Pharmacological chaperone therapy for Fabry disease

Fabry disease is an inherited lysosomal storage disorder caused by deficient α-galactosidase A activity. Many missense mutations in Fabry disease often cause misfolded gene products, which leads to their retention in the endoplasmic reticulum by the quality control system; they are then removed by endoplasmic reticulum-associated degradation. We discovered that a potent α-galactosidase A inhibitor, 1-deoxygalactonojirimycin, acts as a pharmacological chaperone to facilitate the proper folding of the mutant enzyme by binding to its active site, thereby improving its stability and trafficking to the lysosomes in mammalian cells. The oral administration of 1-deoxygalactonojirimycin to transgenic mice expressing human mutant α-galactosidase A resulted in significant increases in α-galactosidase A activity in various organs, with concomitant reductions in globotriaosylceramide, which contributes to the pathology of Fabry disease. Seventy-eight missense mutations were found to be responsive to 1-deoxygalactonojirimycin. These data indicate that many patients with Fabry disease could potentially benefit from pharmacological chaperone therapy.

• Publication year

  2012

• Venue

  Proceedings of the Japan Academy. Series B, Physical and biological sciences

• Publication date

  2012-01-11

• Fields of study

  Biology, Medicine

• Identifiers
  DOI 10.2183/pjab.88.18PMID 22241068PMCID 3278969
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar, PubMed

• No claims are published for this paper.

• No concepts are published for this paper.

• Fabry disease: polymorphic haplotypes and a novel missense mutation in the GLA gene

  2012cited by this paper
• Increased globotriaosylceramide levels in a transgenic mouse expressing human alpha1,4-galactosyltransferase and a mouse model for treating Fabry disease.

  2011cited by this paper
• A Pharmacogenetic Approach to Identify Mutant Forms of α-Galactosidase A that Respond to a Pharmacological Chaperone for Fabry Disease

  2011cited by this paper
• Quality control in the endoplasmic reticulum.

  2010cited by this paper
• Inner ear pathology of alpha-galactosidase A deficient mice, a model of Fabry disease.

  2010cited by this paper
• Functional studies of new GLA gene mutations leading to conformational Fabry disease.

  2010cited by this paper
• The pharmacological chaperone 1-deoxygalactonojirimycin reduces tissue globotriaosylceramide levels in a mouse model of Fabry disease.

  2010cited by this paper
• Preclinical Efficacy and Safety of 1-Deoxygalactonojirimycin in Mice for Fabry Disease

  2009influential reference
• The pharmacological chaperone 1-deoxygalactonojirimycin increases α-galactosidase A levels in Fabry patient cell lines

  2009cited by this paper
• Effect of agalsidase alfa replacement therapy on Fabry disease-related hypertrophic cardiomyopathy: a 12- to 36-month, retrospective, blinded echocardiographic pooled analysis.

  2009cited by this paper
• Drug development and the cellular quality control system.

  2009cited by this paper
• The Pharmacological Chaperone N-butyldeoxynojirimycin Enhances Enzyme Replacement Therapy in Pompe Disease Fibroblasts

  2009cited by this paper
• [Fabry disease].

  2009cited by this paper
• Iminosugars-From Synthesis to Therapeutic Applications

  2009cited by this paper
• Enzyme replacement therapy with agalsidase alfa in patients with Fabry's disease: an analysis of registry data.

  2009cited by this paper
• Effects of a chemical chaperone on genetic mutations in α-galactosidase A in Korean patients with Fabry disease

  2009cited by this paper
• Chemical and Biological Folding Contribute to Temperature‐Sensitive ΔF508 CFTR Trafficking

  2008cited by this paper
• Rescue of mutant alpha-galactosidase A in the endoplasmic reticulum by 1-deoxygalactonojirimycin leads to trafficking to lysosomes.

  2008influential reference
• Identification of pharmacological chaperones as potential therapeutic agents to treat phenylketonuria.

