Your search keyword '"Glucocerebrosidase gene"' showing total 27 results

1. The Landscape of Monogenic Parkinson's Disease in Populations of Non-European Ancestry: A Narrative Review.

Author

Koros, Christos, Bougea, Anastasia, Simitsi, Athina Maria, Papagiannakis, Nikolaos, Angelopoulou, Efthalia, Pachi, Ioanna, Antonelou, Roubina, Bozi, Maria, Stamelou, Maria, and Stefanis, Leonidas

Subjects

*PARKINSON'S disease, *LATIN Americans, *EAST Asians, *AFRICANS, *GENETIC testing, *ETHNICITY, *CHILD patients

Abstract

Introduction: There has been a bias in the existing literature on Parkinson's disease (PD) genetics as most studies involved patients of European ancestry, mostly in Europe and North America. Our target was to review published research data on the genetic profile of PD patients of non-European or mixed ancestry. Methods: We reviewed articles published during the 2000–2023 period, focusing on the genetic status of PD patients of non-European origin (Indian, East and Central Asian, Latin American, sub-Saharan African and Pacific islands). Results: There were substantial differences regarding monogenic PD forms between patients of European and non-European ancestry. The G2019S Leucine Rich Repeat Kinase 2 (LRRK2) mutation was rather scarce in non-European populations. In contrast, East Asian patients carried different mutations like p.I2020T, which is common in Japan. Parkin (PRKN) variants had a global distribution, being common in early-onset PD in Indians, in East Asians, and in early-onset Mexicans. Furthermore, they were occasionally present in Black African PD patients. PTEN-induced kinase 1 (PINK1) and PD protein 7 (DJ-1) variants were described in Indian, East Asian and Pacific Islands populations. Glucocerebrosidase gene variants (GBA1), which represent an important predisposing factor for PD, were found in East and Southeast Asian and Indian populations. Different GBA1 variants have been reported in Black African populations and Latin Americans. Conclusions: Existing data reveal a pronounced heterogeneity in the genetic background of PD. A number of common variants in populations of European ancestry appeared to be absent or scarce in patients of diverse ethnic backgrounds. Large-scale studies that include genetic screening in African, Asian or Latin American populations are underway. The outcomes of such efforts will facilitate further clinical studies and will possibly contribute to the identification of either new pathogenic mutations in already described genes or novel PD-related genes. [ABSTRACT FROM AUTHOR]

Published

2023

2. Disrupted topological organization of resting-state functional brain networks in Parkinson's disease patients with glucocerebrosidase gene mutations.

Author

Hou, Yanbing, Feng, Fei, Zhang, Lingyu, Ou, Ruwei, Lin, Junyu, Gong, Qiyong, and Shang, Huifang

Subjects

*BRAIN, *PREFRONTAL cortex, *PARIETAL lobe, *PILOT projects, *GENETIC mutation, *MAGNETIC resonance imaging, *BRAIN mapping, *GENES, *PARKINSON'S disease, *THEORY, *SYMPTOMS, *RESEARCH funding, *STATISTICAL correlation, *DEFAULT mode network

Abstract

Purpose: The mutations of the glucocerebrosidase (GBA) gene are the greatest genetic risk factor for Parkinson's disease (PD). The mechanism underlying the association between GBA mutations and PD has not been fully elucidated. Methods: Using resting-state functional magnetic resonance imaging and graph theory analysis to investigate the disrupted topological organization in PD patients with GBA mutation (GBA-PD). Eleven GBA-PD patients, 11 noncarriers with PD, and 18 healthy controls (HCs) with a similar age and sex distribution were recruited. Individual whole-brain functional connectome was constructed, and the global and nodal topological disruptions were calculated among groups. Partial correlation analyses between the clinical features of patients with PD and topological alterations were performed. Results: The GBA-PD group showed prominently decreased characteristic path length (Lp) and increased global efficiency (Eg) compared to HCs at the global level; a significantly increased nodal betweenness centrality in the medial prefrontal cortex (mPFC) and precuneus within the default mode network, and precentral gyrus within the sensorimotor network, while a significantly decreased betweenness centrality in nodes within the cingulo-opercular network compared to the noncarrier group at the regional level. The altered nodal betweenness centrality of mPFC was positively correlated with fatigue severity scale scores in all patients with PD. Conclusion: The preliminary pilot study found that GBA-PD patients had a higher functional integration at the global level. The nodal result of the mPFC is congruent with the potential fatigue pathology in PD and is suggestive of a profound effect of GBA mutations on the clinical fatigue in patients with PD. [ABSTRACT FROM AUTHOR]

Published

2023

3. A case of cutaneous collagenous vasculopathy associated with multiple myeloma and with a pathogenic variant of the glucocerebrosidase gene.

Author

Dura, Miroslav, Pock, Lumir, Cetkovska, Petra, Jungova, Alexandra, Nemejcova, Kristyna, and Stork, Jiri

Subjects

*MULTIPLE myeloma, *GENETIC variation, *VASCULAR diseases, *STEM cell transplantation

Abstract

Cutaneous collagenous vasculopathy (CCV) is an extremely rare acquired microangiopathy of unknown etiology. The authors describe a case of a 68‐year‐old man, a carrier of a heterozygous pathogenic variant of the glucocerebrosidase (GBA) gene, who was diagnosed with CCV, revealing uncommon fibrinogen positivity in direct immunofluorescence. The patient was subsequently diagnosed with multiple myeloma. Treatment of the myeloma with combined chemotherapy including bortezomib, followed by autologous stem cell transplantation, led to significant reduction of cutaneous lesions. To the best of the authors' knowledge, this is the first published case of CCV in a carrier of a pathogenic variant of the GBA gene, associated with multiple myeloma and with significant regression of CCV after myeloma treatment. Direct immunofluorescence examination revealed an unusual fibrinogen deposition. Hypothetical causative role of bortezomib treatment was proposed regarding significant regression of CCV. [ABSTRACT FROM AUTHOR]

Published

2022

4. Impact of APOE Genotype on Cognition in Idiopathic and Genetic Forms of Parkinson's Disease.

Author

Koros, Christos, Brockmann, Kathrin, Simitsi, Athina‐Maria, Bougea, Anastasia, Liu, Hui, Hauser, Ann‐Kathrin, Schulte, Claudia, Lerche, Stefanie, Pachi, Ioanna, Papagiannakis, Nikolaos, Antonelou, Roubina, Zahou, Athina, Wurster, Isabel, Efthymiopoulou, Efthymia, Beratis, Ion, Maniati, Matina, Moraitou, Marina, Michelakakis, Helen, Paraskevas, Georgios, and Papageorgiou, Sokratis G.

