Your search keyword '"Glucosylceramidase chemistry"' showing total 154 results

1. Investigating the Impact of the Parkinson's-Associated GBA1 E326K Mutation on β-Glucocerebrosidase Dimerization and Interactome Dynamics Through an In Silico Approach.

Author

Pietrafesa D, Casamassa A, Benassi B, Santoro M, Marano M, Consales C, Rosati J, and Arcangeli C

Subjects

Humans, Mutation, Protein Binding, Lysosomes metabolism, Saposins genetics, Saposins metabolism, Saposins chemistry, Glucosylceramidase genetics, Glucosylceramidase metabolism, Glucosylceramidase chemistry, Parkinson Disease genetics, Parkinson Disease metabolism, Molecular Dynamics Simulation, Protein Multimerization, alpha-Synuclein metabolism, alpha-Synuclein genetics, alpha-Synuclein chemistry

Abstract

Heterozygous mutations or genetic variants in the GBA1 gene, which encodes for the β-glucocerebrosidase (GCase), a lysosomal hydrolase enzyme, may increase the risk of Parkinson's disease (PD) onset. The heterozygous E326K form is one of the most common genetic risk factors for PD worldwide, but, to date, the underlying molecular mechanisms remain unclear. Here, we investigate the effect of the E326K on the structure, stability, dimerization process, and interaction mode with some proteins of the interactome of GCase using multiple molecular dynamics (MD) simulations at pH 5.5 and pH 7.0 to mimic the lysosomal and endoplasmic reticulum environments, respectively. The analysis of the MD trajectories highlights that the E326K mutation did not significantly alter the structural conformation of the catalytic dyad but significantly makes the structure of the dimeric complexes unstable, especially at lysosomal pH, potentially impacting the organization of the quaternary structure. Furthermore, the E326K mutation significantly impacts protein interactions by altering the binding mode with the activator Saposin C (SapC), reducing the binding affinity with the inhibitor α-Synuclein (α-Syn), and increasing the affinity for the Lysosomal integral membrane protein-2 (LIMP-2) transporter.

Published

2024

2. sp 2 -Iminosugar azobenzene O-glycosides: Light-sensitive glycosidase inhibitors with unprecedented tunability and switching factors.

Author

Rivero-Barbarroja G, Carmen Padilla-Pérez M, Maisonneuve S, Isabel García-Moreno M, Tiet B, Vocadlo DJ, Xie J, García Fernández JM, and Ortiz Mellet C

Subjects

Humans, Dose-Response Relationship, Drug, Light, Molecular Structure, Structure-Activity Relationship, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Glucosylceramidase pharmacology, Azo Compounds chemistry, Azo Compounds pharmacology, Azo Compounds chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Enzyme Inhibitors chemical synthesis, Glycoside Hydrolases antagonists & inhibitors, Glycoside Hydrolases metabolism, Glycosides chemistry, Glycosides pharmacology, Glycosides chemical synthesis, Imino Sugars chemistry, Imino Sugars pharmacology, Imino Sugars chemical synthesis

Abstract

The conventional approach to developing light-sensitive glycosidase activity regulators, involving the combination of a glycomimetic moiety and a photoactive azobenzene module, results in conjugates with differences in glycosidase inhibitory activity between the interchangeable E and Z-isomers at the azo group that are generally below one-order of magnitude. In this study, we have exploited the chemical mimic character of sp 2 -iminosugars to access photoswitchable p- and o-azobenzene α-O-glycosides based on the gluco-configured representative ONJ. Notably, we achieved remarkably high switching factors for glycosidase inhibition, favoring either the E- or Z-isomer depending on the aglycone structure. Our data also indicate a correlation between the isomeric state of the azobenzene module and the selectivity towards α- and β-glucosidase isoenzymes. The most effective derivative reached over a 10 3 -fold higher inhibitory potency towards human β-glucocerebrosidase in the Z as compared with the E isomeric form. This sharp contrast is compatible with ex-vivo activation and programmed self-deactivation at physiological temperatures, positioning it as a prime candidate for pharmacological chaperone therapy in Gaucher disease. Additionally, our results illustrate that chemical tailoring enables the engineering of photocommutators with the ability to toggle inhibition between α- and β-glucosidase enzymes in a reversible manner, thus expanding the versatility and potential therapeutic applications of this approach., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

3. Structural and dynamics insights into the GBA variants associated with Parkinson's disease.

Author

Mahmood A, Samad A, Bano S, Umair M, Ajmal A, Ilyas I, Shah AA, Li P, and Hu J

Subjects

Humans, Mutation, Ambroxol chemistry, Polymorphism, Single Nucleotide, Binding Sites, Protein Conformation, Structure-Activity Relationship, Hydrogen Bonding, Glucosylceramidase genetics, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Parkinson Disease genetics, Molecular Docking Simulation, Molecular Dynamics Simulation, Protein Binding

Abstract

The GBA1 gene encodes for the lysosomal enzyme glucocerebrosidase (GCase), which maintains glycosphingolipid homeostasis and regulates the autophagy process. Genomic variants of GBA1 are associated with Goucher disease; however, several heterozygous variants of GBA (E326K, T369M, N370S, L444P) are frequent high-risk factors for Parkinson's disease (PD). The underlying mechanism of these variants has been revealed through functional and patient-centered research, but the structural and dynamical aspects of these variants have not yet been thoroughly investigated. In the current study, we used a thorough computational method to pinpoint the structural changes that GBA underwent because of genomic variants and drug binding mechanisms. According to our findings, PD-linked nsSNP variants of GBA showed structural variation and abnormal dynamics when compared to wild-typ. The docking analysis demonstrated that the mutants E326K, N370S, and L444P have higher binding affinities for Ambroxol. Root means square deviation (RMSD), Root mean square fluctuation analysis (RMSF), and MM-GBSA analysis confirmed that the Ambroxol are more stable in the binding site of N370S and L444P, and that their binding affinities are stronger as compared to the wild-type and T369M variants of GBA. The evaluation of hydrogen bonds and the calculation of the free binding energy provided additional evidence in favor of this conclusion. When docked with Ambroxol, GBA demonstrated an increase in binding affinity and catalytic activity. Understanding the therapeutic efficacy and potential against the aforementioned changes in the GBA will be beneficial in order to use more efficient methods for developing novel drugs.

Published

2024

4. Fragment-Based Discovery of a Series of Allosteric-Binding Site Modulators of β-Glucocerebrosidase.

Author

Palmer N, Agnew C, Benn C, Buffham WJ, Castro JN, Chessari G, Clark M, Cons BD, Coyle JE, Dawson LA, Hamlett CCF, Hodson C, Holding F, Johnson CN, Liebeschuetz JW, Mahajan P, McCarthy JM, Murray CW, O'Reilly M, Peakman T, Price A, Rapti M, Reeks J, Schöpf P, St-Denis JD, Valenzano C, Wallis NG, Walser R, Weir H, Wilsher NE, Woodhead A, Bento CF, and Tisi D

Subjects

Humans, Crystallography, X-Ray, Structure-Activity Relationship, Models, Molecular, Small Molecule Libraries chemistry, Small Molecule Libraries pharmacology, Small Molecule Libraries metabolism, Glucosylceramidase metabolism, Glucosylceramidase antagonists & inhibitors, Glucosylceramidase chemistry, Drug Discovery, Allosteric Site

Abstract

β-Glucocerebrosidase (GBA/GCase) mutations leading to misfolded protein cause Gaucher's disease and are a major genetic risk factor for Parkinson's disease and dementia with Lewy bodies. The identification of small molecule pharmacological chaperones that can stabilize the misfolded protein and increase delivery of degradation-prone mutant GCase to the lysosome is a strategy under active investigation. Here, we describe the first use of fragment-based drug discovery (FBDD) to identify pharmacological chaperones of GCase. The fragment hits were identified by using X-ray crystallography and biophysical techniques. This work led to the discovery of a series of compounds that bind GCase with nM potency and positively modulate GCase activity in cells.

Published

2024

5. Gaucher Disease: A Glance from a Medicinal Chemistry Perspective.

Author

Prencipe F, Barzan C, Savian C, Spalluto G, Carosati E, De Amici M, Mosconi G, Gianferrara T, Federico S, and Da Ros T

Subjects

Humans, Glucosyltransferases antagonists & inhibitors, Glucosyltransferases metabolism, Chemistry, Pharmaceutical, Glucosylceramidase antagonists & inhibitors, Glucosylceramidase metabolism, Glucosylceramidase chemistry, Enzyme Replacement Therapy, Molecular Structure, Gaucher Disease drug therapy, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Enzyme Inhibitors chemical synthesis

Abstract

Rare diseases are particular pathological conditions affecting a limited number of people and few drugs are known to be effective as therapeutic treatment. Gaucher disease, caused by a deficiency of the lysosomal enzyme glucocerebrosidase, belongs to this class of disorders, and it is considered the most common among the Lysosomal Storage Diseases. The two main therapeutic approaches are the Enzyme Replacement Therapy (ERT) and the Substrate Reduction Therapy (SRT). ERT, consisting in replacing the defective enzyme by administering a recombinant enzyme, is effective in alleviating the visceral symptoms, hallmarks of the most common subtype of the disease whereas it has no effects when symptoms involve CNS, since the recombinant protein is unable to significantly cross the Blood Brain Barrier. The SRT strategy involves inhibiting glucosylceramide synthase (GCS), the enzyme responsible for the production of the associated storage molecule. The rational design of new inhibitors of GCS has been hampered by the lack of either the crystal structure of the enzyme or an in-silico model of the active site which could provide important information regarding the interactions of potential inhibitors with the target, but, despite this, interesting results have been obtained and are herein reviewed., (© 2024 Wiley-VCH GmbH.)

Published

2024

6. Identification of ß-Glucocerebrosidase Activators for Glucosylceramide hydrolysis.

Author

Schulze MED, Scholz D, Jnoff E, Hall A, Melin J, Sands ZA, Rodriguez E, and Andre VM

Subjects

Humans, Glucosylceramides, Hydrolysis, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Gaucher Disease drug therapy

Abstract

Several novel chemical series were identified that modulate glucocerebrosidase (GCase). Compounds from these series are active on glucosylceramide, unlike other known GCase modulators. We obtained GCase crystal structures with two compounds that have distinct chemotypes. Positive allosteric modulators bind to a site on GCase and induce conformational changes, but also induce an equilibrium state between monomer and dimer., (© 2024 Wiley‐VCH GmbH.)

Published

2024

7. Pharmacological Chaperones for GCase that Switch Conformation with pH Enhance Enzyme Levels in Gaucher Animal Models.

Author

Santana AG, Robinson K, Vickers C, Deen MC, Chen HM, Zhou S, Dai B, Fuller M, Boraston AB, Vocadlo DJ, Clarke LA, and Withers SG

Subjects

Animals, Hydrogen-Ion Concentration, Mice, Models, Animal, Molecular Chaperones chemistry, Mutation, Gaucher Disease drug therapy, Gaucher Disease genetics, Glucosylceramidase chemistry

Abstract

Gaucher disease is a lysosomal storage disorder caused by mutations which destabilize the native folded form of GCase, triggering degradation and ultimately resulting in low enzyme activity. Pharmacological chaperones (PCs) which stabilize mutant GCase have been used to increase lysosomal activity through improving trafficking efficiency. By engineering their inherent basicity, we have synthesized PCs that change conformation between the ER and the lysosomal environment, thus weakening binding to GCase after its successful trafficking to the lysosome. NMR studies confirmed the conformational change while X-ray data reveal bound conformations and binding modes. These results were further corroborated by cell studies showing increases in GCase activity when using the pH-switchable probe at low dosing. Preliminary in vivo assays with humanized mouse models of Gaucher showed enhanced GCase activity levels in relevant tissues, including the brain, further supporting their potential., (© 2022 Wiley-VCH GmbH.)