  2008cited by this paper
• Prediction of response of mutated alpha-galactosidase A to a pharmacological chaperone

  2008cited by this paper
• PHARMACOLOGICAL CHAPERONE THERAPY

  2008cited by this paper
• Novel mutations of the GLA gene in Japanese patients with Fabry disease and their functional characterization by active site specific chaperone

  2008cited by this paper
• Medicinal use of iminosugars

  2008cited by this paper
• A counterintuitive approach to treat enzyme deficiencies: use of enzyme inhibitors for restoring mutant enzyme activity

  2008influential reference
• Weekly enzyme replacement therapy may slow decline of renal function in patients with Fabry disease who are on long-term biweekly dosing.

  2007cited by this paper
• Cellular and tissue localization of globotriaosylceramide in Fabry disease

  2007cited by this paper
• Mutant α-galactosidase A enzymes identified in Fabry disease patients with residual enzyme activity: biochemical characterization and restoration of normal intracellular processing by 1-deoxygalactonojirimycin

  2007cited by this paper
• Effects of enzyme replacement therapy on the cardiomyopathy of Anderson–Fabry disease: a randomised, double-blind, placebo-controlled clinical trial of agalsidase alfa

  2007cited by this paper
• Screening for pharmacological chaperones in Fabry disease.

  2007cited by this paper
• Active‐site‐specific chaperone therapy for Fabry disease

  2007cited by this paper
• Chemical chaperones improve transport and enhance stability of mutant alpha-glucosidases in glycogen storage disease type II.

  2007cited by this paper
• Pharmacological chaperone corrects lysosomal storage in Fabry disease caused by trafficking-incompetent variants.

  2006cited by this paper
• Hydrophilic iminosugar active‐site‐specific chaperones increase residual glucocerebrosidase activity in fibroblasts from Gaucher patients

  2006cited by this paper
• High incidence of later-onset fabry disease revealed by newborn screening.

  2006cited by this paper
• Long-term therapy with agalsidase alfa for Fabry disease: safety and effects on renal function in a home infusion setting.

  2006cited by this paper
• Lysosomal storage diseases: natural history and ethical and economic aspects.

  2006cited by this paper
• Emerging Strategies for the Treatment of Hereditary Metabolic Storage Disorders

  2006cited by this paper
• Fabry disease: correlation between structural changes in α-galactosidase, and clinical and biochemical phenotypes

  2005cited by this paper
• A synthetic chaperone corrects the trafficking defect and disease phenotype in a protein misfolding disorder

  2005cited by this paper
• Fabry Disease in Patients with End-Stage Renal Failure: The Potential Benefits of Screening

  2005cited by this paper
• Pharmacologic chaperones as a potential treatment for X-linked nephrogenic diabetes insipidus.

  2005cited by this paper
• Transgenic mouse expressing human mutant alpha-galactosidase A in an endogenous enzyme deficient background: a biochemical animal model for studying active-site specific chaperone therapy for Fabry disease.

  2004cited by this paper
• Chemical chaperones protect from effects of apoptosis-inducing mutation in carbonic anhydrase IV identified in retinitis pigmentosa 17.

  2004cited by this paper
• Pharmacological chaperones: potential treatment for conformational diseases.

  2004cited by this paper
• Pharmacological Enhancement of β-Hexosaminidase Activity in Fibroblasts from Adult Tay-Sachs and Sandhoff Patients*

  2004cited by this paper
• Efficient and rapid purification of recombinant human alpha-galactosidase A by affinity column chromatography.

  2004cited by this paper
• The molecular defect leading to Fabry disease: structure of human alpha-galactosidase.

  2004cited by this paper
• Roles of N-linked glycans in the endoplasmic reticulum.

  2004cited by this paper
• EDEM As an Acceptor of Terminally Misfolded Glycoproteins Released from Calnexin

  2003cited by this paper
• Therapeutic approaches to protein-misfolding diseases

  2003cited by this paper
• A contradictory treatment for lysosomal storage disorders: inhibitors enhance mutant enzyme activity.

  2003cited by this paper
• Fabry disease: detection of undiagnosed hemodialysis patients and identification of a "renal variant" phenotype.

  2003cited by this paper
• Chemical chaperone therapy for brain pathology in GM1-gangliosidosis

  2003cited by this paper
• Quality control in the endoplasmic reticulum

  2003cited by this paper
• Substrate reduction therapy in mouse models of the glycosphingolipidoses.

  2003cited by this paper
• Structural basis of Fabry disease.