Published

2023

5. Longitudinal clinical, cognitive, and neuroanatomical changes over 5 years in GBA-positive Parkinson's disease patients.

Author

Leocadi, Michela, Canu, Elisa, Donzuso, Giulia, Stojkovic, Tanja, Basaia, Silvia, Kresojević, Nikola, Stankovic, Iva, Sarasso, Elisabetta, Piramide, Noemi, Tomic, Aleksandra, Markovic, Vladana, Petrovic, Igor, Stefanova, Elka, Kostic, Vladimir S., Filippi, Massimo, and Agosta, Federica

Subjects

*PARKINSON'S disease, *CEREBRAL cortical thinning, *APATHY, *CLINICAL neuropsychology, *PROGRESSIVE supranuclear palsy

Abstract

Objective: To study the longitudinal disease course of Parkinson's disease (PD) patients with glucocerebrosidase (GBA) mutation (GBA-positive) compared to PD non-carriers (GBA-negative) along a 5-year follow-up, evaluating changes in clinical and cognitive outcomes, cortical thickness, and gray-matter (GM) volumes. Methods: Ten GBA-positive and 20 GBA-negative PD patients underwent clinical, neuropsychological, and MRI assessments (cortical thickness and subcortical, hippocampal, and amygdala volumes) at study entry and once a year for 5 years. At baseline and at the last visit, each group of patients was compared with 22 age-matched healthy controls. Clinical, cognitive, and MRI features were compared between groups at baseline and over time. Results: At baseline, GBA-positive and GBA-negative PD patients had similar clinical and cognitive profiles. Compared to GBA-negative and controls, GBA-positive patients showed cortical thinning of left temporal, parietal, and occipital gyri. Over time, compared to GBA-negative, GBA-positive PD patients progressed significantly in motor and cognitive symptoms, and showed a greater pattern of cortical thinning of posterior regions, and frontal and orbito-frontal cortices. After 5 years, compared to controls, GBA-negative PD patients showed a pattern of cortical thinning similar to that showed by GBA-positive cases at baseline. The two groups of patients showed similar patterns of subcortical, hippocampal, and amygdala volume loss over time. Conclusions: Compared to GBA-negative PD, GBA-positive patients experienced a more rapid motor and cognitive decline together with a greater, earlier and faster cortical thinning. Cortical thickness measures may be a useful tool for monitoring and predicting PD progression in accordance with the genetic background. [ABSTRACT FROM AUTHOR]

Published

2022

6. Serum uric acid level as a putative biomarker in Parkinson's disease patients carrying GBA1 mutations: 2-Year data from the PPMI study.

Author

Koros, Christos, Simitsi, Athina-Maria, Papagiannakis, Nikolaos, Bougea, Anastasia, Prentakis, Andreas, Papadimitriou, Dimitra, Pachi, Ioanna, Antonelou, Roubina, Angelopoulou, Efthalia, Beratis, Ion, Bozi, Maria, Papageorgiou, Sokratis G., Trapali, Xenia Geronicola, Stamelou, Maria, and Stefanis, Leonidas

Subjects

*URIC acid, *PARKINSON'S disease, *BIOMARKERS, *TUMOR lysis syndrome, *PARKINSON'S disease diagnosis, *DISEASE progression, *RESEARCH, *RESEARCH methodology, *EVALUATION research, *COMPARATIVE studies, *GLYCOSIDASES, *LONGITUDINAL method

Abstract

Introduction: Blood uric acid represents an important biomarker in sporadic Parkinson's disease (PD). Whether uric acid levels change in genetic forms of PD is beginning to be assessed. The aim of the present study was to evaluate differences in serum uric acid level among PD patients harboring mutations in the glucocerebrosidase (GBA1) gene, sporadic PD, and healthy controls followed longitudinally.Methods: Longitudinal 2-year serum uric acid measurement data of 120 GBA-PD patients have been downloaded from the Parkinson's Progression Markers Initiative (PPMI) database. This cohort was compared with 369 de novo sporadic PD patients and 195 healthy controls enrolled in the same study.Results: Following adjustment for age, sex and BMI the GBA-PD cohort exhibited lower 2-year longitudinal uric acid level as compared to the controls (p = 0.016). Baseline uric acid measurements showed only a marginal difference (p = 0.119), but year 2 uric acid levels were lower in the GBA-PD cohort (p < 0.001). There was no difference in baseline, year 2 and 2-year longitudinal serum uric acid in the GBA-PD cohort as compared to sporadic PD (p = 0.664, p = 0.117 and p = 0.315).Conclusions: This is the first study to assess serum uric acid in a GBA-PD cohort. Our findings suggest that low serum uric acid might be a progression biomarker in GBA-PD. However, more studies (ideally longitudinal) on the association between low serum uric acid and clinical data in GBA-PD are needed. These results are consistent with data from previous reports assessing uric acid as a biomarker in other genetic forms of PD. [ABSTRACT FROM AUTHOR]