Published

2022

8. The interplay between Glucocerebrosidase, α-synuclein and lipids in human models of Parkinson's disease.

Author

Muñoz SS, Petersen D, Marlet FR, Kücükköse E, and Galvagnion C

Subjects

Glucosylceramidase chemistry, Humans, Models, Molecular, alpha-Synuclein chemistry, Glucosylceramidase metabolism, Lipids chemistry, Parkinson Disease metabolism, alpha-Synuclein metabolism

Abstract

Mutations in the gene GBA, encoding glucocerebrosidase (GCase), are the highest genetic risk factor for Parkinson's disease (PD). GCase is a lysosomal glycoprotein responsible for the hydrolysis of glucosylceramide into glucose and ceramide. Mutations in GBA cause a decrease in GCase activity, stability and protein levels which in turn lead to the accumulation of GCase lipid substrates as well as α-synuclein (αS) in vitro and in vivo. αS is the main constituent of Lewy bodies found in the brain of PD patients and an increase in its levels was found to be associated with a decrease in GCase activity/protein levels in vitro and in vivo. In this review, we describe the reported biophysical and biochemical changes that GBA mutations can induce in GCase activity and stability as well as the current overview of the levels of GCase protein/activity, αS and lipids measured in patient-derived samples including post-mortem brains, stem cell-derived neurons, cerebrospinal fluid, blood and fibroblasts as well as in SH-SY5Y cells. In particular, we report how the levels of αS and lipids are affected by/correlated to significant changes in GCase activity/protein levels and which cellular pathways are activated or disrupted by these changes in each model. Finally, we review the current strategies used to revert the changes in the levels of GCase activity/protein, αS and lipids in the context of PD., (Copyright © 2020 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2021

9. Novel β-Glucocerebrosidase Activators That Bind to a New Pocket at a Dimer Interface and Induce Dimerization.

Author

Benz J, Rufer AC, Huber S, Ehler A, Hug M, Topp A, Guba W, Hofmann EC, Jagasia R, and Rodríguez Sarmiento RM

Subjects

Binding Sites, Crystallography, X-Ray, Enzyme Activators chemistry, Glucosylceramidase chemistry, Humans, Kinetics, Molecular Structure, Protein Binding, Pyrazines chemistry, Pyrroles chemistry, Structure-Activity Relationship, Enzyme Activators metabolism, Glucosylceramidase metabolism, Protein Multimerization drug effects, Pyrazines metabolism, Pyrroles metabolism

Abstract

Genetic, preclinical and clinical data link Parkinson's disease and Gaucher's disease and provide a rational entry point to disease modification therapy via enhancement of β-Glucocerebrosidase (GCase) activity. We discovered a new class of pyrrolo[2,3-b]pyrazine activators effecting both Vmax and Km. They bind to human GCase and increase substrate metabolism in the lysosome in a cellular assay. We obtained the first crystal structure for an activator and identified a novel non-inhibitory binding mode at the interface of a dimer, rationalizing the observed structure-activity relationship (SAR). The compound binds GCase inducing formation of a dimeric state at both endoplasmic reticulum (ER) and lysosomal pHs, as confirmed by analytical ultracentrifugation. Importantly, the pyrrolo[2,3-b]pyrazines have central nervous system (CNS) drug-like properties. Our findings are important for future drug discovery efforts in the field of GCase activation and provide a deeper mechanistic understanding of the requirements for enzymatic activation, pointing to the relevance of dimerization., (© 2020 Wiley-VCH GmbH.)

Published

2021

10. Membrane Interactions of α-Synuclein Probed by Neutrons and Photons.

Author

Kaur U and Lee JC

Subjects

Amino Acid Sequence, Cell Membrane chemistry, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Humans, Lipid Bilayers chemistry, Lipid Bilayers metabolism, Neutrons, Phosphatidylcholines chemistry, Photons, Protein Aggregates, Protein Binding, alpha-Synuclein chemistry, Cell Membrane metabolism, alpha-Synuclein metabolism

Abstract

α-Synuclein (α-syn) is a key protein in the etiology of Parkinson's disease. In a disease state, α-syn accumulates as insoluble amyloid fibrils enriched in β-sheet structure. However, in its functional state, α-syn adopts an amphipathic helix upon membrane association and plays a role in synaptic vesicle docking, fusion, and clustering. In this Account, we describe our contributions made in the past decade toward developing a molecular understanding of α-syn membrane interactions, which are crucial for function and have pathological implications. Three topics are covered: α-syn membrane binding probed by neutron reflectometry (NR), the effects of membrane on α-syn amyloid formation, and interactions of α-syn with cellular membranes.NR offers a unique perspective by providing direct measurements of protein penetration depth. By the use of segmentally deuterated α-syn generated through native chemical ligation, the spatial resolution of specific membrane-bound polypeptide regions was determined by NR. Additionally, we used NR to characterize the membrane-bound complex of α-syn and glucocerebrosidase, a lysosomal hydrolase whose mutations are a common genetic risk factor for Parkinson's disease. Although phosphatidylcholine (PC) is the most abundant lipid species in mammalian cells, interactions of PC with α-syn have been largely ignored because they are substantially weaker compared with the electrostatically driven binding of negatively charged lipids. We discovered that α-syn tubulates zwitterionic PC membranes, which is likely related to its involvement in synaptic vesicle fusion by stabilization of membrane curvature. Interestingly, PC lipid tubules inhibit amyloid formation, in contrast to anionic phosphatidylglycerol lipid tubules, which stimulate protein aggregation. We also found that membrane fluidity influences the propensity of α-synuclein amyloid formation. Most recently, we obtained direct evidence of binding of α-syn to exocytic sites on intact cellular membranes using a method called cellular unroofing. This method provides direct access to the cytosolic plasma membrane. Importantly, measurements of fluorescence lifetime distributions revealed that α-syn is more conformationally dynamic at the membrane interface than previously appreciated. This exquisite responsiveness to specific lipid composition and membrane topology is important for both its physiological and pathological functions. Collectively, our work has provided insights into the effects of the chemical nature of phospholipid headgroups on the interplay among membrane remodeling, protein structure, and α-syn amyloid formation.

Published

2021

11. Parkinson's Clustering in Families of Non-Neuronopathic N370S GBA Mutation Carriers Indicates the Presence of Genetic Modifiers.

Author

Dinur T, Becker-Cohen M, Revel-Vilk S, Zimran A, and Arkadir D

Subjects

Cluster Analysis, Glucosylceramidase chemistry, Heterozygote, Humans, Glucosylceramidase genetics, Mutation genetics, Parkinson Disease epidemiology, Parkinson Disease genetics

Abstract

Low penetrance of Parkinson's disease (PD) associated with GBA pathogenic variants indicates the presence of modifiers genes. Clusters of PD cases in certain families with GBA variants would serve as a strong evidence for the clinical relevance of such modifiers. We studied eight family trees of non-Parkinsonian, GBA-N370S homozygote, Gaucher probands, with multiple cases of PD. Differences in PD risk associated with different GBA variants were balanced by variant homozygosity. In these families, all PD cases stemmed from only one of the proband's parents. This observation provides a direct epidemiological evidence for genetic modifiers determining PD risk in GBA variant carriers.

Published

2021

12. Functional Connectivity Analysis in Heterozygous Glucocerebrosidase Mutation Carriers.

Author

Sezgin M, Kicik A, Bilgic B, Kurt E, Bayram A, Hanagası H, Tepgec F, Toksoy G, Gurvit H, Uyguner O, Gokcay G, Demiralp T, and Emre M

Subjects

Glucosylceramidase genetics, Heterozygote, Humans, Mutation genetics, Gaucher Disease, Glucosylceramidase chemistry, Parkinson Disease

Abstract

Background: There is evidence that alterations in functional connectivity (FC) of the striatocortical circuits may appear before the onset of clinical symptoms of Parkinson's disease (PD)., Objective: The aim of this study was to investigate FC of the striatocortical circuitry in asymptomatic carriers of heterozygous glucocerebrosidase (GBA) mutations, which pose a significant risk for developing PD., Methods: Twenty-one parents of confirmed Gaucher disease patients who were carrying heterozygous GBA mutations and 18 healthy individuals matched for age and gender were included. GBA mutation analysis was performed in all participants. Clinical evaluation included neurological examination, Mini Mental State Examination, and UPDRS Part III. Structural and functional MRI data of 18 asymptomatic GBA mutation carriers (asGBAmc) and 17 healthy controls (HC) were available. FC was analyzed with seed-based approach., Results: Eleven asymptomatic mutation carriers had heterozygous p.L483P mutation, 6 subjects heterozygous p.N409S mutation and 1 subject heterozygous p.R392G mutation in GBA gene. Mini-Mental State Examination mean score was 28.77 (±1.16) and 29.64 (±0.70) in asGBAmc and HC groups, respectively (p = 0.012). Significant increased connectivityConclusion:Our results suggest that alterations in striatocortical FC can be detected in asymptomatic heterozygous GBA mutation carriers who are at risk of developing PD. These findings may provide insight into network changes during the asymptomatic phase of PD.

Published

2021

13. Dystonia as initial presentation of compound heterozygous GBA2 mutations: Expanding the phenotypic spectrum of SPG46.

Author

Kloth K, Cozma C, Bester M, Gerloff C, Biskup S, and Zittel S

Subjects

Adult, Cognitive Dysfunction pathology, Dystonia pathology, Female, Glucosylceramidase chemistry, Heterozygote, Humans, Pedigree, Spastic Paraplegia, Hereditary pathology, Cognitive Dysfunction genetics, Dystonia genetics, Glucosylceramidase genetics, Mutation, Phenotype, Spastic Paraplegia, Hereditary genetics

Abstract

GBA2 associated spastic paraplegia type 46 (SPG46) is an autosomal-recessive disorder associated with a clinical presentation of spastic gait, muscle weakness as well as an array of clinical symptoms including pseudobulbar palsy and progressive cognitive decline. Several neurological and non-neurological symptoms are associated with GBA2 mutations. An initial presentation with dystonia has not been reported so far. We report clinical, genetic and brain imaging findings in two siblings with hereditary spastic paraparesis. One sister presented with juvenile-onset leg spasticity and progressed to spastic tetraparesis, cervical and jaw opening dystonia, pseudobulbar symptoms and dementia. The other sister initially developed cervical dystonia in adulthood followed by gait spasticity and cognitive decline in the disease course. Molecular genetic testing revealed novel compound heterozygous variants in GBA2 in both sisters. The initial presentation with cervical dystonia and the differing clinical disease progression expand the clinical phenotype of GBA2 associated SPG46., (Copyright © 2020 Elsevier Masson SAS. All rights reserved.)

Published

2020

14. The biochemical basis of interactions between Glucocerebrosidase and alpha-synuclein in GBA1 mutation carriers.

Author

Toffoli M, Smith L, and Schapira AHV

Subjects

Genetic Predisposition to Disease genetics, Glucosylceramidase chemistry, Glucosylceramidase genetics, Heterozygote, Humans, Mutation, Parkinson Disease metabolism, Protein Structure, Quaternary, Glucosylceramidase metabolism, Parkinson Disease genetics, alpha-Synuclein metabolism

Abstract

The discovery of genes involved in familial as well as sporadic forms of Parkinson disease (PD) constitutes an important milestone in understanding this disorder's pathophysiology and potential treatment. Among these genes, GBA1 is one of the most common and well-studied, but it is still unclear how mutations in GBA1 translate into an increased risk for developing PD. In this review, we provide an overview of the biochemical and structural relationship between GBA1 and PD to help understand the recent advances in the development of PD therapies intended to target this pathway., (© 2020 International Society for Neurochemistry.)

