Cognitive performance of
            <i>GBA</i>
            mutation carriers with early-onset PD

Alcalay, Roy N.; Caccappolo, Elise; Mejia‐Santana, Helen; Tang, Ming; Rosado, Llency; Reilly, Martha Orbe; Ruiz, Diana; Ross, Barbara; Verbitsky, Miguel; Kisselev, Sergey; Louis, Elan D.; Comella, Cynthia L.; Colcher, Amy; Jennings, Danna; Nance, Martha; Bressman, Susan; Scott, William K.; Tanner, Caroline M.; Mickel, Susan F.; Andrews, Howard; Waters, Cheryl; Fahn, Stanley; Côté, Lucien J.; Frucht, Steven J.; Ford, Blair; Rezak, Michael; Novak, Kevin; Friedman, Joseph H.; Pfeiffer, Ronald F.; Marsh, Laura; Hiner, Bradley C.; Siderowf, Andrew; Payami, Haydeh; Molho, Eric; Factor, Stewart A.; Ottman, Ruth; Clark, Lorraine N.; Marder, Karen

doi:10.1212/wnl.0b013e318253d54b

Cited by 238 publications

(244 citation statements)

References 29 publications

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“…Mutations in GBA are now recognized as an independent risk factor for development of cognitive impairment in patients with PD (24)(25)(26)(27). The Gba D409V/D409V mice present several distinct features of synucleinopathies, including cognitive impairment and pathogenic accumulation of α-synuclein, ubiquitin, and tau aggregates (21,22).…”

Section: Gz667161 Ameliorates Cognitive Impairment In the Gba-relatedmentioning

confidence: 99%

Glucosylceramide synthase inhibition alleviates aberrations in synucleinopathy models

Sardi

Viel

Clarke

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

167

161

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Mutations in the glucocerebrosidase gene (GBA) confer a heightened risk of developing Parkinson's disease (PD) and other synucleinopathies, resulting in a lower age of onset and exacerbating disease progression. However, the precise mechanisms by which mutations in GBA increase PD risk and accelerate its progression remain unclear. Here, we investigated the merits of glucosylceramide synthase (GCS) inhibition as a potential treatment for synucleinopathies. Two murine models of synucleinopathy (a Gaucher-related synucleinopathy model, Gba D409V/D409V and a A53T-α-synuclein overexpressing model harboring wild-type alleles of GBA, A53T-SNCA mouse model) were exposed to a brain-penetrant GCS inhibitor, GZ667161. Treatment of Gba D409V/D409V mice with the GCS inhibitor reduced levels of glucosylceramide and glucosylsphingosine in the central nervous system (CNS), demonstrating target engagement. Remarkably, treatment with GZ667161 slowed the accumulation of hippocampal aggregates of α-synuclein, ubiquitin, and tau, and improved the associated memory deficits. Similarly, prolonged treatment of A53T-SNCA mice with GZ667161 reduced membrane-associated α-synuclein in the CNS and ameliorated cognitive deficits. The data support the contention that prolonged antagonism of GCS in the CNS can affect α-synuclein processing and improve behavioral outcomes. Hence, inhibition of GCS represents a diseasemodifying therapeutic strategy for GBA-related synucleinopathies and conceivably for certain forms of sporadic disease.Parkinson's disease | GBA mutations | glucosylceramide synthase | Gaucher disease | Lewy body dementia

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Section: Gz667161 Ameliorates Cognitive Impairment In the Gba-relatedmentioning

confidence: 99%

Glucosylceramide synthase inhibition alleviates aberrations in synucleinopathy models

Sardi

Viel

Clarke

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

167

161

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“…Heterozygotes have a 10-30% chance of developing PD by age 80, which constitutes a 20-fold increase compared to non-carriers [7][8][9][10], and approximately 5-25% of "idiopathic" PD patients carry GBA mutations, making GBA mutations the greatest risk factor for PD discovered to date [11,12].…”

Section: G O'regan Et Al / Gba In Parkinson Diseasementioning

confidence: 99%

“…Several studies assessed the difference in cognitive performance between PD patients with and without GBA mutations [10,55,58,[61][62][63][65][66][67][68][69][70]; according to a recent meta-analysis, the risk of cognitive impairment is estimated to be 3 times higher for patients with GBA mutations [49]. However, significant differences in cognitive function between PD patients with and without GBA mutations were not confirmed in some studies [13,62,71,72].…”