Published

2021

7. Impact of APOE Genotype on Cognition in Idiopathic and Genetic Forms of Parkinson's Disease

Author

Christos Koros, Kathrin Brockmann, Athina‐Maria Simitsi, Anastasia Bougea, Hui Liu, Ann‐Kathrin Hauser, Claudia Schulte, Stefanie Lerche, Ioanna Pachi, Nikolaos Papagiannakis, Roubina Antonelou, Athina Zahou, Isabel Wurster, Efthymia Efthymiopoulou, Ion Beratis, Matina Maniati, Marina Moraitou, Helen Michelakakis, Georgios Paraskevas, Sokratis G. Papageorgiou, Constantin Potagas, Dimitra Papadimitriou, Maria Bozi, Maria Stamelou, Thomas Gasser, and Leonidas Stefanis

Subjects

Genotype, Parkinson's disease, ApoE protein, human, cognitive decline, Cognition, Apolipoproteins E, Neurology, genetics [Parkinson Disease], genetics [alpha-Synuclein], alpha-Synuclein, Humans, genetics [Apolipoproteins E], glucocerebrosidase gene, Neurology (clinical), ddc:610, apolipoprotein E, α-synuclein gene

Published

2023

8. Novel Mutations in the Glucocerebrosidase Gene of Brazilian Patients with Gaucher Disease

Author

Siebert, Marina, Bock, Hugo, Michelin-Tirelli, Kristiane, Coelho, Janice C., Giugliani, Roberto, Saraiva-Pereira, Maria Luiza, Zschocke, Johannes, editor, Gibson, K. Michael, editor, Brown, Garry, editor, Morava, Eva, editor, and Peters, Verena, editor

Published

2013

9. Bioinformatics analysis and identification of genes and molecular pathways involved in Parkinson’s disease in patients with mutations in the glucocerebrosidase gene

Author

Guo-Qian Li, Xiao-Xia Yang, Zhi-Sheng Wu, Dan-Dan Xu, Xiao-Qiang Liu, and Jie-Hua Wang

Subjects

Parkinson's disease, Gene mutation, Biology, corticotropin-releasing hormone, Gene expression, Databases, Genetic, medicine, Humans, Protein Interaction Maps, KEGG, Gene, MTNR1B Parkinson’s disease, Genetics, General Neuroscience, Gene Expression Profiling, Computational Biology, Parkinson Disease, medicine.disease, Melatonin receptor 1B, Mutation, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, glucocerebrosidase gene, Glucosylceramidase, Signal transduction, Cellular, Molecular and Developmental Neuroscience, Glucocerebrosidase

Abstract

Supplemental Digital Content is available in the text., Glucocerebrosidase (GBA) mutations occur frequently in Parkinson’s disease (PD) patients. This study aims to identify potential crucial genes and pathways associated with GBA mutations in patients with PD and to further analyze new molecular mechanisms related to the occurrence of gene mutations from the perspective of bioinformatics. Gene expression profiles of datasets GSE53424 and GSE99142 were acquired from the Gene Expression Ominibus database. Differentially expressed genes (DEGs) were detected, using the ‘limma’ package in R, comparing IDI-PD 1 (idiopathic PD patients) and GBA-PD 1 [PD patients with heterozygous GBA mutations (GBA N370S)] group samples. The functions of top modules were assessed using the DAVID, whereas gene ontology and Kyoto Encyclopedia of Genes and Genomes pathway enrichment analyses were performed. Protein–protein interaction networks were assembled with Cytoscape software and separated into subnetworks using the Molecular Complex Detection Algorithm. Data from GSE53424 and GSE99142 were also extracted to verify our findings. There were 283 DEGs identified in PD patients heterozygous for GBA mutations. Module analysis revealed that GBA mutations in PD patients were associated with significant pathways, including Calcium signaling pathway, Rap1 signaling pathway and Cytokine–cytokine receptor interaction. Hub genes of the two modules were corticotropin-releasing hormone (CRH) and Melatonin receptor 1B (MTNR1B). The expression of CRH was downregulated, whereas that of MTNR1B was upregulated in PD patients with GBA mutations. The expression of CRH and MTNR1B has diagnostic value for PD patients with heterozygous GBA mutations. Novel DEGs and pathways identified herein might provide new insights into the underlying molecular mechanisms of heterozygous GBA mutations in PD patients.

Published

2021

10. Commentary: Possible involvement of lysosomal dysfunction in pathological changes of the brain in aged progranulin-deficient mice.

Author

Timothy J Sargeant

Subjects

Lysosomal Storage Diseases, Lysosomes, Neurodegenerative Diseases, Parkinson's disease, glucocerebrosidase gene, Frontotemporal dementia (FTD), Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2016

11. Molecular Characteristics in Japanese Patients with Lipidosis: Novel Mutations in Metachromatic Leukodystrophy and Gaucher Disease

Author

Eto, Yoshikatsu, Kawame, Hiroshi, Hasegawa, Yoriyasu, Ohashi, Toy A, Ida, Hiroyuki, Tokoro, Toshiharu, Dhalla, Naranjan S., editor, Yazaki, Yoshio, editor, and Mochizuki, Seibu, editor

Published

1993

12. Impact of glucocerebrosidase mutations on motor and nonmotor complications in Parkinson's disease.

Author

Oeda, Tomoko, Umemura, Atsushi, Mori, Yuko, Tomita, Satoshi, Kohsaka, Masayuki, Park, Kwiyoung, Inoue, Kimiko, Fujimura, Harutoshi, Hasegawa, Hiroshi, Sugiyama, Hiroshi, and Sawada, Hideyuki

Subjects

*GAUCHER'S disease, *GENETIC mutation, *RETROSPECTIVE studies, *POSITRON emission tomography, *CEREBRAL circulation