Published

2020

15. Imino- and Azasugar Protonation Inside Human Acid β-Glucosidase, the Enzyme that is Defective in Gaucher Disease.

Author

Matassini C, Warren J, Wang B, Goti A, Cardona F, Morrone A, and Bols M

Subjects

Enzyme Assays, Fluorescent Dyes chemistry, Glucosylceramidase antagonists & inhibitors, Humans, Phenanthrenes chemistry, 1-Deoxynojirimycin analogs & derivatives, Enzyme Inhibitors chemistry, Glucosylceramidase chemistry, Imino Pyranoses chemistry, Protons

Abstract

Gaucher disease is caused by mutations in human acid β-glucosidase or glucocerebrosidase (GCase), the enzyme responsible for hydrolysis of glucosyl ceramide in the lysosomes. Imino- and azasugars such as 1-deoxynojirimycin and isofagomine are strong inhibitors of the enzyme and are of interest in pharmacological chaperone therapy of the disease. Despite several crystal structures of the enzyme with the imino- and azasugars bound in the active site having been resolved, the actual acid-base chemistry of the binding is not known. In this study we show, using photoinduced electron transfer (PET), that 1-deoxynojirimycin and isofagomine derivatives are protonated by human acid β-glucosidase when bound, even if they are completely unprotonated outside the enzyme. While isofagomine derivative protonation to some degree was foreshadowed by earlier crystal structures, 1-deoxynojirimycin derivatives were not believed to act as basic amines in the enzyme., (© 2020 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2020

16. A baculoviral system for the production of human β-glucocerebrosidase enables atomic resolution analysis.

Author

Rowland RJ, Wu L, Liu F, and Davies GJ

Subjects

Baculoviridae genetics, Cloning, Molecular methods, Humans, Ligands, Protein Binding, Protein Conformation, Glucosides metabolism, Glucosylceramidase biosynthesis, Glucosylceramidase chemistry, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry

Abstract

The lysosomal glycoside hydrolase β-glucocerebrosidase (GBA; sometimes called GBA1 or GC ase ) catalyses the hydrolysis of glycosphingolipids. Inherited deficiencies in GBA cause the lysosomal storage disorder Gaucher disease (GD). Consequently, GBA is of considerable medical interest, with continuous advances in the development of inhibitors, chaperones and activity-based probes. The development of new GBA inhibitors requires a source of active protein; however, the majority of structural and mechanistic studies of GBA today rely on clinical enzyme-replacement therapy (ERT) formulations, which are incredibly costly and are often difficult to obtain in adequate supply. Here, the production of active crystallizable GBA in insect cells using a baculovirus expression system is reported, providing a nonclinical source of recombinant GBA with comparable activity and biophysical properties to ERT preparations. Furthermore, a novel crystal form of GBA is described which diffracts to give a 0.98 Å resolution unliganded structure. A structure in complex with the inactivator 2,4-dinitrophenyl-2-deoxy-2-fluoro-β-D-glucopyranoside was also obtained, demonstrating the ability of this GBA formulation to be used in ligand-binding studies. In light of its purity, stability and activity, the GBA production protocol described here should circumvent the need for ERT formulations for structural and biochemical studies and serve to support GD research., (open access.)

Published

2020

17. Recombinant β-Glucocerebrosidase specific immunoaffinity ligands selected from phage-displayed combinatorial scFv libraries.

Author

Anisimov RL, Ershova OA, Ershov AV, Filatova MA, Katorkin SA, and Simonov VM

Subjects

Animals, Antibody Specificity, CHO Cells, Cricetulus, Enzyme Assays, Enzymes, Immobilized chemistry, Enzymes, Immobilized immunology, Ethylene Glycol chemistry, Glucosides chemistry, Glucosylceramidase chemistry, Glucosylceramidase immunology, Humans, Kinetics, Ligands, Polystyrenes chemistry, Protein Binding, Recombinant Proteins chemistry, Recombinant Proteins immunology, Recombinant Proteins isolation & purification, Single-Chain Antibodies biosynthesis, Single-Chain Antibodies chemistry, Chromatography, Affinity methods, Enzymes, Immobilized isolation & purification, Glucosylceramidase isolation & purification, Peptide Library, Single-Chain Antibodies isolation & purification

Abstract

Antibodies specific to β-Glucocerebrosidase were selected from phage displayed naïve scFv libraries. Biopannings were performed against recombinant human protein β-Glucocerebrosidase immobilized on polystyrene surface, specific phages were eluted with 50% ethylene glycol in citrate buffer (pH 6.0). Several specific binders were discovered and converted to full-size hIgG1 antibodies leading to highly stable binders with dissociation constants (Kd) in the range 10-40 nM. The antibodies were used further as ligands for affinity chromatography, where efficient and selective recovery of biologically active β-Glucocerebrosidase from cultured media of Chinese hamster ovary cells was demonstrated. β-Glucocerebrosidase was purified to nearly homogeneous state and had specific activity comparable to the commercially available preparations (40-44 U/mg protein). The obtained immunoaffinity sorbents have high capacity and can be easily regenerated., (Copyright © 2020. Published by Elsevier Inc.)

Published

2020

18. The Arabidopsis At GCD3 protein is a glucosylceramidase that preferentially hydrolyzes long-acyl-chain glucosylceramides.

Author

Dai GY, Yin J, Li KE, Chen DK, Liu Z, Bi FC, Rong C, and Yao N

Subjects

1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin pharmacology, Animals, Arabidopsis metabolism, Arabidopsis Proteins antagonists & inhibitors, Arabidopsis Proteins chemistry, Biosynthetic Pathways drug effects, Glucosylceramidase antagonists & inhibitors, Glucosylceramidase chemistry, Glucosylceramides genetics, Humans, Metabolism drug effects, Microtubule-Associated Proteins antagonists & inhibitors, Microtubule-Associated Proteins chemistry, Plant Leaves metabolism, Recombinant Proteins chemistry, Recombinant Proteins genetics, Signal Transduction drug effects, Sphingolipids metabolism, Arabidopsis genetics, Arabidopsis Proteins genetics, Glucosylceramidase genetics, Glucosylceramides metabolism, Microtubule-Associated Proteins genetics

Abstract

Cellular membranes contain many lipids, some of which, such as sphingolipids, have important structural and signaling functions. The common sphingolipid glucosylceramide (GlcCer) is present in plants, fungi, and animals. As a major plant sphingolipid, GlcCer is involved in the formation of lipid microdomains, and the regulation of GlcCer is key for acclimation to stress. Although the GlcCer biosynthetic pathway has been elucidated, little is known about GlcCer catabolism, and a plant GlcCer-degrading enzyme (glucosylceramidase (GCD)) has yet to be identified. Here, we identified AtGCD3 , one of four Arabidopsis thaliana homologs of human nonlysosomal glucosylceramidase, as a plant GCD. We found that recombinant At GCD3 has a low K m for the fluorescent lipid C 6 -NBD GlcCer and preferentially hydrolyzes long acyl-chain GlcCer purified from Arabidopsis leaves. Testing of inhibitors of mammalian glucosylceramidases revealed that a specific inhibitor of human β-glucosidase 2, N -butyldeoxynojirimycin, inhibits At GCD3 more effectively than does a specific inhibitor of human β-glucosidase 1, conduritol β-epoxide. We also found that Glu-499 and Asp-647 in At GCD3 are vital for GCD activity. GFP- At GCD3 fusion proteins mainly localized to the plasma membrane or the endoplasmic reticulum membrane. No obvious growth defects or changes in sphingolipid contents were observed in gcd3 mutants. Our results indicate that At GCD3 is a plant glucosylceramidase that participates in GlcCer catabolism by preferentially hydrolyzing long-acyl-chain GlcCers., (© 2020 Dai et al.)

Published

2020

19. Scaffolds for Sustained Release of Ambroxol Hydrochloride, a Pharmacological Chaperone That Increases the Activity of Misfolded β-Glucocerebrosidase.

Author

Enshaei H, Molina BG, Del Valle LJ, Estrany F, Arnan C, Puiggalí J, Saperas N, and Alemán C

Subjects

Ambroxol pharmacology, Drug Compounding methods, Drug Liberation, Electrochemical Techniques, Hot Temperature, Kinetics, Protective Agents pharmacology, Protein Folding drug effects, Protein Stability, Ambroxol chemistry, Delayed-Action Preparations chemistry, Glucosylceramidase chemistry, Polyesters chemistry, Protective Agents chemistry

Abstract

Ambroxol is a pharmacological chaperone (PC) for Gaucher disease that increases lysosomal activity of misfolded β-glucocerebrosidase (GCase) while displaying a safe toxicological profile. In this work, different poly(ε-caprolactone) (PCL)-based systems are developed to regulate the sustained release of small polar drugs in physiological environments. For this purpose, ambroxol is selected as test case since the encapsulation and release of PCs using polymeric scaffolds have not been explored yet. More specifically, ambroxol is successfully loaded in electrospun PCL microfibers, which are subsequently coated with additional PCL layers using dip-coating or spin-coating. The time needed to achieve 80% release of loaded ambroxol increases from ≈15 min for uncoated fibrous scaffolds to 3 days and 1 week for dip-coated and spin-coated systems, respectively. Furthermore, it is proven that the released drug maintains its bioactivity, protecting GCase against induced thermal denaturation., (© 2019 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

20. Mechanism of glucocerebrosidase activation and dysfunction in Gaucher disease unraveled by molecular dynamics and deep learning.

Author

Romero R, Ramanathan A, Yuen T, Bhowmik D, Mathew M, Munshi LB, Javaid S, Bloch M, Lizneva D, Rahimova A, Khan A, Taneja C, Kim SM, Sun L, New MI, Haider S, and Zaidi M

Subjects

Catalytic Domain, Enzyme Activation, Glucosylceramidase chemistry, Humans, Hydrogen Bonding, Mutant Proteins chemistry, Protein Interaction Maps, Protein Structure, Secondary, Saposins metabolism, Deep Learning, Gaucher Disease enzymology, Gaucher Disease physiopathology, Glucosylceramidase metabolism, Molecular Dynamics Simulation

Abstract

The lysosomal enzyme glucocerebrosidase-1 (GCase) catalyzes the cleavage of a major glycolipid glucosylceramide into glucose and ceramide. The absence of fully functional GCase leads to the accumulation of its lipid substrates in lysosomes, causing Gaucher disease, an autosomal recessive disorder that displays profound genotype-phenotype nonconcordance. More than 250 disease-causing mutations in GBA1 , the gene encoding GCase, have been discovered, although only one of these, N370S, causes 70% of disease. Here, we have used a knowledge-based docking protocol that considers experimental data of protein-protein binding to generate a complex between GCase and its known facilitator protein saposin C (SAPC). Multiscale molecular-dynamics simulations were used to study lipid self-assembly, membrane insertion, and the dynamics of the interactions between different components of the complex. Deep learning was applied to propose a model that explains the mechanism of GCase activation, which requires SAPC. Notably, we find that conformational changes in the loops at the entrance of the substrate-binding site are stabilized by direct interactions with SAPC and that the loss of such interactions induced by N370S and another common mutation, L444P, result in destabilization of the complex and reduced GCase activation. Our findings provide an atomistic-level explanation for GCase activation and the precise mechanism through which N370S and L444P cause Gaucher disease., Competing Interests: The authors declare no conflict of interest.