Section: Non Motor Featuresmentioning

confidence: 99%

“…There is poor agreement on the role of the GBA polymorphisms E326K on cognition: one study found that both E326K patients and GBA mutation patients have a higher risk of cognitive deterioration [75], another found that the association between GBA and cognitive decline was significant in E326K patients but not in PD patients with GBA mutations [53] and, finally, patients with PD and GBA mutations but not E326K or other polymorphisms progress to dementia more rapidly than non-carriers [52]. Specific cognitive profiles have been associated with GBA mutations in PD patients: one study focused on memory and visuospatial domains [10], while another on abstraction and orientation domains [61]. Impairment in working memory, executive function and visuospatial abilities seemed to be a characteristic of PD both with GBA mutations and E326K variant [75].…”

Section: Non Motor Featuresmentioning

confidence: 99%

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Glucocerebrosidase Mutations in Parkinson Disease

O’Regan

deSouza

Balestrino

et al. 2017

JPD

102

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Abstract.Following the discovery of a higher than expected incidence of Parkinson Disease (PD) in Gaucher disease, a lysosomal storage disorder, mutations in the glucocerebrocidase (GBA) gene, which encodes a lysosomal enzyme involved in sphingolipid degradation were explored in the context of idiopathic PD. GBA mutations are now known to be the single largest risk factor for development of idiopathic PD. Clinically, on imaging and pharmacologically, GBA PD is almost identical to idiopathic PD, other than certain features that can be identified in the specialist research setting but not in routine clinical practice. In patients with a known GBA mutation, it is possible to monitor for prodromal signs of PD. The clinical similarity with idiopathic PD and the chance to identify PD at a pre-clinical stage provides a unique opportunity to research therapeutic options for early PD, before major irreversible neurodegeneration occurs. However, to date, the molecular mechanisms which lead to this increased PD risk in GBA mutation carriers are not fully elucidated. Experimental models to define the molecular mechanisms and test therapeutic options include cell culture, transgenic mice and other in vivo models amenable to genetic manipulation, such as drosophilia. Some key pathological pathways of interest in the context of GBA mutations include alpha synuclein aggregation, lysosomal-autophagy axis changes and endoplasmic reticulum stress. Therapeutic agents that exploit these pathways are being developed and include the small molecule chaperone Ambroxol. This review aims to summarise the main features of GBA-PD and provide insights into the pathological relevance of GBA mutations on molecular pathways and the therapeutic implications for PD resulting from investigation of the role of GBA in PD.

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“…The frequency of GBA1 mutation in subjects with mixed pathology of LB-type and AD-type was in between that of pure LB and pure AD subjects, suggesting a strong association between GBA1 mutation and LB-type neuropathological changes. Another study suggested that GBA1 mutation status might be an independent risk factor for cognitive impairment in patients with PD (Alcalay et al , 2012 ) (also see below for the relationship between GBA1 mutation and LB pathology).…”

Section: Gba1 Mutations In Parkinson ' S Diseasementioning

confidence: 99%

Glucocerebrosidase, a new player changing the old rules in Lewy body diseases

Yang

Lee

Lee³

et al. 2013

Biological Chemistry

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Mutations in the gene encoding glucocerebrosidase ( GBA1 ) cause Gaucher disease (GD), a lysosomal storage disease with recessive inheritance. Glucocerebrosidase (GCase) is a lysosomal lipid hydrolase that digests glycolipid substrates, such as glucosylceramide and glucosylsphingosine. GBA1 mutations have been implicated in Lewy body diseases (LBDs), such as Parkinson ' s disease and dementia with Lewy bodies. Parkinsonism occurs more frequently in certain types of GD, and GBA1 mutation carriers are more likely to have LBDs than noncarriers. Furthermore, GCase is often found in Lewy bodies, which are composed of α -synuclein fibrils as well as a variety of proteins and vesicles. In this review, we discuss potential mechanisms of action of GBA1 mutations in LBDs with particular emphasis on α -synuclein aggregation by reviewing the current literature on the role of GCase in lysosomal functions and glycolipid metabolism.

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Cognitive performance of GBA mutation carriers with early-onset PD

Cited by 238 publications

References 29 publications

Glucosylceramide synthase inhibition alleviates aberrations in synucleinopathy models

Glucosylceramide synthase inhibition alleviates aberrations in synucleinopathy models

Glucocerebrosidase Mutations in Parkinson Disease

Glucocerebrosidase, a new player changing the old rules in Lewy body diseases

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