Abstract

Homozygous mutations of the glucocerebrosidase gene ( GBA ) cause Gaucher disease (GD), and heterozygous mutations of GBA are a major risk factor for Parkinson's disease (PD). This study examined the impact of GBA mutations on the longitudinal clinical course of PD patients by retrospective cohort design. GBA- coding regions were fully sequenced in 215 PD patients and GD-associated GBA mutations were identified in 19 (8.8%) PD patients. In a retrospective cohort study, time to develop dementia, psychosis, wearing-off, and dyskinesia were examined. Survival time analysis followed a maximum 12-year observation (median 6.0 years), revealing that PD patients with GD-associated mutations developed dementia and psychosis significantly earlier than those without mutations ( p < 0.001 and p = 0.017, respectively). Adjusted hazard ratios of GBA mutations were 8.3 for dementia ( p < 0.001) and 3.1 for psychosis ( p = 0.002). No statistically significant differences were observed for wearing-off and dyskinesia between the groups. N-isopropyl-p[ 123 I] iodoamphetamine single-photon emission tomography pixel-by-pixel analysis revealed that regional cerebral blood flow was reduced in the bilateral parietal cortex, including the precuneus of GD-associated mutant PD patients, compared with matched PD controls without mutations. [ABSTRACT FROM AUTHOR]

Published

2015

13. Longitudinal clinical, cognitive, and neuroanatomical changes over 5 years in GBA-positive Parkinson's disease patients

Author

Giulia Donzuso, Federica Agosta, Nikola Kresojević, Aleksandra Tomić, Tanja Stojkovic, Elisa Canu, Igor Petrović, Iva Stankovic, Noemi Piramide, Michela Leocadi, Vladana Markovic, Massimo Filippi, Silvia Basaia, Elisabetta Sarasso, Vladimir S. Kostic, Elka Stefanova, Leocadi, M., Canu, E., Donzuso, G., Stojkovic, T., Basaia, S., Kresojevic, N., Stankovic, I., Sarasso, E., Piramide, N., Tomic, A., Markovic, V., Petrovic, I., Stefanova, E., Kostic, V. S., Filippi, M., and Agosta, F.

Subjects

medicine.medical_specialty, Neurology, Parkinson's disease, Amygdala, Cortical thickness, 03 medical and health sciences, 0302 clinical medicine, Magnetic resonance imaging, Cognition, Glucocerebrosidase gene, Internal medicine, medicine, Humans, Cognitive Dysfunction, Cognitive decline, Gray Matter, 030304 developmental biology, Neuroradiology, 0303 health sciences, medicine.diagnostic_test, business.industry, Neuropsychology, Parkinson Disease, medicine.disease, medicine.anatomical_structure, Mutation, Cardiology, Parkinson’s disease, Glucosylceramidase, GBA, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Objective: To study the longitudinal disease course of Parkinson’s disease (PD) patients with glucocerebrosidase (GBA) mutation (GBA-positive) compared to PD non-carriers (GBA-negative) along a 5-year follow-up, evaluating changes in clinical and cognitive outcomes, cortical thickness, and gray-matter (GM) volumes. Methods: Ten GBA-positive and 20 GBA-negative PD patients underwent clinical, neuropsychological, and MRI assessments (cortical thickness and subcortical, hippocampal, and amygdala volumes) at study entry and once a year for 5 years. At baseline and at the last visit, each group of patients was compared with 22 age-matched healthy controls. Clinical, cognitive, and MRI features were compared between groups at baseline and over time. Results: At baseline, GBA-positive and GBA-negative PD patients had similar clinical and cognitive profiles. Compared to GBA-negative and controls, GBA-positive patients showed cortical thinning of left temporal, parietal, and occipital gyri. Over time, compared to GBA-negative, GBA-positive PD patients progressed significantly in motor and cognitive symptoms, and showed a greater pattern of cortical thinning of posterior regions, and frontal and orbito-frontal cortices. After 5 years, compared to controls, GBA-negative PD patients showed a pattern of cortical thinning similar to that showed by GBA-positive cases at baseline. The two groups of patients showed similar patterns of subcortical, hippocampal, and amygdala volume loss over time. Conclusions: Compared to GBA-negative PD, GBA-positive patients experienced a more rapid motor and cognitive decline together with a greater, earlier and faster cortical thinning. Cortical thickness measures may be a useful tool for monitoring and predicting PD progression in accordance with the genetic background.

Published

2021

14. Glucocerebrosidase involvement in Parkinson Disease and other Synucleinopathies

Author

Maria Rosario Almeida

Subjects

Parkinson Disease, glucocerebrosidase gene, Lewy body pathology, synucleinopathies, Neurology. Diseases of the nervous system, RC346-429

Abstract

Mutations in the both copies (homozygous or compound heterozygous) of the gene encoding the lysosomal enzyme glucocerebrosidase, which cleaves the glycolipid glucocerebroside into glucose and ceramide causes Gaucher Disease. However, multiple independent studies have also reported an association between GBA mutations and Parkinsonism with an increased frequency of heterozygous GBA mutations in various cohorts of patients with parkinsonism and other Lewy body disorders. Furthermore, GBA mutation carriers exhibit diverse parkinsonian phenotypes and present a diffuse pattern of Lewy body distribution in the cerebral cortex. This review provides an overview of the genetic basis for this association in various diseases with dysfunction of the central nervous system in which affected individuals developed Parkinsonian symptoms. The emerging clinical, pathological and genetic studies in neuronal synucleinopathies suggest a common underlying mechanism in the etiology of these neurodegenerative disorders.