Published

2019

21. Gaucher disease: single gene molecular characterization of one-hundred Indian patients reveals novel variants and the most prevalent mutation.

Author

Sheth J, Bhavsar R, Mistri M, Pancholi D, Bavdekar A, Dalal A, Ranganath P, Girisha KM, Shukla A, Phadke S, Puri R, Panigrahi I, Kaur A, Muranjan M, Goyal M, Ramadevi R, Shah R, Nampoothiri S, Danda S, Datar C, Kapoor S, Bhatwadekar S, and Sheth F

Subjects

Adolescent, Adult, Amino Acid Substitution, Child, Child, Preschool, Exons, Female, Gaucher Disease metabolism, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Humans, India, Infant, Infant, Newborn, Male, Models, Molecular, Structural Homology, Protein, Young Adult, Gaucher Disease genetics, Glucosylceramidase genetics, Mutation, Sequence Analysis, DNA methods, White People genetics

Abstract

Background: Gaucher disease is a rare pan-ethnic, lysosomal storage disorder resulting due to beta-Glucosidase (GBA1) gene defect. This leads to the glucocerebrosidase enzyme deficiency and an increased accumulation of undegraded glycolipid glucocerebroside inside the cells' lysosomes. To date, nearly 460 mutations have been described in the GBA1 gene. With the aim to determine mutations spectrum and molecular pathology of Gaucher disease in India, the present study investigated one hundred unrelated patients (age range: 1 day to 31 years) having splenomegaly, with or without hepatomegaly, cytopenia and bone abnormality in some of the patients., Methods: The biochemical investigation for the plasma chitotriosidase enzyme activity and β-Glucosidase enzyme activity confirmed the Gaucher disease. The mutations were identified by screening the patients' whole GBA gene coding region using bidirectional Sanger sequencing., Results: The biochemical analysis revealed a significant reduction in the β-Glucosidase activity in all patients. Sanger sequencing established 71 patients with homozygous mutation and 22 patients with compound heterozygous mutation in GBA1 gene. Lack of identification of mutations in three patients suggests the possibility of either large deletion/duplication or deep intronic variations in the GBA1 gene. In four cases, where the proband died due to confirmed Gaucher disease, the parents were found to be a carrier. Overall, the study identified 33 mutations in 100 patients that also covers four missense mutations (p.Ser136Leu, p.Leu279Val, p.Gly383Asp, p.Gly399Arg) not previously reported in Gaucher disease patients. The mutation p.Leu483Pro was identified as the most commonly occurring Gaucher disease mutation in the study (62% patients). The second common mutations identified were p.Arg535Cys (7% patients) and RecNcil (7% patients). Another complex mutation Complex C was identified in a compound heterozygous status (3% patients). The homology modeling of the novel mutations suggested the destabilization of the GBA protein structure due to conformational changes., Conclusions: The study reports four novel and 29 known mutations identified in the GBA1 gene in one-hundred Gaucher patients. The given study establishes p.Leu483Pro as the most prevalent mutation in the Indian patients with type 1 Gaucher disease that provide new insight into the molecular basis of Gaucher Disease in India.

Published

2019

22. The heat shock protein amplifier arimoclomol improves refolding, maturation and lysosomal activity of glucocerebrosidase.

Author

Fog CK, Zago P, Malini E, Solanko LM, Peruzzo P, Bornaes C, Magnoni R, Mehmedbasic A, Petersen NHT, Bembi B, Aerts JFMG, Dardis A, and Kirkegaard T

Subjects

Cell Line, Endoplasmic Reticulum metabolism, Enzyme Activation drug effects, Fibroblasts drug effects, Fibroblasts metabolism, Gaucher Disease genetics, Gaucher Disease metabolism, Glucosylceramidase genetics, Golgi Apparatus metabolism, Heat-Shock Proteins metabolism, Humans, Mutation, Neurons, Protein Processing, Post-Translational, Protein Transport, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Hydroxylamines pharmacology, Lysosomes metabolism, Protein Refolding drug effects

Abstract

Background: Gaucher Disease is caused by mutations of the GBA gene which encodes the lysosomal enzyme acid beta-glucosidase (GCase). GBA mutations commonly affect GCase function by perturbing its protein homeostasis rather than its catalytic activity. Heat shock proteins are well known cytoprotective molecules with functions in protein homeostasis and lysosomal function and their manipulation has been suggested as a potential therapeutic strategy for GD. The investigational drug arimoclomol, which is in phase II/III clinical trials, is a well-characterized HSP amplifier and has been extensively clinically tested. Importantly, arimoclomol efficiently crosses the blood-brain-barrier presenting an opportunity to target the neurological manifestations of GD, which remains without a disease-modifying therapy., Methods: We used a range of biological and biochemical in vitro assays to assess the effect of arimoclomol on GCase activity in ex vivo systems of primary fibroblasts and neuronal-like cells from GD patients., Findings: We found that arimoclomol induced relevant HSPs such as ER-resident HSP70 (BiP) and enhanced the folding, maturation, activity, and correct cellular localization of mutated GCase across several genotypes including the common L444P and N370S mutations in primary cells from GD patients. These effects where recapitulated in a human neuronal model of GD obtained by differentiation of multipotent adult stem cells., Interpretation: These data demonstrate the potential of HSP-targeting therapies in GCase-deficiencies and strongly support the clinical development of arimoclomol as a potential therapeutic option for the neuronopathic forms of GD., Funding: The research was funded by Orphazyme A/S, Copenhagen, Denmark., (Copyright © 2018 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2018

23. Distinguishing the differences in β-glycosylceramidase folds, dynamics, and actions informs therapeutic uses.

Author

Ben Bdira F, Artola M, Overkleeft HS, Ubbink M, and Aerts JMFG

Subjects

Animals, Cerebrosides metabolism, Gaucher Disease metabolism, Glycoconjugates metabolism, Glycolipids metabolism, Humans, Lactase-Phlorizin Hydrolase metabolism, Parkinson Disease metabolism, Glucosylceramidase chemistry, Glucosylceramidase metabolism

Abstract

Glycosyl hydrolases (GHs) are carbohydrate-active enzymes that hydrolyze a specific β-glycosidic bond in glycoconjugate substrates; β-glucosidases degrade glucosylceramide, a ubiquitous glycosphingolipid. GHs are grouped into structurally similar families that themselves can be grouped into clans. GH1, GH5, and GH30 glycosidases belong to clan A hydrolases with a catalytic (β/α) 8 TIM barrel domain, whereas GH116 belongs to clan O with a catalytic (α/α) 6 domain. In humans, GH abnormalities underlie metabolic diseases. The lysosomal enzyme glucocerebrosidase (family GH30), deficient in Gaucher disease and implicated in Parkinson disease etiology, and the cytosol-facing membrane-bound glucosylceramidase (family GH116) remove the terminal glucose from the ceramide lipid moiety. Here, we compare enzyme differences in fold, action, dynamics, and catalytic domain stabilization by binding site occupancy. We also explore other glycosidases with reported glycosylceramidase activity, including human cytosolic β-glucosidase, intestinal lactase-phlorizin hydrolase, and lysosomal galactosylceramidase. Last, we describe the successful translation of research to practice: recombinant glycosidases and glucosylceramide metabolism modulators are approved drug products (enzyme replacement therapies). Activity-based probes now facilitate the diagnosis of enzyme deficiency and screening for compounds that interact with the catalytic pocket of glycosidases. Future research may deepen the understanding of the functional variety of these enzymes and their therapeutic potential., (Copyright © 2018 Ben Bdira et al.)

Published

2018

24. Design of a New α-1- C -Alkyl-DAB Derivative Acting as a Pharmacological Chaperone for β-Glucocerebrosidase Using Ligand Docking and Molecular Dynamics Simulation.

Author

Nakagome I, Kato A, Yamaotsu N, Yoshida T, Ozawa SI, Adachi I, and Hirono S

Subjects

Binding Sites, Enzyme Stability drug effects, Glucosylceramidase chemistry, Humans, Imino Sugars therapeutic use, Ligands, Molecular Chaperones chemistry, Molecular Docking Simulation, Molecular Dynamics Simulation, Mutant Proteins chemistry, Point Mutation, Protein Binding, Sugar Alcohols antagonists & inhibitors, Sugar Alcohols therapeutic use, Gaucher Disease drug therapy, Glucosylceramidase antagonists & inhibitors, Imino Sugars chemistry, Sugar Alcohols chemistry

Abstract

Some point mutations in β-glucocerebrosidase cause either improper folding or instability of this protein, resulting in Gaucher disease. Pharmacological chaperones bind to the mutant enzyme and stabilize this enzyme; thus, pharmacological chaperone therapy was proposed as a potential treatment for Gaucher disease. The binding affinities of α-1- C -alkyl 1,4-dideoxy-1,4-imino-d-arabinitol (DAB) derivatives, which act as pharmacological chaperones for β-glucocerebrosidase, abruptly increased upon elongation of their alkyl chain. In this study, the primary causes of such an increase in binding affinity were analyzed using protein⁻ligand docking and molecular dynamics simulations. We found that the activity cliff between α-1- C -heptyl-DAB and α-1- C -octyl-DAB was due to the shape and size of the hydrophobic binding site accommodating the alkyl chains, and that the interaction with this hydrophobic site controlled the binding affinity of the ligands well. Furthermore, based on the aromatic/hydrophobic properties of the binding site, a 7-(tetralin-2-yl)-heptyl-DAB compound was designed and synthesized. This compound had significantly enhanced activity. The design strategy in consideration of aromatic interactions in the hydrophobic pocket was useful for generating effective pharmacological chaperones for the treatment of Gaucher disease.

Published

2018

25. The Production of Human β-Glucocerebrosidase in Nicotiana benthamiana Root Culture.

Author

Naphatsamon U, Ohashi T, Misaki R, and Fujiyama K

Subjects

Concanavalin A chemistry, Culture Media chemistry, Gaucher Disease enzymology, Glucosylceramidase chemistry, Glucosylceramidase genetics, Humans, Indoleacetic Acids pharmacology, Plant Roots cytology, Plant Roots drug effects, Plants, Genetically Modified enzymology, Plants, Genetically Modified genetics, Recombinant Proteins biosynthesis, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins isolation & purification, Time Factors, Nicotiana genetics, Glucosylceramidase biosynthesis, Glucosylceramidase isolation & purification, Plant Roots enzymology, Nicotiana enzymology

Abstract

Gaucher disease is caused by a deficiency of the enzyme glucocerebrosidase (GCase). Currently, enzyme-replacement therapy using recombinant GCase produced in mammalian cells is considered the most effective treatment. Plants are an attractive alternative host for recombinant protein production due to the low cost of large-scale production and lack of risk of contamination by human pathogens. Compared to whole plants, root cultures can grow faster. Therefore, this study aimed to produce recombinant GCase in a Nicotiana benthamiana root culture. Root culture of a GCase-producing transgenic plant was induced by indole-3-acetic acid at the concentration of 1 mg/L. Recombinant GCase was successfully produced in roots as a functional protein with an enzyme activity equal to 81.40 ± 17.99 units/mg total protein. Crude proteins were extracted from the roots. Recombinant GCase could be purified by concanavalin A and phenyl 650C chromatography. The productivity of GCase was approximately 1 µg/g of the root. A N -glycan analysis of purified GCase was performed using nano LC/MS. The Man₃XylFucGlcNAc₂ structure was predominant in purified GCase with two plant-specific glycan residues. This study presents evidence for a new, safe and efficient system of recombinant GCase production that might be applied to other recombinant proteins.

