pH‐Responsive Trihydroxylated Piperidines Rescue The Glucocerebrosidase Activity in Human Fibroblasts Bearing The Neuronopathic Gaucher‐Related L444P/L444P Mutations in GBA1 Gene

Author:

Davighi Maria Giulia12,Matassini Camilla1,Clemente Francesca1,Paoli Paolo3,Morrone Amelia45,Cacciarini Martina16,Goti Andrea1,Cardona Francesca1ORCID

Affiliation:

1. Department of Chemistry “Ugo Schiff” (DICUS) University of Florence Via della Lastruccia 3–13 50019 Sesto F.no (FI) Italy

2. Current address: BioMedical Engineering and Imaging Institute Icahn School of Medicine at Mount Sinai 1470 Madison Ave, New York 10029 New York USA

3. Department of Experimental and Clinical Biomedical Sciences University of Florence Viale Morgagni 50 50134 Firenze Italy

4. Laboratory of Molecular Biology of Neurometabolic Diseases Meyer Children's Hospital IRCCS Viale Pieraccini 24 50139 Firenze Italy

5. Department of Neurosciences Psychology Drug Research and Child Health University of Florence Viale Pieraccini 24 50139 Firenze Italy

6. Department of Chemistry University of Copenhagen Universitetsparken 5 DK-2100 Copenhagen Ø Denmark

Abstract

AbstractEngineering bioactive iminosugars with pH‐responsive groups is an emerging approach to develop pharmacological chaperones (PCs) able to improve lysosomal trafficking and enzymatic activity rescue of mutated enzymes. The use of inexpensive l‐malic acid allowed introduction of orthoester units into the lipophilic chain of an enantiomerically pure iminosugar affording only two diastereoisomers contrary to previous related studies. The iminosugar was prepared stereoselectively from the chiral pool (d‐mannose) and chosen as the lead bioactive compound, to develop novel candidates for restoring the lysosomal enzyme glucocerebrosidase (GCase) activity. The stability of orthoester‐appended iminosugars was studied by 1H NMR spectroscopy both in neutral and acidic environments, and the loss of inhibitory activity with time in acid medium was demonstrated on cell lysates. Moreover, the ability to rescue GCase activity in the lysosomes as the result of a chaperoning effect was explored. A remarkable pharmacological chaperone activity was measured in fibroblasts hosting the homozygous L444P/L444P mutation, a cell line resistant to most PCs, besides the more commonly responding N370S mutation.

Funder

Ministero dell’Istruzione, dell’Università e della Ricerca

Regione Toscana

Publisher

Wiley

Subject

Organic Chemistry,Molecular Biology,Molecular Medicine,Biochemistry

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