Published

2012

15. White matter abnormalities in Parkinson's disease patients with glucocerebrosidase gene mutations.

Author

Agosta, Federica, Kostic, Vladimir S., Davidovic, Kristina, Kresojević, Nikola, Sarro, Lidia, Svetel, Marina, Stanković, Iva, Comi, Giancarlo, Klein, Christine, and Filippi, Massimo

Abstract

ABSTRACT Glucocerebrosidase gene mutations represent a genetic risk factor for the development of Parkinson's disease. This study investigated brain alterations in Parkinson's disease patients carrying heterozygous glucocerebrosidase gene mutations using structural and diffusion tensor magnetic resonance imaging. Among 360 Parkinson's disease patients screened for glucocerebrosidase gene mutations, 19 heterozygous mutation carriers (5.3%) were identified. Of these, 15 patients underwent a neuropsychological evaluation and a magnetic resonance imaging scan. Sixteen age- and sex-matched healthy controls and 14 idiopathic Parkinson's disease patients without glucocerebrosidase gene mutations were also studied. Tract-based spatial statistics was used to perform a white matter voxel-wise analysis of diffusion tensor magnetic resonance imaging metrics. Mean fractional anisotropy values were obtained from white matter tracts of interest. Voxel-based morphometry was used to assess gray-matter atrophy. Cognitive deficits were found in 9 mutation carrier patients (60%). Compared with controls, Parkinson's disease patients carrying glucocerebrosidase gene mutations showed decreased fractional anisotropy in the olfactory tracts, corpus callosum, and anterior limb of the internal capsule bilaterally, as well as in the right anterior external capsule, and left cingulum, parahippocampal tract, parietal portion of the superior longitudinal fasciculus, and occipital white matter. Mutation carrier patients also had decreased fractional anisotropy of the majority of white matter tracts compared with Parkinson's disease patients with no mutations. No white matter abnormalities were found in Parkinson's disease patients without glucocerebrosidase gene mutations. No gray matter difference was found between patients and controls. In Parkinson's disease patients, verbal fluency scores correlated with white matter abnormalities. Parkinson's disease patients carrying glucocerebrosidase gene mutations experience a distributed pattern of white matter abnormalities involving the interhemispheric, frontal corticocortical, and parahippocampal tracts. White matter pathology in these patients may have an impact on the clinical manifestations of the disease, including cognitive impairment. © 2013 Movement Disorder Society [ABSTRACT FROM AUTHOR]

Published

2013

16. Glucocerebrosidase gene variants in parkinsonian patients with Machado Joseph/spinocerebellar ataxia 3

Author

Siebert, M., Donis, K.C., Socal, M., Rieder, C.R.M., Emmel, V.E., Vairo, F., Michelin-Tirelli, K., França, M., D’Abreu, A.C., Bettencourt, C., Lima, M., Lopes Cendes, I., Saraiva-Pereira, M.L., and Jardim, L.B.

Subjects

*PARKINSON'S disease, *GENETIC mutation, *PHENOTYPES, *LEUCOCYTES, *ENZYME activation, *FISHER exact test, *GENEALOGY

Abstract

Abstract: Machado-Joseph disease/spinocerebellar ataxia type 3 (MJD/SCA3) may rarely presents a parkinsonian phenotype. Considering that mutations in the glucocerebrosidase (GBA) gene have been associated with Parkinson disease, we investigated whether these would be more prevalent in MJD/SCA3 patients with parkinsonian manifestations than in those without them. Methods: MJD/SCA3 patients with parkinsonian features were identified and compared to relatives and to a MJD/SCA3 control group with no such features. The GBA gene was sequenced and, in a subset of patients and in normal volunteers, GBA enzyme activity was measured. Results: We have identified nine index MJD/SCA3 patients with parkinsonian manifestations. Overall, GBA sequence variations were found in 3/9 MJD/SCA3 index cases with parkinsonian manifestations (33%) and in 0/40 MJD/SCA3 controls without parkinsonism (p =0.03, Fisher exact test). The GBA sequence variations found were p.K(-27)R, p.E326K, and p.T369M. The latter two sequence variations were also found in two symptomatic relatives with no parkinsonian manifestations. A MJD/SCA3 relative belonging to the first positive pedigree and carrier of the p.K(-27)R mutation also presented parkinsonian manifestations. GBA activity in MJD/SCA3 patients was similar to those found in the normal control group. Conclusion: Sequence variations at the GBA gene may play a role as a minor, modifying gene of MJD/SCA3 phenotype. This hypothetical role was not related to changes in GBA activity in peripheral leukocytes. [Copyright &y& Elsevier]

Published

2012

17. Commentary: Possible involvement of lysosomal dysfunction in pathological changes of the brain in aged progranulin-deficient mice.

Author

Sargeant, Timothy J. and Buee, Luc

Subjects

LYSOSOMAL storage diseases, NEUROLOGICAL disorders, PROGRANULIN, NEURONAL ceroid-lipofuscinosis

Abstract

The author discusses the research paper "Possible involvement of lysosomal dysfunction in pathological changes of the brain in aged progranulin-deficient mice" by Y. Tanaka and colleagues. Topics discussed include the neuropathological consequences of progranulin knock out in a mouse model, neuronal ceroid lipofuscinosis also known as Batten's disease caused by Loss of progranulin function by Granulin (GRN) mutation, and genetic link between GRN and Batten's disease.

