Abstract:A series of hybrid analogues was designed by combination of the iminoxylitol scaffold of parent 1C9-DIX with triazolylalkyl side chains. The resulting compounds were considered potential pharmacological chaperones in Gaucher disease. The DIX analogues reported here were synthesized by CuAAC click chemistry from scaffold 1 (α-1-C-propargyl-1,5-dideoxy-1,5-imino-D-xylitol) and screened as imiglucerase inhibitors. A set of selected compounds were tested as β-glucocerebrosidase (GBA1) enhancers in fibroblasts from… Show more
“…8 ). This might be an explanation for the exceptional ligand properties as well as the selectivity of C-1-substituted DIX derivatives, which has been observed previously by others and us for similar alkyl-iminoxylitols [ 30 , 34 , 36 – 40 ]. Fig.…”
Section: Introductionsupporting
confidence: 73%
“…We decided to introduce either an ester group or an imidazole residue. Both functional groups have been found to be suitable for ligand properties of GCase [ 34 , 36 ].…”
Section: Resultsmentioning
confidence: 99%
“…Compain and co-workers synthesized a library of 1- C -triazolylalkyl side chain-modified DIX analogues (Fig. 4 ), including compounds 12 , by a click chemistry approach, and found that some of these are GCase enhancers for selected Gaucher disease genotype mutants [ 35 , 36 ]. Fig.…”
Modified 1,5-dideoxy-1,5-imino-
d
-xylitol analogues with different substitution patterns involving position C-1 and/or the ring nitrogen were prepared, which were designed to serve as precursors for the preparation of iminoxylitol-based ligands and tools for the elucidation and modulation of human lysosomal
β
-glucocerebrosidase. Biological evaluation of the synthesized glycomimetics with a series of glycoside hydrolases revealed that these substitution patterns elicit excellent
β
-glucosidase selectivities.
Graphical abstract
Electronic supplementary material
The online version of this article (10.1007/s00706-019-02427-1) contains supplementary material, which is available to authorized users.
“…8 ). This might be an explanation for the exceptional ligand properties as well as the selectivity of C-1-substituted DIX derivatives, which has been observed previously by others and us for similar alkyl-iminoxylitols [ 30 , 34 , 36 – 40 ]. Fig.…”
Section: Introductionsupporting
confidence: 73%
“…We decided to introduce either an ester group or an imidazole residue. Both functional groups have been found to be suitable for ligand properties of GCase [ 34 , 36 ].…”
Section: Resultsmentioning
confidence: 99%
“…Compain and co-workers synthesized a library of 1- C -triazolylalkyl side chain-modified DIX analogues (Fig. 4 ), including compounds 12 , by a click chemistry approach, and found that some of these are GCase enhancers for selected Gaucher disease genotype mutants [ 35 , 36 ]. Fig.…”
Modified 1,5-dideoxy-1,5-imino-
d
-xylitol analogues with different substitution patterns involving position C-1 and/or the ring nitrogen were prepared, which were designed to serve as precursors for the preparation of iminoxylitol-based ligands and tools for the elucidation and modulation of human lysosomal
β
-glucocerebrosidase. Biological evaluation of the synthesized glycomimetics with a series of glycoside hydrolases revealed that these substitution patterns elicit excellent
β
-glucosidase selectivities.
Graphical abstract
Electronic supplementary material
The online version of this article (10.1007/s00706-019-02427-1) contains supplementary material, which is available to authorized users.
“…Paradigmatic examples are shown in Figure 2 . Compounds 7 [ 38 ] have been introduced by Mellet and coworkers, d - xylo configured 1- C -alkyl iminosugars 8 [ 39 ] represent another important family which is also true for compounds 9 [ 40 ], all showing significant properties as pharmacological chaperones for mutant GCases.…”
The scope of a series of N-alkylated iminosugar based inhibitors in the d-gluco as well as d-xylo configuration towards their interaction with human lysosomal β-glucocerebrosidase has been evaluated. A versatile synthetic toolbox has been developed for the synthesis of N-alkylated iminosugar scaffolds conjugated to a variety of terminal groups via a benzoic acid ester linker. The terminal groups such as nitrile, azide, alkyne, nonafluoro-tert-butyl and amino substituents enable follow-up chemistry as well as visualisation experiments. All compounds showed promising inhibitory properties as well as selectivities for β-glucosidases, some exhibiting activities in the low nanomolar range for β-glucocerebrosidase.
“…However, while several examples of N ‐ and O ‐armed alkynyl iminosugars have been published, only one example of a 1‐ C ‐propargyl compound has been reported to date in the piperidine series (i.e., 1‐ C ‐propargyl‐1‐deoxyimino‐ d ‐xylitol) . A few examples based on a pyrrolidine core have been obtained by organocatalysis or through addition to cyclic N,O‐acetals or to cyclic nitrones …”
The convenient preparation of 1,4‐dideoxy‐1,4‐imino‐l‐arabinitol derivatives bearing a propargyl group through the addition of a trimethylsilylpropargyl Grignard reagent to an N‐sulfinylglycosylamine is reported. One of these compounds was coupled by a triazole tether to various aromatic and heteroaromatic groups to give structures that can be considered to be simplified mimics of UDP‐Galf, the substrate of GlfT2, a galactofuranosyltransferase present in mycobacteria. The new compounds were evaluated as inhibitors of this enzyme and were found to have significant activity (IC50 values in the high µm to low mm range), despite the absence of the diphospho linkage present in the parent sugar nucleotide.
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