Gaucher disease ascertained through a Parkinson's center: Imaging and clinical characterization

Saunders‐Pullman, Rachel; Hagenah, Johann; Dhawan, Vijay; Stanley, Kaili; Pastores, Gregory M.; Sathe, Swati; Tagliati, Michele; Condefer, Kelly A.; Palmese, Christina A.; Brüggemann, Norbert; Klein, Christine; Roe, AM; Kornreich, Ruth; Ozelius, Laurie J.; Bressman, Susan

doi:10.1002/mds.23046

Cited by 80 publications

(83 citation statements)

References 51 publications

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“…Similar to PINK1 17 and glucocerebrosidaseassociated PD, 16,18 but unlike PD due to parkin mutations, 15 most 8 but not all 19 LRRK2 mutation studies support the idea that olfaction is impaired in this genetic form. 8 While the degree of olfactory pathology has not been formally quantified in PD and LRRK2 PD, our clinical data support the notion that LRRK2 pathology may not be as extensive.…”

Section: Resultsmentioning

confidence: 68%

Olfactory dysfunction in LRRK2 G2019S mutation carriers

Saunders‐Pullman

Stanley

Wang³

et al. 2011

Neurology

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Section: Resultsmentioning

confidence: 68%

Olfactory dysfunction in LRRK2 G2019S mutation carriers

Saunders‐Pullman

Stanley

Wang³

et al. 2011

Neurology

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“…These studies revealed sensory-driven compensatory mechanisms in cortico-thalamo-cortical circuits (Bezard et al, 2003;Escola et al, 2003;Pessiglione et al, 2003), but it remains unclear to what extent these animal models can be generalized to human Parkinson's disease. More recently, neuroimaging studies in non-manifesting carriers of mutations known to cause monogenetic forms of Parkinson's disease, such as Parkin (PARK2) or PINK1 (PARK6) mutations (Broussolle et al, 2000;Hilker et al, 2001;Khan et al, 2002aKhan et al, , b, 2005bWalter et al, 2004;Buhmann et al, 2005;Baumer et al, 2007;Binkofski et al, 2007;Hagenah et al, 2007Hagenah et al, , 2008Schweitzer et al, 2007;van Nuenen et al, 2009a, b;Reetz et al, 2010;Saunders-Pullman et al, 2010), have been used to map cerebral changes occurring before the clinical onset of Parkinson's disease (Farrer, 2006). Non-manifesting carriers of these mutations showed structural and functional alterations similar to those observed in idiopathic Parkinson's disease, for example, nigrostriatal and premotor dysfunctions.…”

Section: Introductionmentioning

confidence: 99%

Cerebral pathological and compensatory mechanisms in the premotor phase of leucine-rich repeat kinase 2 parkinsonism

Nuenen

Helmich

Ferraye

et al. 2012

Brain

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Compensatory cerebral mechanisms can delay motor symptom onset in Parkinson's disease. We aim to characterize these compensatory mechanisms and early disease-related changes by quantifying movement-related cerebral function in subjects at significantly increased risk of developing Parkinson's disease, namely carriers of a leucine-rich repeat kinase 2-G2019S mutation associated with dominantly inherited parkinsonism. Functional magnetic resonance imaging was used to examine cerebral activity evoked during internal selection of motor representations, a core motor deficit in clinically overt Parkinson's disease. Thirty-nine healthy first-degree relatives of Ashkenazi Jewish patients with Parkinson's disease, who carry the leucinerich repeat kinase 2-G2019S mutation, participated in this study. Twenty-one carriers of the leucine-rich repeat kinase 2-G2019S mutation and 18 non-carriers of this mutation were engaged in a motor imagery task (laterality judgements of left or right hands) known to be sensitive to motor control parameters. Behavioural performance of both groups was matched. Mutation carriers and non-carriers were equally sensitive to the extent and biomechanical constraints of the imagined movements in relation to the current posture of the participants' hands. Cerebral activity differed between groups, such that leucine-rich repeat kinase 2-G2019S carriers had reduced imagery-related activity in the right caudate nucleus and increased activity in the right dorsal premotor cortex. More severe striatal impairment was associated with stronger effective connectivity between the right dorsal premotor cortex and the right extrastriate body area. These findings suggest that altered movement-related activity in the caudate nuclei of leucine-rich repeat kinase 2-G2019S carriers might remain behaviourally latent by virtue of cortical

