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      Parkinson’s Disease and Fabry Disease: Clinical, Biochemical and Neuroimaging Analysis of Three Pedigrees

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          Abstract

          Background:

          Sporadic Parkinson’s disease (PD) patients have lower α-galactosidase A ( α-GAL A) enzymatic activity and Fabry disease (FD) patients potentially carry an increased risk of PD.

          Objective:

          Determination of PD prevalence in FD and clinical, biochemical and vascular neuroimaging description of FD pedigrees with concomitant PD.

          Methods:

          Clinical screening for PD in 229 FD patients belonging to 31 families, harbouring GLA gene mutation p.F113L, and subsequent pedigree analysis. Gender-stratified comparison of FD+/PD+ patients with their family members with FD but without PD (FD+/PD–) regarding Mainz scores, plasma & leukocytes α-GAL A enzymatic activity, urinary Gb3 and plasma Lyso-Gb3, vascular brain neuroimaging.

          Results:

          Prevalence of PD in FD was 1.3% (3/229) (3% in patients aged ≥50 years). Three FD patients, one female (73 years old) (P1) and two males (60 and 65 years old) (P2 and P3), three different pedigrees, presented akinetic-rigid PD, with weak response to levodopa (16% – 36%), and dopaminergic deficiency on 18F-DOPA PET. No pathogenic mutations were found in a PD gene panel. FD+/PD+ patients had worse clinical severity of FD (above upper 75% IQR in Mainz scores), and cortico-subcortical white matter/small vessel lesions. P3 patient was under enzyme therapy, started 1 year before PD diagnosis. P2-P3 patients had higher leucocyte α-GAL A activity (2,2-3 vs.1,0 (median)(nmol/h/mg)).

          Conclusion:

          We have shown a high prevalence of PD in a late-onset phenotype of FD, presenting high cerebrovascular burden and weak response to levodopa. Further studies will untangle how much of this PD phenotype is due to Gb3 deposition versus cerebrovascular lesions in the nigro-striatal network.

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          Most cited references24

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          Occurrence of Parkinson's syndrome in type I Gaucher disease.

          B. Bembi, T Turezkite, A Zimran (1996)
          Gaucher disease, the most prevalent glycolipid storage disorder, is classically subdivided into types according to the presence or absence of neurological involvement. Type I has hitherto been considered non-neuronopathic. We present six cases and a review of the literature of Parkinsonian symptoms in type I Gaucher disease patients. The hallmark of this atypical Parkinsonian syndrome is a relatively severe clinical course with early appearance of neurological signs in the 4th to 6th decade of life, aggressive progression of the signs and refractoriness to conventional anti-Parkinson therapy. We discuss the implications of these findings in the light of enzyme replacement therapy for Gaucher disease.
          Article 0 comments Cited 110 times – based on 0 reviews     Review now
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            Montreal Cognitive Assessment (MoCA): normative study for the Portuguese population.

            Sandra Freitas, Mário R Simões, Lara Alves (2011)
            The Montreal Cognitive Assessment (MoCA) is a brief cognitive screening instrument with good psychometric features and an excellent sensitivity in the early detection of mild cognitive decline. The MoCA was applied to a community-based sample of cognitively healthy adults (n = 650), stratified according to sociodemographic variables (age, gender, educational level, geographic region, geographic localization, and residence area), with a distribution similar to that observed in the Portuguese population. The normative data were determined according to age and education as these were the sociodemographic variables that most significantly contributed to the prediction of the MoCA scores, explaining 49% of their variance.
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              Gaucher disease with parkinsonian manifestations: does glucocerebrosidase deficiency contribute to a vulnerability to parkinsonism?