  2002cited by this paper
• Molecular Chaperones in the Cytosol: from Nascent Chain to Folded Protein

  2002cited by this paper
• Chemical chaperones increase the cellular activity of N370S β-glucosidase: A therapeutic strategy for Gaucher disease

  2002cited by this paper
• The Metabolic and Molecular Bases of Inherited Disease

  2001cited by this paper
• Enzyme replacement therapy in Fabry disease

  2001cited by this paper
• The action of molecular chaperones in the early secretory pathway.

  2001cited by this paper
• Enzyme replacement therapy in Fabry disease: a randomized controlled trial.

  2001cited by this paper
• A phase 1/2 clinical trial of enzyme replacement in fabry disease: pharmacokinetic, substrate clearance, and safety studies.

  2001cited by this paper
• Not such a dismal science: the economics of protein synthesis, folding, degradation and antigen processing.

  2001cited by this paper
• Improvement in cardiac function in the cardiac variant of Fabry's disease with galactose-infusion therapy.

  2001cited by this paper
• Safety and efficacy of recombinant human alpha-galactosidase a replacement therapy in Fabry's disease

  2001cited by this paper
• Safety and efficacy of recombinant human alpha-galactosidase A replacement therapy in Fabry's disease.

  2001cited by this paper
• Reduction of globotriaosylceramide in Fabry disease mice by substrate deprivation.

  2000cited by this paper
• The Hsc70 co-chaperone CHIP targets immature CFTR for proteasomal degradation

  2000cited by this paper
• Characterization of two alpha-galactosidase mutants (Q279E and R301Q) found in an atypical variant of Fabry disease.

  2000cited by this paper
• Rapid degradation of a large fraction of newly synthesized proteins by proteasomes

  2000cited by this paper
• Role of Ser-65 in the activity of alpha-galactosidase A: characterization of a point mutation (S65T) detected in a patient with Fabry disease.

  2000cited by this paper
• In vitro inhibition and intracellular enhancement of lysosomal alpha-galactosidase A activity in Fabry lymphoblasts by 1-deoxygalactonojirimycin and its derivatives.

  2000cited by this paper
• Accelerated transport and maturation of lysosomal α–galactosidase A in Fabry lymphoblasts by an enzyme inhibitor

  1999cited by this paper
• Alpha-galactosidase transgenic mouse: heterogeneous gene expression and posttranslational glycosylation in tissues.

  1998cited by this paper
• Folding of secretory and membrane proteins.

  1998cited by this paper
• Specific alpha-galactosidase inhibitors, N-methylcalystegines--structure/activity relationships of calystegines from Lycium chinense.

  1997cited by this paper
• alpha-Galactosidase A deficient mice: a model of Fabry disease.

  1997cited by this paper
• The effects of calystegines isolated from edible fruits and vegetables on mammalian liver glycosidases.

  1997cited by this paper
• Generation and characterization of transgenic mice expressing a human mutant α‐galactosidase with an R301Q substitution causing a variant form of Fabry disease

  1997cited by this paper
• Quality control in the secretory pathway.

  1995cited by this paper
• Calystegins of Physalis alkekengi var. francheti (Solanaceae). Structure determination and their glycosidase inhibitory activities.

  1995cited by this paper
• Defective protein folding as a basis of human disease.

  1995cited by this paper
• Mutant (δF508) Cystic Fibrosis Transmembrane Conductance Regulator Cl− Channel Is Functional When Retained in Endoplasmic Reticulum of Mammalian Cells (*)

  1995cited by this paper
• An atypical variant of Fabry's disease in men with left ventricular hypertrophy.

  1995cited by this paper
• Human alpha-galactosidase gene expression: significance of two peptide regions encoded by exons 1-2 and 6.

  1994cited by this paper
• Characterization of a mutant alpha-galactosidase gene product for the late-onset cardiac form of Fabry disease.

  1993cited by this paper
• Point mutations in the upstream region of the α-galactosidase A gene exon 6 in an atypical variant of Fabry disease

  1992cited by this paper
• An atypical variant of Fabry's disease with manifestations confined to the myocardium.

  1991cited by this paper
• Protein degradation in the endoplasmic reticulum.

  1990cited by this paper
• Protein oligomerization in the endoplasmic reticulum.