Published

2018

26. β-Glucocerebrosidase Modulators Promote Dimerization of β-Glucocerebrosidase and Reveal an Allosteric Binding Site.

Author

Zheng J, Chen L, Skinner OS, Ysselstein D, Remis J, Lansbury P, Skerlj R, Mrosek M, Heunisch U, Krapp S, Charrow J, Schwake M, Kelleher NL, Silverman RB, and Krainc D

Subjects

Crystallography, X-Ray, Fibroblasts metabolism, Glucosylceramidase genetics, HEK293 Cells, Humans, Mass Spectrometry, Models, Molecular, Molecular Structure, Mutation, Allosteric Site drug effects, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Protein Multimerization drug effects

Abstract

β-Glucocerebrosidase (GCase) mutations cause Gaucher's disease and are a high risk factor in Parkinson's disease. The implementation of a small molecule modulator is a strategy to restore proper folding and lysosome delivery of degradation-prone mutant GCase. Here, we present a potent quinazoline modulator, JZ-4109, which stabilizes wild-type and N370S mutant GCase and increases GCase abundance in patient-derived fibroblast cells. We then developed a covalent modification strategy using a lysine targeted inactivator (JZ-5029) for in vitro mechanistic studies. By using native top-down mass spectrometry, we located two potentially covalently modified lysines. We obtained the first crystal structure, at 2.2 Å resolution, of a GCase with a noniminosugar modulator covalently bound, and were able to identify the exact lysine residue modified (Lys346) and reveal an allosteric binding site. GCase dimerization was induced by our modulator binding, which was observed by native mass spectrometry, its crystal structure, and size exclusion chromatography with a multiangle light scattering detector. Finally, the dimer form was confirmed by negative staining transmission electron microscopy studies. Our newly discovered allosteric site and observed GCase dimerization provide a new mechanistic insight into GCase and its noniminosugar modulators and facilitate the rational design of novel GCase modulators for Gaucher's disease and Parkinson's disease.

Published

2018

27. Enzymes as Immunotherapeutics.

Author

Farhadi SA, Bracho-Sanchez E, Freeman SL, Keselowsky BG, and Hudalla GA

Subjects

Animals, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents immunology, Anti-Inflammatory Agents therapeutic use, Antineoplastic Agents chemistry, Antineoplastic Agents immunology, Antineoplastic Agents therapeutic use, Asparaginase chemistry, Asparaginase immunology, Asparaginase therapeutic use, Biocatalysis, Enzymes, Immobilized chemistry, Enzymes, Immobilized immunology, Enzymes, Immobilized therapeutic use, Fabry Disease immunology, Fabry Disease therapy, Gaucher Disease immunology, Gaucher Disease therapy, Glucosylceramidase chemistry, Glucosylceramidase immunology, Glucosylceramidase therapeutic use, Glycosylation, Humans, Immunoconjugates chemistry, Immunoconjugates immunology, Immunoconjugates therapeutic use, Inflammation immunology, Inflammation therapy, Lysosomal Storage Diseases immunology, Lysosomal Storage Diseases therapy, Neoplasms immunology, Neoplasms therapy, alpha-Galactosidase chemistry, alpha-Galactosidase immunology, alpha-Galactosidase therapeutic use, Enzyme Therapy methods, Immunotherapy methods

Abstract

Enzymes are attractive as immunotherapeutics because they can catalyze shifts in the local availability of immunostimulatory and immunosuppressive signals. Clinical success of enzyme immunotherapeutics frequently hinges upon achieving sustained biocatalysis over relevant time scales. The time scale and location of biocatalysis are often dictated by the location of the substrate. For example, therapeutic enzymes that convert substrates distributed systemically are typically designed to have a long half-life in circulation, whereas enzymes that convert substrates localized to a specific tissue or cell population can be more effective when designed to accumulate at the target site. This Topical Review surveys approaches to improve enzyme immunotherapeutic efficacy via chemical modification, encapsulation, and immobilization that increases enzyme accumulation at target sites or extends enzyme half-life in circulation. Examples provided illustrate "replacement therapies" to restore deficient enzyme function, as well as "enhancement therapies" that augment native enzyme function via supraphysiologic doses. Existing FDA-approved enzyme immunotherapies are highlighted, followed by discussion of emerging experimental strategies such as those designed to enhance antitumor immunity or resolve inflammation.

Published

2018

28. Clinical and molecular characteristics of patients with Gaucher disease in Southern China.

Author

Feng Y, Huang Y, Tang C, Hu H, Zhao X, Sheng H, Zhang W, Tan M, Xie T, Zheng J, Liu Z, Su X, Shao Y, Li X, Cheng J, Mao X, and Liu L

Subjects

Adolescent, Adult, Aged, Animals, Asian People genetics, COS Cells, Child, Child, Preschool, China epidemiology, Chlorocebus aethiops, Female, Gaucher Disease epidemiology, Genotype, Glucosylceramidase chemistry, Homozygote, Humans, Infant, Male, Middle Aged, Models, Molecular, Mutation, Missense, Point Mutation, Protein Conformation, Young Adult, Gaucher Disease genetics, Glucosylceramidase genetics, Mutation

Abstract

Gaucher disease (GD) is a common lysosomal storage disorder caused by the deficiency of acid β-glucosidase, due to mutations in the GBA gene. To explore the clinical and molecular characteristics of GD patients from Southern China, GBA gene were analyzed by nest PCR and direct Sanger-sequencing. Novel missense mutations were transiently transfected in COS-7 cells by plasmid system for functional verification. Among the 22 GD patients, 19 patients were classified as type 1 and three as type 2. Over 60% of the type 1 patient had the onset before two years of age and about 42% of them died before three years of age. Six type 1 patients with L444P homozygous genotype, presented with early onset and severe hepatosplenomegaly. Four novel mutations Y22C, F109L, L149F and c.983_990delCCCACTGG were identified. The GBA activities in vitro of novel mutants Y22C, F109L and L149F were 20.2%, 6.9% and 6.5% of the wild-type, respectively. L444P mutation accounted for 47.7% of the mutant alleles. Our results revealed that type 1 GD tends to present with a severe phenotype among southern Chinese. L444P was the most prevalent mutation and L444P homozygous genotype was associated with severe type 1 GD. Three novel missense mutations identified were pathogenic., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2018

29. Investigation of novel pharmacological chaperones for Gaucher Disease.

Author

Yilmazer B, Yagci ZB, Bakar E, Ozden B, Ulgen K, and Ozkirimli E

Subjects

Binding Sites, Catalytic Domain, Computer Simulation, Drug Discovery, Gaucher Disease, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Humans, Ligands, Models, Molecular, Molecular Conformation, Molecular Docking Simulation, Molecular Dynamics Simulation, Protein Binding, Structure-Activity Relationship, Molecular Chaperones chemistry, Pharmaceutical Preparations chemistry

Abstract

Beta-Glucocerebrosidase (GBA) is a lysosomal protein that is responsible for the hydrolysis of glycosylceramide into glucose and ceramide. Mutations in GBA lead to the accumulation of glycosylceramide in the lysosome causing an enlargement of the spleen and the liver and skeletal deformations. This disease is called Gaucher Disease. Enzyme replacement therapies and substrate reduction methods that are used to treat Gaucher Disease fail when the disease is neuropathic because they fail to pass the blood brain barrier. In this work, QSAR, virtual screening, docking and molecular dynamics simulations were performed to obtain a set of compounds that might be pharmacological chaperones for GBA. ZINC Database was screened using ligand-based and structure-based pharmacophore hypotheses. After docking of these molecules and filtration based on druglikeness, top ranking ligands were identified and their binding stabilities were examined using MD simulations. As a result, seven new compounds that can potentially cross the blood brain barrier were proposed as GBA inhibitors. Three of the seven compounds have a tricyclic pyrido-thieno-pyrimidine scaffold and one has the dioxino quinolone scaffold. Derivatives of these scaffolds have been reported as antiallergic agents, antibiotic and anticancer compounds. These results offer a new approach for the development of new drugs against neuropathic Gaucher Disease Type 2 and Type 3., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

30. Stabilization of Glucocerebrosidase by Active Site Occupancy.

Author

Ben Bdira F, Kallemeijn WW, Oussoren SV, Scheij S, Bleijlevens B, Florea BI, van Roomen CPAA, Ottenhoff R, van Kooten MJFM, Walvoort MTC, Witte MD, Boot RG, Ubbink M, Overkleeft HS, and Aerts JMFG

Subjects

Animals, Binding Sites, Enzyme Stability drug effects, Imino Pyranoses chemistry, Imino Pyranoses pharmacology, Liver drug effects, Liver enzymology, Mice, Molecular Structure, Temperature, Catalytic Domain physiology, Enzyme Stability physiology, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Imino Pyranoses metabolism

Abstract

Glucocerebrosidase (GBA) is a lysosomal β-glucosidase that degrades glucosylceramide. Its deficiency results in Gaucher disease (GD). We examined the effects of active site occupancy of GBA on its structural stability. For this, we made use of cyclophellitol-derived activity-based probes (ABPs) that bind irreversibly to the catalytic nucleophile (E340), and for comparison, we used the potent reversible inhibitor isofagomine. We demonstrate that cyclophellitol ABPs improve the stability of GBA in vitro, as revealed by thermodynamic measurements (T m increase by 21 °C), and introduce resistance to tryptic digestion. The stabilizing effect of cell-permeable cyclophellitol ABPs is also observed in intact cultured cells containing wild-type GBA, N370S GBA (labile in lysosomes), and L444P GBA (exhibits impaired ER folding): all show marked increases in lysosomal forms of GBA molecules upon exposure to ABPs. The same stabilization effect is observed for endogenous GBA in the liver of wild-type mice injected with cyclophellitol ABPs. Stabilization effects similar to those observed with ABPs were also noted at high concentrations of the reversible inhibitor isofagomine. In conclusion, we provide evidence that the increase in cellular levels of GBA by ABPs and by the reversible inhibitor is in part caused by their ability to stabilize GBA folding, which increases the resistance of GBA against breakdown by lysosomal proteases. These effects are more pronounced in the case of the amphiphilic ABPs, presumably due to their high lipophilic potential, which may promote further structural compactness of GBA through hydrophobic interactions. Our study provides further rationale for the design of chaperones for GBA to ameliorate Gaucher disease.

Published

2017

31. Stereodivergent synthesis of right- and left-handed iminoxylitol heterodimers and monomers. Study of their impact on β-glucocerebrosidase activity.

Author

Stauffert F, Serra-Vinardell J, Gómez-Grau M, Michelakakis H, Mavridou I, Grinberg D, Vilageliu L, Casas J, Bodlenner A, Delgado A, and Compain P

Subjects

Catalytic Domain, Chemistry Techniques, Synthetic, Enzyme Inhibitors chemistry, Fibroblasts drug effects, Fibroblasts enzymology, Gaucher Disease enzymology, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Humans, Protein Transport, Stereoisomerism, Xylitol chemistry, Dimerization, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Glucosylceramidase antagonists & inhibitors, Xylitol chemical synthesis, Xylitol pharmacology

Abstract

A library of dimers and heterodimers of both enantiomers of 2-O-alkylated iminoxylitol derivatives has been synthesised and evaluated on β-glucocerebrosidase (GCase), the enzyme responsible for Gaucher disease (GD). Although the objective was to target simultaneously the active site and a secondary binding site of the glucosidase, the (-)-2-iminoxylitol moiety seemed detrimental for imiglucerase inhibition and no significant enhancement was obtained in G202R, N370S and L444P fibroblasts. However, all compounds having at least one (+)-2-O-alkyl iminoxylitol are GCase inhibitors in the nano molar range and are significant GCase activity enhancers in G202R fibroblats, as confirmed by a decrease of glucosylceramide levels and by co-localization studies.