Published

2016

18. A molecular analysis of theGBAgene in Caucasian South Africans with Parkinson's disease

Author

David G. Anderson, Francois H. van der Westhuizen, Melinda Barkhuizen, Anne Grobler, 10213503 - Van der Westhuizen, Francois Hendrikus, 11008857 - Grobler, Anne Frederica, 21686866 - Barkhuizen, Melinda, Kindergeneeskunde, RS: MHeNs - R3 - Neuroscience, and Promovendi MHN

Subjects

Glucocerebrosidase, 0301 basic medicine, medicine.medical_specialty, Parkinson's disease, Gaucher disease, Disease, VARIANTS, MECHANISMS, GAUCHER-DISEASE, 03 medical and health sciences, Exon, 0302 clinical medicine, Internal medicine, Genetic screening, Genetics, medicine, COHORT, Risk factor, Molecular Biology, Gene, Genetics (clinical), RISK, IDENTIFICATION, glucocerebrosidase, MUTATIONS, business.industry, Modeling, modeling, Original Articles, genetic screening, medicine.disease, GLUCOCEREBROSIDASE GENE, Molecular analysis, Afrikaner, 030104 developmental biology, ONSET, Cohort, Parkinson’s disease, Original Article, business, 030217 neurology & neurosurgery

Abstract

BackgroundThe molecular basis of Parkinson's disease in South African population groups remains elusive. To date, substitutions in the GBA gene are the most common large-effect genetic risk factor for Parkinson's disease. The primary objective of this study was to determine the prevalence of GBA substitutions in South Africans with idiopathic Parkinson's disease.MethodsParticipants were recruited from tertiary hospitals in the Gauteng Province in South Africa. All participants were screened for substitutions in GBA exon 8-11 and the full coding region was analysed in 20 participants. Peripheral -glucocerebrosidase enzymatic activity of GBA-carriers was measured in mixed leukocytes.ResultsOf 105 Caucasian Parkinson's disease participants (82.7% Afrikaner) with an average age of disease onset of 61.912.2years and 40 controls (age 73.4 +/- 12.4years) were included. Heterozygous GBA substitutions were identified in 12.38% of affected participants (p.G35A, p.E326K, p.I368T, p.T369M, p.N370S, p.P387L and p.K441N) and 5.00% of controls (p.E326K and p.T369M). The substitutions ranged from predicted benign to moderately damaging; with p.E326K and p.T369M most prevalent, followed by the Afrikaner Gaucher disease substitution p.P387L. Severe Gaucher disease mutations, like p.L444P, were absent in this cohort. Enzyme activity analysis revealed a nonsignificant reduction in the GBA-Parkinson's disease individuals (14.49 +/- 2.30nmol/h/mg protein vs. 15.98 +/- 3.06nmol/h/mg in control samples). GBA substitutions occur in both young-onset and late-onset Parkinson's cases in the cohort.ConclusionMild GBA substitutions that may not cause Gaucher disease were a common risk factor for Parkinson's disease in the participant group.

Published

2017

19. Expression and functional characterization of mutated glucocerebrosidase alleles causing Gaucher disease in Spanish patients

Author

Alfonso, Pilar, Rodríguez-Rey, José Carlos, Gañán, Alberto, Pérez-Calvo, Juan Ignacio, Giralt, Manuel, Giraldo, Pilar, and Pocoví, Miguel

Subjects

*GAUCHER'S disease, *ENZYMES, *HETEROGENEITY, *GENES

Abstract

Background: Gaucher disease (GD) is a heterogeneous disease characterized by an impaired activity of the lysosomal glucocerebrosidase. This heterogeneity is attributed in part to the existence of a large number of mutations in the corresponding gene. Subjects and methods: To establish genotype–phenotype relationships, we analyzed the residual enzyme activities of six naturally occurring mutations found in Spanish population in the glucocerebrosidase gene [c.160G > A (V15M), c.485T>C (M123T), c.914C>T (P266L), c.1124T>C (L336P), c.1207A>C (S364R) and c.1510–1512delTCT (S465del)]. The mutated genes were subcloned into the mammalian expression vector pCR® 3.1 and expressed by transient transfection in COS cells. The enzymatic activity of the expressed protein were measured and compared with the wild-type human glucocerebrosidase cDNA. Also, two previously alleles, c.1226A>G (N370S) and c.1448T>C (L444P), were used for comparative purposes. Results: The residual activity of the expressed proteins using the synthetic substrate (4-methylumbelliferyl-β-d-glucopyranoside, 4MU-Glu) ranged from 5.5% (for the 3-bp deletion) to 42.7% (for S364R mutation) of the activity of the wild-type enzyme. Conclusion: The present analyses may help to better understand the molecular basis and the pathogenesis of Gaucher disease. However, results of expression of mutated enzymes are necessary but not sufficient to explain the ultimate clinical outcome of Gaucher disease. [Copyright &y& Elsevier]

Published

2004

20. High Prevalence of the 55-bp Deletion (c.1263del55) in Exon 9 of the Glucocerebrosidase Gene Causing Misdiagnosis (for Homozygous N370S (c.1226A > G) Mutation) in Spanish Gaucher Disease Patients

Author

Torralba, M. A., Alfonso, P., Pérez-Calvo, J. I., Cenarro, A., Pastores, G. M., Giraldo, P., Civeira, F., and Pocovı, M.

Subjects

*GAUCHER'S disease, *LYSOSOMAL storage diseases, *GENETIC mutation

Abstract

ABSTRACTGaucher disease (GD) is the most frequent lysosomal storage disease, caused by mutations in the acid β-glucosidase gene (GBA). The c.1226A > G (N370S) mutation is associated with non-neuronopathic disease (type 1). However, we have observed some discrepancy between genotype and phenotype in Spanish Gaucher disease patients homozygous for the c.1226A > G mutation. A deletion of 55 bp in the exon 9 GBA gene, corresponding to the deleted portion of the β-glucosidase pseudogene, has been previously reported as a cause of erroneous assignment of 1226G/1226G homozygous patients when the genotype has been performed by PCR assay. We had originally identified 25 (out of 124) unrelated Gaucher disease patients as being putative homozygotes for the c.1226A > G mutation. By means of a new PCR-based assay, we were able to distinguish between the true homozygous patients and the carriers of the 55-bp deletion in exon 9 of the GBA gene. The 55-bp deletion was detected in 10 out of 25 samples (40%) [7 with the 55-bp deletion, 1 RecTL, 1 RecNciI (both including the deletion) and one rearrangement]. Such a high prevalence in this sample suggests that this allele can be more common than expected among GD patients. [Copyright &y& Elsevier]

Published

2002

21. Mutation analysis in 46 British and Irish patients with Gaucher's disease.

Author

Hatton, C. E., Cooper, A., Whitehouse, C., and Wraith, J. E.