  1989cited by this paper
• Structural organization of the human alpha-galactosidase A gene: further evidence for the absence of a 3' untranslated region.

  1988cited by this paper
• Synthesis and processing of alpha-galactosidase A in human fibroblasts. Evidence for different mutations in Fabry disease.

  1987cited by this paper
• Human alpha-galactosidase A: nucleotide sequence of a cDNA clone encoding the mature enzyme.

  1986cited by this paper
• Experimental and theoretical aspects of protein folding.

  1975cited by this paper
• Renal pathologic lesions and functional alterations in a man with Fabry's disease.

  1973cited by this paper
• Enzymatic defect in Fabry's disease. Ceramidetrihexosidase deficiency.

  1967cited by this paper

• Cryo-ablation management of atrial fibrillation in Fabry disease without agalsidase alpha: a case report

  2025cites this paper
• Expert review in diagnostic, therapeutic and follow-up of Fabry disease in Latin America based on patient care standards

  2025cites this paper
• Bioinformatics-Driven Multi-Factorial Insight into α-Galactosidase Mutations

  2025cites this paper
• Effects of Enzyme Replacement Therapy on Cardiac MRI Findings in Fabry Disease: A Systematic Review and Meta-Analysis.

  2024cites this paper
• Identification of potential pharmacological chaperones that selectively stabilize mutated Aspartoacylases in Canavan disease.

  2024cites this paper
• Design and Pharmacological Chaperone Effects of N-(4'-Phenylbutyl)-DAB Derivatives Targeting the Lipophilic Pocket of Lysosomal Acid α-Glucosidase.

  2023cites this paper
• Therapeutic Role of DGJ (1‐deoxygalactonojirimycin) in Fabry Disease: Theoretical Insights

  2023cites this paper
• Clinical and diagnostic aspects of Fabry disease management: a narrative review with a particular focus on Brazilian experts’ perspectives

  2022cites this paper
• Functional characterization of novel variants found in patients with suspected Fabry disease.

  2022cites this paper
• 5-C-Branched Deoxynojirimycin: Strategy for Designing a 1-Deoxynojirimycin-Based Pharmacological Chaperone with a Nanomolar Affinity for Pompe Disease.

  2022cites this paper
• A New Genetic Insight for Orphan Renal Disorder, Fabry: A Review

  2021cites this paper
• Pharmacological Therapy in Inborn Errors of Metabolism

  2020cites this paper
• Assistance for Folding of Disease-Causing Plasma Membrane Proteins

  2020cites this paper
• Strategy for Designing Selective Lysosomal Acid α-Glucosidase Inhibitors: Binding Orientation and Influence on Selectivity

  2020cites this paper
• Computational and modeling approaches to understand the impact of the Fabry's disease causing mutation (D92Y) on the interaction with pharmacological chaperone 1-deoxygalactonojirimycin (DGJ).

  2019cites this paper
• Efficacy and safety of migalastat in a Japanese population: a subgroup analysis of the ATTRACT study

  2019cites this paper
• Functional Characterization and Pharmacological Evaluation of a Novel GLA Missense Mutation Found in a Severely Affected Fabry Disease Family

  2019cites this paper
• A small molecule chaperone rescues the stability and activity of a cancer‐associated variant of NAD(P)H:quinone oxidoreductase 1 in vitro

  2019cites this paper
• New Advanced Strategies for the Treatment of Lysosomal Diseases Affecting the Central Nervous System.

  2019cites this paper
• Inflammatory response and its relation to sphingolipid metabolism proteins: Chaperones as potential indirect anti-inflammatory agents.

  2019cites this paper
• A comparative computational approach toward pharmacological chaperones (NN-DNJ and ambroxol) on N370S and L444P mutations causing Gaucher's disease.

  2019cites this paper
• Identification of a novel loss-of-function mutation of the GLA gene in a Chinese Han family with Fabry disease

  2018cites this paper
• Pharmacoperone drugs: targeting misfolded proteins causing lysosomal storage-, ion channels-, and G protein-coupled receptors-associated conformational disorders

  2018cites this paper
• In silico analyses of essential interactions of iminosugars with the Hex A active site and evaluation of their pharmacological chaperone effects for Tay-Sachs disease.