Published

2017

32. The metabolism of glucocerebrosides - From 1965 to the present.

Author

Futerman AH and Platt FM

Subjects

Enzyme Replacement Therapy methods, Gaucher Disease genetics, Gaucher Disease metabolism, Glucosylceramidase chemistry, History, 20th Century, History, 21st Century, Humans, Mutation, Protein Structure, Tertiary, Gaucher Disease drug therapy, Glucosylceramidase genetics, Glucosylceramides metabolism

Abstract

Gaucher disease is caused by the defective catabolism of the simple glycosphingolipid, glucosylceramide (GlcCer), due to mutations in the GBA1 gene which encodes for acid β-glucosidase (GCase), the lysosomal enzyme that degrades GlcCer. Today, Gaucher disease patients are routinely treated with recombinant GCase, in a treatment regimen known as enzyme replacement therapy (ERT). We now review the biochemical basis of ERT and discuss how this treatment has advanced since it was first pioneered by Dr. Roscoe Brady in the 1960s. We will place particular emphasis on the three dimensional structure of GCase, and subsequently discuss a relatively new treatment paradigm, substrate reduction therapy (SRT), in which GlcCer synthesis is partially inhibited, thus reducing its accumulation. Both of these approaches are based on studies and concepts developed by Dr. Brady over his remarkable research career spanning six decades., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2017

33. New Directions in Gaucher Disease.

Author

Horowitz M, Elstein D, Zimran A, and Goker-Alpan O

Subjects

Age of Onset, Animals, Cell Line, Gaucher Disease complications, Glucosylceramidase chemistry, Humans, Mitophagy, Mutation, Protein Folding, Unfolded Protein Response, Gaucher Disease classification, Gaucher Disease genetics, Glucosylceramidase genetics, Parkinson Disease genetics

Abstract

In Gaucher disease (GD), mutant lysosomal acid β-glucocerebrosidase fails to properly hydrolyze its substrate, glucosylceramide, which accumulates in the lysosomes. Due to its phenotypic heterogeneity, GD has been classified into type 1, non-neuronopathic, and types 2 and 3, the neuronopathic forms, based on the primary involvement of the central nervous system. Neuroinflammation and necroptotic death may appear in the neuronopathic forms of GD, whereas type 1 GD patients may develop Parkinson disease (PD), a prototype of protein misfolding disorders of the nervous system. PD is significantly more prevalent among GD carriers and patients than among the non-GD populations. It is apparent that the amount of mutant enzyme present in lysosomes depends on the amount of mutant enzyme recognized as correctly folded in the endoplasmic reticulum (ER) for physiologically correct transport through the Golgi apparatus to the lysosome. Mutant enzyme recognized as misfolded is retained in the ER, inducing the Unfolded Protein Response. In the current review, we present three discrete areas of interest: molecular and cellular mechanisms underlying the association between GD and PD; the clinical and genetic associations between GD and PD; and treatment options for GD. We also discuss the relevance of induced pleuripotent stem cells to the above associations., (© 2016 WILEY PERIODICALS, INC.)

Published

2016

34. Aglycon diversity of brain sterylglucosides: structure determination of cholesteryl- and sitosterylglucoside.

Author

Akiyama H, Nakajima K, Itoh Y, Sayano T, Ohashi Y, Yamaguchi Y, Greimel P, and Hirabayashi Y

Subjects

Animals, Cholesterol analogs & derivatives, Cholesterol metabolism, Galactosylceramides metabolism, Gaucher Disease metabolism, Gaucher Disease pathology, Glucosylceramidase metabolism, Glucosylceramides chemistry, Glucosylceramides metabolism, Humans, Magnetic Resonance Spectroscopy, Mice, Sitosterols chemistry, Sitosterols metabolism, Brain Chemistry, Cholesterol chemistry, Galactosylceramides chemistry, Glucosylceramidase chemistry

Abstract

To date, sterylglucosides have been reported to be present in various fungi, plants, and animals. In bacteria, such as Helicobacter pylori, proton NMR spectral analysis of isolated 1-O-cholesteryl-β-d-glucopyranoside (GlcChol) demonstrated the presence of an α-glucosidic linkage. By contrast, in animals, no detailed structural analysis of GlcChol has been reported, in part because animal-derived samples contain a high abundance of glucosylceramides (GlcCers)/galactosylceramides, which exhibit highly similar chromatographic behavior to GlcChol. A key step in vertebrate GlcChol biosynthesis is the transglucosylation reaction catalyzed by glucocerebrosidase (GBA)1 or GBA2, utilizing GlcCer as a glucose donor. These steps are expected to produce a β-glucosidic linkage. Impaired GBA1 and GBA2 function is associated with neurological disorders, such as cerebellar ataxia, spastic paraplegia, and Parkinson's disease. Utilizing a novel three-step chromatographic procedure, we prepared highly enriched GlcChol from embryonic chicken brain, allowing complete structural confirmation of the β-glucosidic linkage by 1 H-NMR analysis. Unexpectedly, during purification, two additional sterylglucoside fractions were isolated. NMR and GC/MS analyses confirmed that the plant-type sitosterylglucoside in vertebrate brain is present throughout embryonic development. The aglycon structure of the remaining sterylglucoside (GSX-2) remains elusive due to its low abundance. Together, our results uncovered unexpected aglycon heterogeneity of sterylglucosides in vertebrate brain., (Copyright © 2016 by the American Society for Biochemistry and Molecular Biology, Inc.)

Published

2016

35. Bicyclic isoureas derived from 1-deoxynojirimycin are potent inhibitors of β-glucocerebrosidase.

Author

Sevšek A, Čelan M, Erjavec B, Quarles van Ufford L, Sastre Toraño J, Moret EE, Pieters RJ, and Martin NI

Subjects

Enzyme Inhibitors metabolism, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Inhibitory Concentration 50, Molecular Docking Simulation, Protein Conformation, Urease metabolism, 1-Deoxynojirimycin chemistry, Bridged Bicyclo Compounds, Heterocyclic chemistry, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Glucosylceramidase antagonists & inhibitors, Urease chemistry, Urease pharmacology

Abstract

A series of bicyclic isourea derivatives were prepared from 1-deoxynojirimycin using a concise synthetic protocol proceeding via a guanidino intermediate. Inhibition assays with a panel of glycosidases revealed that these deoxynojirimycin-derived bicyclic isoureas display very potent inhibition against human recombinant β-glucocerebrosidase with IC50 values in the low nanomolar range.

Published

2016

36. Perspective: Finding common ground.

Author

Futerman AH and Hardy J

Subjects

Alleles, Animals, Gaucher Disease classification, Gaucher Disease physiopathology, Glucosylceramidase chemistry, Glucosylceramidase deficiency, Glucosylceramidase genetics, Glucosylceramides metabolism, Humans, Lysosomes enzymology, Lysosomes genetics, Mice, Mutation, Parkinson Disease metabolism, Parkinson Disease physiopathology, Uncertainty, alpha-Synuclein metabolism, Gaucher Disease enzymology, Gaucher Disease genetics, Glucosylceramidase metabolism, Lysosomes metabolism, Models, Biological, Parkinson Disease enzymology, Parkinson Disease genetics

Published

2016

37. Hydrophobic Interactions Contribute to Conformational Stabilization of Endoglycoceramidase II by Mechanism-Based Probes.

Author

Ben Bdira F, Jiang J, Kallemeijn W, de Haan A, Florea BI, Bleijlevens B, Boot R, Overkleeft HS, Aerts JM, and Ubbink M

Subjects

Amino Acid Sequence, Bacterial Proteins genetics, Bacterial Proteins metabolism, Catalytic Domain, Cyclohexanols chemistry, Enzyme Stability, Gaucher Disease enzymology, Glucosylceramidase chemistry, Glucosylceramidase genetics, Glucosylceramidase metabolism, Glycoside Hydrolases genetics, Glycoside Hydrolases metabolism, Humans, Hydrophobic and Hydrophilic Interactions, Models, Molecular, Molecular Probes chemistry, Protein Conformation, Recombinant Proteins chemistry, Recombinant Proteins genetics, Recombinant Proteins metabolism, Rhodococcus enzymology, Rhodococcus genetics, Structural Homology, Protein, Bacterial Proteins chemistry, Glycoside Hydrolases chemistry

Abstract

Small compound active site interactors receive considerable attention for their ability to positively influence the fold of glycosidases. Endoglycoceramidase II (EGCII) from Rhodococcus sp. is an endo-β-glucosidase releasing the complete glycan from ceramide in glycosphingolipids. Cleavage of the β-glycosidic linkage between glucose and ceramide is also catalyzed by glucocerebrosidase (GBA), the exo-β-glucosidase deficient in Gaucher disease. We demonstrate that established β-glucoside-configured cyclophellitol-type activity-based probes (ABPs) for GBA also are effective, mechanism-based, and irreversible inhibitors of EGCII. The stability of EGCII is markedly enhanced by formation of covalent complexes with cyclophellitol ABPs substituted with hydrophobic moieties, as evidenced by an increased melting temperature, resistance against tryptic digestion, changes in (15)N-(1)H transverse relaxation optimized spectroscopy spectra of the [(15)N]Leu-labeled enzyme, and relative hydrophobicity as determined by 8-anilino-1-naphthalenesulfonic acid fluorescence. The stabilization of EGCII conformation correlates with the shape and hydrophobicity of the substituents of the ABPs. We conclude that the amphipathic active site binders with aliphatic moieties act as a "hydrophobic zipper" on the flexible EGCII protein structure.

Published

2016

38. Investigation of original multivalent iminosugars as pharmacological chaperones for the treatment of Gaucher disease.

Author

Laigre E, Hazelard D, Casas J, Serra-Vinardell J, Michelakakis H, Mavridou I, Aerts JM, Delgado A, and Compain P

Subjects

Click Chemistry, Enzyme Activation drug effects, Enzyme Reactivators pharmacology, Fibroblasts enzymology, Fibroblasts pathology, Gaucher Disease drug therapy, Gaucher Disease enzymology, Gaucher Disease pathology, Glucosylceramidase deficiency, Humans, Imino Sugars pharmacology, Kinetics, Lysosomes enzymology, Molecular Targeted Therapy, Morpholines chemistry, Prodrugs pharmacology, Protein Binding, Protein Folding, Enzyme Reactivators chemical synthesis, Fibroblasts drug effects, Glucosylceramidase chemistry, Imino Sugars chemical synthesis, Lysosomes drug effects, Prodrugs chemical synthesis

Abstract

Multivalent iminosugars conjugated with a morpholine moiety and/or designed as prodrugs have been prepared and evaluated as new classes of pharmacological chaperones for the treatment of Gaucher disease. This study further confirms the interest of the prodrug concept and shows that the addition of a lysosome-targeting morpholine unit into iminosugar cluster structures has no significant impact on the chaperone activity on Gaucher cells., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2016

39. A Novel Functional Missense Mutation p.T219A in Type 1 Gaucher's Disease.

Author

Liu LY, Liu F, Du SC, Jiang SY, Wang HJ, Zhang J, Wang W, and Ma D

Subjects

Child, Preschool, Glucosylceramidase chemistry, Humans, Male, Models, Molecular, Protein Structure, Tertiary, Sequence Analysis, DNA, Gaucher Disease genetics, Glucosylceramidase genetics, Mutation, Missense

Abstract

Background: Gaucher's disease (GD) is an autosomal recessive disorder caused by a deficiency of acid β-glucosidase (glucocerebrosidase [GBA]) that results in the accumulation of glucocerebroside within macrophages. Many mutations have been reported to be associated with this disorder. This study aimed to discover more mutations and provide data for the genetic pattern of the gene, which will help the development of quick and accurate genetic diagnostic tools for this disease., Methods: Genomic DNA was obtained from peripheral blood leukocytes of the patient and Sanger sequencing is used to sequence GBA gene. Sequence alignments of mammalian β-GBA (GCase) and three-dimensional protein structure prediction of the mutation were made. A construct of this mutant and its compound heterozygous counterpart were used to measure GCase in vitro., Results: GCase is relatively conserved at p.T219A. This novel mutation differs from its wild-type in structure. Moreover, it also causes a reduction in GCase enzyme activity., Conclusion: This novel mutation (c.655A>G, p.T219A) is a pathogenic missense mutation, which contributes to GD.