Abstract

DNA from 46 unrelated patients with Gaucher's disease was analysed for 10 known mutations: 84GG(c84 G 85ins), N370S (c1226G), L444P (c1448C), R463C (c1504T), R496H (c1604A), IVS2+1, D409H (c1342C), RecNcil (c1448C-1498C), RecTL (c1342C-1498C), and c1263del (c1264-1318del). Fifty four mutations (90%) were identified in 30 patients with type I disease. These included a previously undescribed recombinant mutation RecA456P (c1448C-1484C). Thirteen (54%) of 24 type II alleles were identified, including one new point mutation N462K (c1503G) and one new 55bp deletion also incorporating the RecTL mutations c1263del+RecTL (c1264del-1498C). All four type III patients were homozygous for the L444P point mutation. Generally, patients with one copy of the N370S mutation had mild adult onset disease, regardless of the nature of their second mutation. Three exceptions had childhood onset disease and genotypes N370S/R463C, N370S/RecA456P, and N370S/?. The L444P/L444P genotype was thought to be associated with neurological disease. Two type I patients with this genotype who exhibited no central nervous system disease were identified, however. The R463C and c1263del mutations were found to be present at a higher frequency than reported in other populations and they should be included in any mutation screen of this population. The recombinant mutations RecA456P and c1263del+RecTL have not been previously described and are the fourth and fifth recombinant mutations identified in the glucocerebrosidase gene. [ABSTRACT FROM AUTHOR]

Published

1997

22. The Molecular Biology of Gaucher Disease

Author

Beutler, E., Sorge, J., Zimran, A., West, C., Kuhl, W., Westwood, B., Gelbart, T., Salvayre, Robert, editor, Douste-Blazy, Louis, editor, and Gatt, Shimon, editor

Published

1988

23. Impact of glucocerebrosidase mutations on motor and nonmotor complications in Parkinson's disease

Author

Kwiyoung Park, Hiroshi Hasegawa, Hiroshi Sugiyama, Kimiko Inoue, Harutoshi Fujimura, Tomoko Oeda, Yuko Mori, Hideyuki Sawada, Satoshi Tomita, Atsushi Umemura, and Masayuki Kohsaka

Subjects

Male, Aging, Psychosis, medicine.medical_specialty, Pathology, Parkinson's disease, MIBG scintigraphy, Neuroscience(all), Motor Disorders, Clinical Neurology, Gastroenterology, Cohort Studies, Clinical course, Glucocerebrosidase gene, Risk Factors, Internal medicine, Parietal Lobe, medicine, Dementia, Humans, Risk factor, Genetic Association Studies, Aged, Retrospective Studies, Tomography, Emission-Computed, Single-Photon, business.industry, General Neuroscience, Retrospective cohort study, Parkinson Disease, Middle Aged, medicine.disease, Ageing, Dyskinesia, Regional Blood Flow, SPECT, Mutation, Glucosylceramidase, Female, Neurology (clinical), medicine.symptom, Geriatrics and Gerontology, business, Glucocerebrosidase, Cohort study, Developmental Biology

Abstract

Homozygous mutations of the glucocerebrosidase gene (GBA) cause Gaucher disease (GD), and heterozygous mutations of GBA are a major risk factor for Parkinson's disease (PD). This study examined the impact of GBA mutations on the longitudinal clinical course of PD patients by retrospective cohort design. GBA-coding regions were fully sequenced in 215 PD patients and GD-associated GBA mutations were identified in 19 (8.8%) PD patients. In a retrospective cohort study, time to develop dementia, psychosis, wearing-off, and dyskinesia were examined. Survival time analysis followed a maximum 12-year observation (median 6.0 years), revealing that PD patients with GD-associated mutations developed dementia and psychosis significantly earlier than those without mutations (p < 0.001 and p = 0.017, respectively). Adjusted hazard ratios of GBA mutations were 8.3 for dementia (p < 0.001) and 3.1 for psychosis (p = 0.002). No statistically significant differences were observed for wearing-off and dyskinesia between the groups. N-isopropyl-p[123I] iodoamphetamine single-photon emission tomography pixel-by-pixel analysis revealed that regional cerebral blood flow was reduced in the bilateral parietal cortex, including the precuneus of GD-associated mutant PD patients, compared with matched PD controls without mutations.

Published

2015

24. Expression variation in lysosomal storage disorder genes

Author

Mason, Lyndel Ann and Mason, Lyndel Ann

Abstract

Metachromatic leukodystrophy (MLD) and Gaucher disease (GD) are caused by a deficiency of arylsulphatase A (ASA) and b-glucocerebrosidase (GBA), respectively. They are lysosomal storage disorders with a heterogeneous clinical spectrum encompassing visceral, skeletal and neurologic involvement resulting in high morbidity and mortality. The overall aim of this study is to elucidate the genetic component/s of high ASA and GBA enzyme activity in normal healthy individuals with the ultimate goal of using this information to produce greater protein activity from a recombinant protein. A wide variation in ASA and GBA enzyme activity levels has been observed in the normal population. The first objective of this project was to identify and characterise single nucleotide polymorphisms (SNPs) in the arylsulphatase A (ARSA) and glucocerebrosidase (GBA) genes that are responsible for determining the levels of expressed enzyme activity in the normal population. The second objective was to assess the contribution of transcriptional regulation and TCP80 mediated translational control to normal enzyme variation. TCP80, a translational control protein that interacts with the GBA coding region, is a splice variant of the interleukin binding factor 3 (ILF3) gene. Ten samples from individuals with high ASA activity and twenty samples from individuals with high GBA activity were screened for polymorphisms via denaturing high pressure liquid chromatography (dHPLC) and sequencing. The frequency of these polymorphisms in the normal population was determined using dot-blot hybridisation. Fifteen ARSA polymorphisms (4 promoter, 5 coding, 5 intronic and 1 poly(A) signal) and two GBA polymorphisms (1 intronic and 1 in 3¢-UTR) were identified. Two low frequency ASA polymorphisms (2723A > G, W193C) were found to be correlated with low activity, while another low frequency ASA polymorphism (1101+123C > T) was found to be correlated with high activity in a population of 113 individuals. Real time P