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“…At the Movement Disorder Center at Beth Israel Medical Center, patients with two or more Ashkenazi Jewish grandparents who met diagnostic criteria for PD were invited to participate in a genetic study of PD (Pankratz et al 2002). Consent was obtained, blood or saliva samples were collected, and DNA was isolated and screened for the eight common Ashkenazi Jewish GBA mutations (N370S, L444P, 84GG, IVS2+1G!A, V394L, del55bp, D409H, and R496H) (Saunders-Pullman et al 2010) and the leucine-rich repeat kinase 2 (LRRK2) G2019S mutation (Ozelius et al 2006). The institutional review board at Beth Israel Medical Center approved the study procedures, and all subjects provided informed consent.…”

Section: Methodsmentioning

confidence: 99%

“…As cognitive impairment is associated with psychosis in PD and GBA mutations are associated with DLB (Nalls et al 2013;Fenelon et al 2000), it is not surprising that there is a high prevalence of hallucinations in GBA-PD (Neumann et al 2009). Cognitive impairment is also a prominent feature of PD in patients with biallelic GBA mutations (Saunders-Pullman et al 2010), but this represents a much smaller group of patients compared to those with monoallelic GBA mutations.…”

Section: Introductionmentioning

confidence: 99%

Cognitive and Antipsychotic Medication Use in Monoallelic GBA-Related Parkinson Disease

et al. 2014

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Mutations in glucosidase, beta, acid (GBA) are associated with cognitive impairment in Parkinson disease (PD) as well as dementia with Lewy bodies. For both of these diseases, dementia and hallucinations are typically treated with cholinesterase inhibitors and antipsychotics. However, in some lysosomal storage disorders certain antipsychotic medications are poorly tolerated. This study examined cholinesterase inhibitor and antipsychotic use in monoallelic GBA-related PD to explore potential pharmacogenetic relationships. Monoallelic GBA mutation carriers with PD (GBA-PD) with at least two clinic visits (n ¼ 34) were matched for age-of-onset and gender to GBA and leucine-rich repeat kinase 2 (LRRK2) mutation negative idiopathic PD subjects (IPD) (n ¼ 60). Information regarding cholinesterase inhibitor and antipsychotic use as well as impaired cognition (UPDRS Mentation >1) and hallucinations (UPDRS Thought Disorder >1) were obtained. GBA-PD more frequently reported hallucinations (HR ¼ 5.0; p ¼ 0.01) and they were more likely to have cognitive impairment but this was not statistically significant (HR 2.2, p ¼ 0.07). Antipsychotic use was not significantly different between GBA-PD and IPD (HR ¼ 1.9; p ¼ 0.28), but GBA-PD were more likely to have sustained cholinesterase inhibitor use (HR ¼ 3.1; p ¼ 0.008), even after adjustment for cognition and hallucinations. Consistent with reports of worse cognition, GBA-PD patients are more likely to use cholinesterase inhibitors compared to IPD. While there was no difference in antipsychotic use between IPD and GBA-PD, persistent use of quetiapine in GBA-PD suggests that it is tolerated and that a significant interaction is unlikely. Further prospective study in larger samples with more extensive cognitive assessment is warranted to better understand pharmacogenetic relationships in GBA-PD.

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Gaucher disease ascertained through a Parkinson's center: Imaging and clinical characterization

Cited by 80 publications

References 51 publications

Olfactory dysfunction in LRRK2 G2019S mutation carriers

Olfactory dysfunction in LRRK2 G2019S mutation carriers

Cerebral pathological and compensatory mechanisms in the premotor phase of leucine-rich repeat kinase 2 parkinsonism

Cognitive and Antipsychotic Medication Use in Monoallelic GBA-Related Parkinson Disease

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