and as pharmacological chaperone in Gaucher disease fibroblasts. Activity enhancements in N370S/N370S mutants analogous to those achieved with the reference compound ambroxol were attained with a more favorable chaperone/inhibitor balance.
引用
收藏
页码:6857 / 6865
页数:9
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