Published

2006

25. Identification of a novel recombinant allele in three unrelated Italian Gaucher patients: Implications for prognosis and genetic counseling

Author

Raffaella Mazzotti, Rosanna Gatti, Fiorina Giona, Gloria Bonuccelli, and Mirella Filocamo

Subjects

Adult, Genetic counseling, DNA Mutational Analysis, Molecular Sequence Data, Biology, medicine.disease_cause, Sequence Homology, Nucleic Acid, Genotype, medicine, gaucher disease, Humans, Point Mutation, Allele, Molecular Biology, Gene, Genotyping, Alleles, Aged, Gene Rearrangement, Genetics, Mutation, genetic counseling, Base Sequence, recombinant allele, DNA, Cell Biology, Hematology, Prognosis, genotyping, glucocerebrosidase gene, Amino Acid Substitution, Child, Preschool, Glucosylceramidase, Molecular Medicine, Glucocerebrosidase, Pseudogenes, Founder effect

Abstract

Gaucher disease (GD) results from deleterious mutations in the glucocerebrosidase gene. The relatively high frequency of some of these, especially at cDNA nucleotide 1226G (N370S) and at cDNA nucleotide 1448C (L444P), has led to the development of rapid screening techniques that can sometimes be misleading. In this report, we describe a novel rearrangement between the glucocerebrosidase gene and its pseudogene, identified as a consequence of a discrepancy between the genotype, homozygous for the common 1226G mutation, of an Italian patient with type 1 Gaucher disease, and the absence of the 1226G allele in her daughter. Additional investigations went on to reveal a novel recombinant allele beginning in intron 6 and extending through the rest of the coding sequence. Italian GD patients found homozygous for a specific mutation or with one or both alleles still unknown were further investigated and the novel recombinant allele was identified in an adult type 1 patient previously genotyped 1226G/1226G and in a young patient with an unknown genotype. The detection of this allele in three unrelated GD patients originating from the same geographic area in central Italy suggested a founder effect. This study emphasizes the implications of an accurate genotyping for the prognostic value of glucocerebrosidase genotype and reliable genetic counseling.

Published

2000

26. Uncoupling of osteoblast-osteoclast regulation in a chemical murine model of Gaucher disease.

Author

Mucci JM, Suqueli García F, de Francesco PN, Ceci R, Di Genaro S, Fossati CA, Delpino MV, and Rozenfeld PA

Subjects

Animals, Antigens, Differentiation metabolism, Bone Marrow Cells physiology, Calcification, Physiologic, Cell Differentiation, Cells, Cultured, Culture Media, Conditioned, Gaucher Disease chemically induced, Gaucher Disease metabolism, Inositol analogs & derivatives, Mice, Mice, Inbred C57BL, Mice, Knockout, Osteolysis metabolism, Tumor Necrosis Factor-alpha physiology, Gaucher Disease pathology, Osteoblasts metabolism, Osteoclasts physiology

Abstract

Gaucher disease (GD) is caused by mutations in the GBA gene that confer a deficient level of activity of glucocerebrosidase (GCase). This deficiency leads to accumulation of the glycolipid glucocerebroside in the lysosomes of cells of monocyte/macrophage system. Type I GD is the mildest form and is characterized by the absence of neuronopathic affection. Bone compromise in Gaucher disease patients is the most disabling aspect of the disease. However, pathophysiological aspects of skeletal alterations are still poorly understood. The homeostasis of bone tissue is maintained by the balanced processes of bone resorption by osteoclasts and formation by osteoblasts. We decided to test whether bone resorption and/or bone formation could be altered by the use of a chemical in vitro murine model of Gaucher disease. We used two sources of cells from monocyte/macrophages lineage isolated from normal mice, splenocytes (S) and peritoneal macrophages (PM), and were exposed to CBE, the inhibitor of GCase (S-CBE and PM-CBE, respectively). Addition of both conditioned media (CM) from S-CBE and PM-CBE induced the differentiation of osteoclasts precursors from bone marrow to mature and functional osteoclasts. TNF-α could be one of the factors responsible for this effect. On the other hand, addition of CM to an osteoblast cell culture resulted in a reduction in expression of alkaline phosphatase and mineralization process. In conclusion, these results suggest implication of changes in both bone formation and bone resorption and are consistent with the idea that both sides of the homeostatic balance are affected in GD., (© 2013.)

Published

2013

27. Glucocerebrosidase involvement in Parkinson disease and other synucleinopathies.

Author

Almeida Mdo R

Abstract

Mutations in both copies (homozygous or compound heterozygous) of the gene encoding the lysosomal enzyme glucocerebrosidase, which cleaves the glycolipid glucocerebroside into glucose and ceramide cause Gaucher disease. However, multiple independent studies have also reported an association between GBA mutations and Parkinsonism with an increased frequency of heterozygous GBA mutations in various cohorts of patients with parkinsonism and other Lewy body disorders. Furthermore, GBA mutation carriers exhibit diverse parkinsonian phenotypes and present a diffuse pattern of Lewy body distribution in the cerebral cortex. This review provides an overview of the genetic basis for this association in various diseases with dysfunction of the central nervous system in which affected individuals developed Parkinsonian symptoms. The emerging clinical, pathological, and genetic studies in neuronal synucleinopathies suggest a common underlying mechanism in the etiology of these neurodegenerative disorders.

Published

2012