Issue 15, 2012

Synthesis of N-substituted ε-hexonolactams as pharmacological chaperones for the treatment of N370S mutant Gaucher disease

Abstract

A series of N-substituted ε-hexonolactams have been designed and prepared by a concise route with a tandem ring-expansion reaction as the key step. Some of the N-substituted ε-hexonolactams show better enhancements to N370S mutant β-glucocerebrosidase activity than NB-DNJ and NN-DNJ. Both the experimental results and computational studies highlight the importance of the carbonyl group for stabilizing protein folds in the mutant enzyme. The structure–activity relationships are also discussed. These novel N-alkylated iminosugars are promising pharmacological chaperones for the treatment of N370S mutant Gaucher disease.

Graphical abstract: Synthesis of N-substituted ε-hexonolactams as pharmacological chaperones for the treatment of N370S mutant Gaucher disease

Supplementary files

Article information

Article type
Communication
Submitted
26 Nov 2011
Accepted
06 Jan 2012
First published
09 Jan 2012

Org. Biomol. Chem., 2012,10, 2923-2927

Synthesis of N-substituted ε-hexonolactams as pharmacological chaperones for the treatment of N370S mutant Gaucher disease

G. Wang, G. Twigg, T. D. Butters, S. Zhang, L. Zhang, L. Zhang and X. Ye, Org. Biomol. Chem., 2012, 10, 2923 DOI: 10.1039/C2OB06987C

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