Published

2016

40. Glycosylation is crucial for a proper catalytic site organization in human glucocerebrosidase.

Author

Pol-Fachin L, Siebert M, Verli H, and Saraiva-Pereira ML

Subjects

Catalytic Domain, Gaucher Disease enzymology, Glycosylation, Humans, Glucosylceramidase chemistry, Molecular Dynamics Simulation

Abstract

Gaucher disease, an autosomal recessive disorder, is caused by a deficiency of glucocerebrosidase (GCase) enzyme, a peripheral membrane-associated glycoprotein that hydrolyses glucosylceramide in lysosomes. Glycosylation is essential for the development of a catalytically active enzyme, specifically in the first site, located at Asn19. However, both the molecular basis of the relevance of N-glycosylation over GCase activity and the effects of glycosylation over its structure and dynamics are still not fully understood. Thus, the present work evaluated GCase enzyme in increasing glycosylation content using triplicate unbiased molecular dynamics simulations. Accordingly, the N-linked glycan chains caused local conformational stabilization effects over the protein, as well as in regions flanking the enzyme catalytic dyad. In the case of the Asn19-linked glycan, it also occurred around region 438-444, where one of the most prevalent GCase mutations is found. Markedly, an increasing catalytic dyad organization was related to increasing glycosylation contents, offering the first atomic-level explanation for the experimental observation that GCase activity is controlled by glycosylation, especially at Asn19.

Published

2016

41. Current and Novel Aspects on the Non-lysosomal β-Glucosylceramidase GBA2.

Author

Massimo A, Maura S, Nicoletta L, Giulia M, Valentina M, Elena C, Alessandro P, Rosaria B, and Sandro S

Subjects

Amino Acid Sequence, Animals, Glucosylceramidase chemistry, Humans, Lysosomes enzymology, Mice, Molecular Sequence Data, Subcellular Fractions enzymology, Glucosylceramidase metabolism

Abstract

The non-lysosomal β-glucosylceramidase GBA2 (EC3.2.1.45, GH116) is ubiquitously expressed in various mammal tissues and cell types where it catalyzes the hydrolysis of glucosylceramide into glucose and ceramide. Although it has been known for many years that the central nervous system is the main site of GBA2 expression and activity, little information has been available so far on the role of this protein in the neuronal development, senescence and homeostasis. In the present review, we summarize the state-of-the art of this enzyme and in particular, we focus on the current knowledge on its structure, its physico-chemical properties and its subcellular localization. Data on the involvement of GBA2 in physiopathological processes are also described, with particular emphasis on the studies that have indicated the direct involvement of GBA2 in neuronal development and neurological disorders. A discussion of some open questions and future perspectives related to GBA2 are finally reported. We conclude that further investigations on this β-glucosylceramidase will provide new clues about the physiology of the central nervous system.

Published

2016

42. Klotho-Related Protein KLrP: Structure and Functions.

Author

Hayashi Y and Ito M

Subjects

Animals, Brain enzymology, Crystallography, X-Ray, Cytosol enzymology, Fibroblasts enzymology, Gaucher Disease enzymology, Gene Knockdown Techniques, Glucosylceramides metabolism, Glucuronidase genetics, Humans, Hydrogen-Ion Concentration, Inositol analogs & derivatives, Inositol pharmacology, Klotho Proteins, Models, Molecular, Molecular Structure, Mutation, Rats, Zebrafish, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Glucuronidase chemistry, Glucuronidase metabolism

Abstract

Klotho (KL) family proteins share one or two glycoside hydrolase (GH) motifs homologous to GH family 1. However, the biological significance of GH motifs in KL family proteins remains elusive. We describe here that KL-related protein (KLrP), which is composed of a single GH motif, is a cytosolic β-glucocerebrosidase (GCase, EC 3.2.1.145). We detected a neutral conduritol B epoxide (CBE)-insensitive glucosylceramide (GlcCer)-degrading activity in the cytosol fractions of human fibroblasts, rat brains, and zebrafish embryos. KL family proteins emerged as a potent candidate for the neutral GCase using a bioinformatics approach. Recombinant human KLrP, but not α-KL, β-KL, or KLPH, exhibited GCase activity with a neutral pH optimum in the presence of CBE. We solved the crystal structures of KLrP and a KLrP mutant (E165Q) in complex with glucose, which indicate that KLrP forms a (β/α)8TIM barrel structure with the double-displacement mechanism of the retaining β-glycosidase. Furthermore, knockdown of endogenous KLrP in CHOP cells using small interfering RNA (siRNA) decreased the CBE-insensitive neutral GCase activity and increased the cellular levels of GlcCer, which suggests that KLrP is involved in a novel GlcCer catabolism pathway. A KLrP D106N mutant was discovered in patients with severe Gaucher disease; however, this mutation did not affect the GCase activity of KLrP., (© 2016 Elsevier Inc. All rights reserved.)

Published

2016

43. The effects of chemically synthesized saposin C on glucosylceramide-β-glucosidase.

Author

Yoneshige A, Muto M, Watanabe T, Hojo H, and Matsuda J

Subjects

Cathepsin D chemistry, Cholesterol chemistry, Gaucher Disease enzymology, Humans, Glucosylceramidase chemistry, Saposins chemical synthesis

Abstract

Objective: Saposin C (SAP-C) is an essential activator of glucosylceramide (GlcCer)-β-glucosidase (GCase), the enzyme deficient in Gaucher's disease. In this study, we investigated the effects of chemically synthesized SAP-Cs (synthetic SAP-Cs) on GCase., Methods: Enzymatic assays and western blot analyses were carried out to evaluate the effects of two kinds of synthetic SAP-Cs, a non-glycosylated form and a N-glycosylated form bearing a complex type nonasaccharide, on GCase with respect to its activation, stabilization, and protection. Imiglucerase (Cerezyme) was used as the GCase. To mimic physiological conditions, GCase activity was assayed in the presence of 4-nitrobenzo-2-oxa-1,3-diazole-labeled GlcCer-containing liposomes composed of bis(monoacylglycero)phosphate, l-α-phosphatidylcholine, and cholesterol., Results: GCase activities increased depending on the concentration of synthetic SAP-Cs. SAP-Cs at a concentration of 1μM increased GCase activities significantly, by 14- to 22-fold (non-glycosylated SAP-C: 22.9±0.16; nona-glycosylated SAP-C: 14.9±0.19; without SAP-C: 1.05±0.035pmol/h/ng GCase). These values equaled or surpassed previously published values obtained using recombinant non-glycosylated SAP-C. Both synthetic SAP-Cs were as effective as bovine serum albumin in stabilizing GCase at 37°C. Western blot analysis revealed that synthetic SAP-Cs specifically protected GCase from cathepsin D digestion., Conclusions: The results demonstrate that these novel, chemically synthesized SAP-Cs function as activators, stabilizers, and protectors of GCase, suggesting their utility in enzyme replacement therapy in patients with Gaucher's disease., (Copyright © 2015 The Canadian Society of Clinical Chemists. Published by Elsevier Inc. All rights reserved.)

Published

2015

44. Synthesis and evaluation of hydroxymethylaminocyclitols as glycosidase inhibitors.

Author

Trapero A, Egido-Gabás M, Bujons J, and Llebaria A

Subjects

Cyclitols chemistry, Cyclohexanols chemistry, Kinetics, Structure-Activity Relationship, alpha-Glucosidases, Cyclitols chemical synthesis, Cyclohexanols chemical synthesis, Enzyme Inhibitors chemistry, Glucosylceramidase antagonists & inhibitors, Glucosylceramidase chemistry, beta-Glucosidase antagonists & inhibitors, beta-Glucosidase chemistry

Abstract

Four series of C7N aminocyclitol analogues of glucose were synthesized by stereocontrolled epoxide opening of hydroxyl protected forms of the cyclohexane epoxides cyclophellitol and 1,6-epi-cyclophellitol. The resulting hydroxymethyl substituted aminocyclitols were tested as glycosidase inhibitors. Cyclitols having an amino group in an α configuration at a position equivalent to the anomeric in the sugar were found to be low micromolar inhibitors of the α-glucosidase from baker's yeast with Ki's near to 2 μM. On the other hand, N-octyl aminocyclitols having the nitrogen substituents in an α or β configuration were found to be good inhibitors of recombinant β-glucocerebrosidase with Ki values between 8.3 and 17 μM, and also inhibited lysosomal β-glucosidase activity in live cells at low-micromolar concentrations. A computational docking study suggests a differential binding among the different series of β-glucocerebrosidase inhibitors. In agreement with the experimental results, the binding poses obtained indicate that the presence of an alkyl lipid substituent in the inhibitor mimicking one of the lipid chains in the substrate is critical for potency. In contrast, the matching of hydroxymethyl substituents in the aminocyclitols and the parent glucosylceramide does not seem to be strictly necessary for potent inhibition, indicating the risk of simplifying structural analogies in sugar mimetic design.

Published

2015

45. Direct site-specific glycoform identification and quantitative comparison of glycoprotein therapeutics: imiglucerase and velaglucerase alfa.

Author

Ye H, Hill J, Gucinski AC, Boyne MT 2nd, and Buhse LF

Subjects

Amino Acid Sequence, Animals, CHO Cells, Cricetinae, Cricetulus, Enzyme Replacement Therapy methods, Glycoproteins chemistry, Glycosylation, Humans, Recombinant Proteins chemistry, Chromatography, Liquid methods, Glucosylceramidase chemistry, Mass Spectrometry methods

Abstract

Gaucher disease, the most common lysosomal metabolic disorder, can be treated with enzyme replacement therapy (ERT). Recombinant human glucocerebrosidase imiglucerase (Cerezyme(®)), produced in Chinese hamster ovary cells, has been used for ERT of Gaucher disease for 20 years. Another recombinant glucocerebrosidase velaglucerase alfa (VPRIV), expressed in a human fibroblast cell line, was approved by the US Food and Drug Administration in 2010. The amino acid sequence difference at residue 495 of these two products is well documented. The overall N-linked qualitative glycan composition of these two products has also been reported previously. Herein, employing our recently developed approach utilizing isobaric tandem mass tag (TMT) labeling and an LTQ Orbitrap XL electron transfer dissociation (ETD) hybrid mass spectrometer, the site-specific glycoforms of these products were identified with ETD and collision-induced dissociation (CID) spectra. The quantitative comparison of site-specific glycans was achieved utilizing higher-energy collisional dissociation (HCD) spectra with a NanoMate used as both a fraction collector and a sample introduction device. From the trypsin-digested mixture of these two products, over 90 glycopeptides were identified by accurate mass matching. In addition to those previously reported, additional glycopeptides were detected with moderate abundance. The relative amount of each glycoform at a specific glycosylation site was determined based on reporter signal intensities of the TMT labeling reagents. This is the first report of site-specific simultaneous qualitative and quantitative comparison of glycoforms for Cerezyme(®) and VPRIV. The results demonstrate that this method could be utilized for biosimilarity determination and counterfeit identification of glycoproteins.