              N Tayebi (2003)
              Among the phenotypes associated with Gaucher disease, the deficiency of glucocerebrosidase, are rare patients with early onset, treatment-refractory parkinsonism. Sequencing of glucocerebrosidase in 17 such patients revealed 12 different genotypes. Fourteen patients had the common "non-neuronopathic" N370S mutation, including five N370S homozygotes. While brain glucosylsphingosine levels were not elevated, Lewy bodies were seen in the four brains available for study. The shared clinical and neuropathologic findings in this subgroup suggest that the deficiency in glucocerebrosidase may contribute to a vulnerability to parkinsonism.
              Article 0 comments Cited 82 times – based on 0 reviews     Review now
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                Author and article information

                Journal
                Journal ID (nlm-ta): J Parkinsons Dis
                Journal ID (iso-abbrev): J Parkinsons Dis
                Journal ID (publisher-id): JPD
                Title: Journal of Parkinson's Disease
                Publisher: IOS Press (Nieuwe Hemweg 6B, 1013 BG Amsterdam, The Netherlands )
                ISSN (Print): 1877-7171
                ISSN (Electronic): 1877-718X
                Publication date (Electronic, preprint): 24 September 2019
                Publication date (Electronic, pub): 13 January 2020
                Publication date (Electronic, collection): 2020
                Volume: 10
                Issue: 1
                Pages: 141-152
                Affiliations
                [a ]Neurology Department, Reference Center on Lysosomal Storage Disorders , Hospital da Senhora da Oliveira, EPE, Guimarães, Portugal
                [b ]Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho , Braga, Portugal; ICVS/3Bs PT Government Associate Laboratory, Braga/Guimarães, Portugal
                [c ]Cardiology Department, Reference Center on Lysosomal Storage Disorders , Hospital da Senhora da Oliveira, EPE, Guimarães, Portugal
                [d ]Neuroradiology Department, Reference Center on Lysosomal Storage Disorders , Hospital da Senhora da Oliveira, EPE, Guimarães, Portugal
                [e ]Anatomic Pathology Service, Pathology Department, Hospital and University Center of Porto , Porto, Portugal
                [f ]Newborn Screening, Metabolism and Genetic Unit, Genetics Department, National Institute for Health Doutor Ricardo Jorge (INSA)
                [g ]Centro Algoritmi, Campus Azurem, University of Minho , Guimarães, Braga, Portugal
                [h ]Genetics Department, Reference Center on Lysosomal Storage Disorders , Hospital Senhora da Oliveira, Guimarães, Portugal
                [i ]Laboratory of Clinical Pharmacology and Therapeutics, Faculdade de Medicina, Universidade de Lisboa, Lisbon, Portugal; Instituto de Medicina Molecular , Lisbon, Portugal; CNS – Campus Neurológico Sénior, Torres Vedras, Portugal
                [j ]European Reference Network for Hereditary Metabolic Disorders (MetabERN)
                Author notes
                [* ]Correspondence to: Prof. Dr. Miguel Gago, Serviço de Neurologia, Hospital da Senhora da Oliveira, EPE, Guimarães, Rua dos Cutileiros, Creixomil. 4835-044 Guimarães, Portugal. Tel.: +35 1919490689; E-mails: miguelfgago@ 123456yahoo.com , miguelgago@ 123456hospitaldeguimaraes.min-saude.pt .
                Article
                Publisher ID: JPD191704
                DOI: 10.3233/JPD-191704
                PMC ID: 7029331
                PubMed ID: 31594250
                SO-VID: e7fe3cb1-849f-4660-a0ad-e6dc07724c43
                Copyright © © 2020 – IOS Press and the authors. All rights reserved
                License:

                This is an open access article distributed under the terms of the Creative Commons Attribution Non-Commercial (CC BY-NC 4.0) License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

                History
                Categories
                Subject: Research Report

                Keywords: fabry disease,parkinson’s disease,gla,α-galactosidase a,gb3,brain magnetic resonance imaging
                Data availability:
                Keywords: fabry disease, parkinson’s disease, gla, α-galactosidase a, gb3, brain magnetic resonance imaging

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