  2017cites this paper
• Chemical chaperone treatment for galactosialidosis: Effect of NOEV on β-galactosidase activities in fibroblasts.

  2016cites this paper
• New therapeutic approaches for Krabbe disease: The potential of pharmacological chaperones

  2016cites this paper
• N‐Alkyl‐, 1‐C‐Alkyl‐, and 5‐C‐Alkyl‐1,5‐dideoxy‐1,5‐imino‐(l)‐ribitols as Galactosidase Inhibitors

  2016cites this paper
• Using CRISPR/Cas9-Mediated GLA Gene Knockout as an In Vitro Drug Screening Model for Fabry Disease

  2016cites this paper
• Personalized Pharmacoperones for Lysosomal Storage Disorder: Approach for Next-Generation Treatment.

  2016cites this paper
• Screening of Fabry disease in patients with end-stage renal disease of unknown etiology: the first Thailand study

  2016cites this paper
• Carbohydrate-Processing Enzymes of the Lysosome: Diseases Caused by Misfolded Mutants and Sugar Mimetics as Correcting Pharmacological Chaperones.

  2016cites this paper
• Unexplained peripheral neuropathic pain and/or stroke

  2016cites this paper
• Isolation and SAR studies of bicyclic iminosugars from Castanospermum australe as glycosidase inhibitors.

  2015cites this paper
• Mystery Case: A 21-year-old man with visual loss following marijuana use

  2015influential citation
• Chaperone therapy for Krabbe disease: potential for late-onset GALC mutations

  2015cites this paper
• Lysosomal Storage Disorders

  2015cites this paper
• Combined Therapies for Lysosomal Storage Diseases.

  2015cites this paper
• Towards detailed structural understanding of α-ʟ-fucosidase : insights through X-ray crystallography and inhibitor-binding

  2015cites this paper
• Natural product and natural product derived drugs in clinical trials.

  2014cites this paper
• Using pharmacological chaperones to restore proteostasis.

  2014cites this paper
• Iminosugar‐Based Galactoside Mimics as Inhibitors of Galactocerebrosidase: SAR Studies and Comparison with Other Lysosomal Galactosidases

  2014cites this paper
• Sphingolipids and lysosomal pathologies.

  2014cites this paper
• Pharmacological chaperoning: a primer on mechanism and pharmacology.

  2014cites this paper
• Lysosomal Storage Disorders Including Neuronal Ceroid Lipofuscinoses

  2014cites this paper
• Emerging novel concept of chaperone therapies for protein misfolding diseases

  2014cites this paper
• Concept and Development of Chaperone Therapy for Protein Misfolding Diseases

  2014cites this paper
• A thermodynamic assay to test pharmacological chaperones for Fabry disease

  2014influential citation
• Fabry_CEP: a tool to identify Fabry mutations responsive to pharmacological chaperones

  2013cites this paper
• Fabry Disease: A Review of Ophthalmic and Systemic Manifestations

  2013cites this paper
• Glucocerebrosidase inhibitors for the treatment of Gaucher disease.

  2013cites this paper
• Unfolded protein response in Gaucher disease: from human to Drosophila

  2013cites this paper
• A high-throughput screening assay using Krabbe disease patient cells.

  2013cites this paper
• Enfermedad de Fabry. Diagnóstico dermatológico temprano y tratamiento

  2013cites this paper
• Coronary microvascular dysfunction is an early feature of cardiac involvement in patients with Anderson–Fabry disease

  2013cites this paper
• A symptomatic Fabry disease mouse model generated by inducing globotriaosylceramide synthesis.

  2013cites this paper
• Biochemical phenotype of a common disease-causing mutation and a possible therapeutic approach for the phosphomannomutase 2-associated disorder of glycosylation

  2013influential citation
• Gene Therapy for Fabry Disease: A Review of the Literature

  2013cites this paper
• Alteration of proteomic profiles in PBMC isolated from patients with Fabry disease: preliminary findings.

  2013cites this paper
• Multiplex analysis of novel urinary lyso-Gb3-related biomarkers for Fabry disease by tandem mass spectrometry.

  2013cites this paper
• Treatment options for lysosomal storage disorders: developing insights

  2012influential citation
• Fabry disease: a case report

  year unknowncites this paper