Published

2015

46. Dissociation of glucocerebrosidase dimer in solution by its co-factor, saposin C.

Author

Gruschus JM, Jiang Z, Yap TL, Hill SA, Grishaev A, Piszczek G, Sidransky E, and Lee JC

Subjects

Catalytic Domain, Humans, Models, Molecular, Nuclear Magnetic Resonance, Biomolecular, Protein Multimerization, Protein Stability, Saposins chemistry, alpha-Synuclein metabolism, Gaucher Disease enzymology, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Parkinson Disease enzymology, Saposins metabolism

Abstract

Mutations in the gene for the lysosomal enzyme glucocerebrosidase (GCase) cause Gaucher disease and are the most common risk factor for Parkinson disease (PD). Analytical ultracentrifugation of 8 μM GCase shows equilibrium between monomer and dimer forms. However, in the presence of its co-factor saposin C (Sap C), only monomer GCase is seen. Isothermal calorimetry confirms that Sap C associates with GCase in solution in a 1:1 complex (Kd = 2.1 ± 1.1 μM). Saturation cross-transfer NMR determined that the region of Sap C contacting GCase includes residues 63-66 and 74-76, which is distinct from the region known to enhance GCase activity. Because α-synuclein (α-syn), a protein closely associated with PD etiology, competes with Sap C for GCase binding, its interaction with GCase was also measured by ultracentrifugation and saturation cross-transfer. Unlike Sap C, binding of α-syn to GCase does not affect multimerization. However, adding α-syn reduces saturation cross-transfer from Sap C to GCase, confirming displacement. To explore where Sap C might disrupt multimeric GCase, GCase x-ray structures were analyzed using the program PISA, which predicted stable dimer and tetramer forms. For the most frequently predicted multimer interface, the GCase active sites are partially buried, suggesting that Sap C might disrupt the multimer by binding near the active site., (Published by Elsevier Inc.)

Published

2015

47. Membrane anchors effectively traffic recombinant human glucocerebrosidase to the protein storage vacuole of Arabidopsis seeds but do not adequately control N-glycan maturation.

Author

He X, Galpin JD, Miao Y, Jiang L, Grabowski GA, and Kermode AR

Subjects

Arabidopsis genetics, Enteropeptidase metabolism, Golgi Apparatus metabolism, Humans, Plants, Genetically Modified, Protein Structure, Tertiary, Seeds metabolism, Seeds ultrastructure, Vacuoles ultrastructure, Arabidopsis metabolism, Cell Membrane metabolism, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Polysaccharides metabolism, Recombinant Proteins metabolism, Vacuoles metabolism

Abstract

Key Message: Human glucocerebrosidase with vacuolar anchoring domains was targeted to protein storage vacuoles (PSVs) of Arabidopsis seeds, but unexpectedly via the Golgi complex. PSV-targeting to effectively avoid problematic N-glycans is protein dependent. Plant-specific N-glycosylation patterns elaborated within the Golgi complex are a major limitation of using plants to produce biopharmaceuticals as the presence of β1,2 xylose and/or α1,3 fucose residues on the recombinant glycoprotein can render the product immunogenic if administrated parenterally. A reporter protein fused to a vacuolar membrane targeting motif comprised of the BP-80 transmembrane domain (TMD), and the cytoplasmic tail (CT) of α-tonoplast intrinsic protein (α-TIP) is delivered to protein storage vacuoles (PSVs) of tobacco seeds by ER-derived transport vesicles that bypass the Golgi complex. This prompted us to investigate whether a pharmaceutical glycoprotein is targeted to PSVs using the same targeting sequences, thus avoiding the unwanted plant-Golgi-specific complex N-glycan modifications. The human lysosomal acid β-glucosidase (glucocerebrosidase; GCase) (EC 3.2.1.45) fused to the BP-80 TMD and α-TIP CT was produced in Arabidopsis thaliana wild-type (Col-0) seeds. The chimeric GCase became localized in PSVs but transited through the Golgi complex, as indicated by biochemical analyses of the recombinant protein's N-glycans. Our findings suggest that use of this PSV-targeting strategy to avoid problematic N-glycan maturation on recombinant therapeutic proteins is not consistently effective, as it is likely protein- and/or species-specific.

Published

2014

48. The LIMP-2/SCARB2 binding motif on acid β-glucosidase: basic and applied implications for Gaucher disease and associated neurodegenerative diseases.

Author

Liou B, Haffey WD, Greis KD, and Grabowski GA

Subjects

Alanine genetics, Amines metabolism, Amino Acid Motifs, Amino Acid Sequence, Amino Acid Substitution, Animals, Binding, Competitive, Gaucher Disease pathology, Glucosylceramidase deficiency, Green Fluorescent Proteins metabolism, Humans, Hydrogen-Ion Concentration, Immunoprecipitation, Mice, Models, Molecular, Molecular Sequence Data, Mutagenesis, Mutation genetics, Neurodegenerative Diseases pathology, Peptides chemistry, Peptides metabolism, Protein Binding, Protein Structure, Tertiary, Protein Transport, Transfection, Gaucher Disease enzymology, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Lysosomal Membrane Proteins metabolism, Neurodegenerative Diseases enzymology, Receptors, Scavenger metabolism

Abstract

The acid β-glucosidase (glucocerbrosidase (GCase)) binding sequence to LIMP-2 (lysosomal integral membrane protein 2), the receptor for intracellular GCase trafficking to the lysosome, has been identified. Heterologous expression of deletion constructs, the available GCase crystal structures, and binding and co-localization of identified peptides or mutant GCases were used to identify and characterize a highly conserved 11-amino acid sequence, DSPIIVDITKD, within human GCase. The binding to LIMP-2 is not dependent upon a single amino acid, but the interactions of GCase with LIMP-2 are heavily influenced by Asp(399) and the di-isoleucines, Ile(402) and Ile(403). A single alanine substitution at any of these decreases GCase binding to LIMP-2 and alters its pH-dependent binding as well as diminishing the trafficking of GCase to the lysosome and significantly increasing GCase secretion. Enterovirus 71 also binds to LIMP-2 (also known as SCARB2) on the external surface of the plasma membrane. However, the LIMP-2/SCARB2 binding sequences for enterovirus 71 and GCase are not similar, indicating that LIMP-2/SCARB2 may have multiple or overlapping binding sites with differing specificities. These findings have therapeutic implications for the production of GCase and the distribution of this enzyme that is delivered to various organs., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

49. Mass spectrometric study of gas-phase ions of acid β-glucosidase (Cerezyme) and iminosugar pharmacological chaperones.

Author

Rajabi K

Subjects

Amino Acid Sequence, Deoxyglucose analogs & derivatives, Gases chemistry, Glucosylceramidase metabolism, Glycosylation, Imino Sugars metabolism, Ions chemistry, Models, Molecular, Molecular Sequence Data, Tandem Mass Spectrometry, Glucosylceramidase chemistry, Imino Sugars chemistry

Abstract

The effect on the conformations and stability of gas-phase ions of Cerezyme, a glycoprotein, when bound to three small-molecule chaperones has been studied using intact ESI MS, collision cross section and MS/MS measurements. To distinguish between the peaks from apo and small-molecule complex ions, Cerezyme is deglycosylated (dg-Cer). ESI MS of dg-Cer reveals that glycosylation accounts for 8.5% of the molecular weight. When excess chaperone, either covalent (2FGF) or noncovalent (A and B iminosugars), is added to solutions of dg-Cer, mass spectra show peaks from 1:1 chaperone-enzyme complexes as well as free enzyme. On average, ions of the apoenzyme have 1.6 times higher cross sections when activated in the source region of the mass spectrometer. For a given charge state, ions of complexes of 2FGF and B have about 30% and 8.4% lower cross sections, respectively, compared to the apoenzyme. Thus, binding the chaperones causes the gas-phase protein to adopt more compact conformations. The noncovalent complex ions dissociate by the loss of charged chaperones. In the gas phase, the relative stability of dg-Cer with B is higher than that with the A, whereas in solution A binds enzyme more strongly than B. Nevertheless, the disagreement is explained based on the greater number of contacts between the B and dg-Cer than the A and dg-Cer (13 vs. 8), indicating the importance of noncovalent interactions within the protein-chaperone complex in the absence of solvent. Findings in this work suggest a hypothesis towards predicting a consistent correlation between gas-phase properties to solution binding properties., (Copyright © 2014 John Wiley & Sons, Ltd.)

Published

2014

50. Selective chaperone effect of aminocyclitol derivatives on G202R and other mutant glucocerebrosidases causing Gaucher disease.

Author

Serra-Vinardell J, Díaz L, Gutiérrez-de Terán H, Sánchez-Ollé G, Bujons J, Michelakakis H, Mavridou I, Aerts JM, Delgado A, Grinberg D, Vilageliu L, and Casas J

Subjects

Apoptosis drug effects, Cells, Cultured, Crystallography, X-Ray, Enzyme Inhibitors pharmacology, Fibroblasts enzymology, Fibroblasts pathology, Fluorescent Antibody Technique, Gaucher Disease enzymology, Gaucher Disease genetics, Glucosylceramidase chemistry, Glucosylceramidase metabolism, Humans, Lipids, Microscopy, Confocal, Molecular Dynamics Simulation, Protein Conformation, Protein Folding, Skin enzymology, Skin pathology, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Sphingolipids, Fibroblasts drug effects, Gaucher Disease drug therapy, Glucosylceramidase genetics, Imino Pyranoses pharmacology, Molecular Chaperones pharmacology, Mutation genetics, Skin drug effects

Abstract

Gaucher disease is an autosomal recessive lysosomal disorder characterized by the accumulation of glucosylceramide as a result of a deficiency of the enzyme glucocerebrosidase. Several competitive glucocerebrosidase inhibitors are able to act as pharmacological chaperones for an efficient rescue of the mutated, misfolded forms of the enzyme. Along this line, we report in this work on the ability of several aminocyclitols to increase the residual glucocerebrosidase activity in patient fibroblasts with different genotypes. Some of the compounds were slightly active on fibroblasts bearing some mutations, including the highly prevalent N370S mutation. All compounds were highly active as enzyme activity enhancers on fibroblasts from Gaucher disease patients containing the G202R mutation. Moreover, using the novel tagged sphingolipid ω-azidosphingosine, a reduction in the tagged glucosylceramide accumulation was also observed for selected aminocyclitols. Attempts to explain the activity impairment observed in glucocerebrosidase bearing the G202R mutation by comparative molecular dynamic studies on wild type and the G202R mutated proteins (free and isofagomine-bound, in both cases) were unsuccessful. Under the simulation conditions used, no clear effect of the G202R mutation neither over the global structure of the protein nor on the loops that constitute the glucocerebrosidase active site was observed. Since the G202R residue is located on the protein surface, altered protein-membrane or protein-protein interactions could account for the observed differences. In conclusion, we have tested novel compounds that have shown some chaperone effect on particular glucocerebrosidase mutant enzymes, supporting the enhancement therapy as an alternative approach for Gaucher disease., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2014