TY - JOUR
T1 - Phenotypic effect of GBA1 variants in individuals with and without Parkinson's disease: The RAPSODI study
AU - Toffoli, Marco
AU - Chohan, Harneek
AU - Mullin, Stephen
AU - Jesuthasan, Aaron
AU - Yalkic, Selen
AU - Koletsi, Sofia
AU - Menozzi, Elisa
AU - Rahall, Soraya
AU - Limbachiya, Naomi
AU - Loefflad, Nadine
AU - Higgins, Abigail
AU - Bestwick, Jonathan
AU - Lucas-Del-Pozo, Sara
AU - Fierli, Federico
AU - Farbos, Audrey
AU - Mezabrovschi, Roxana
AU - Lee-Yin, Chiao
AU - Schrag, Anette
AU - Moreno-Martinez, David
AU - Hughes, Derralynn
AU - Noyce, Alastair
AU - Colclough, Kevin
AU - Jeffries, Aaron R.
AU - Proukakis, Christos
AU - Schapira, Anthony H.V.
PY - 2023/11
Y1 - 2023/11
N2 - Background
Variants in the GBA1 gene cause the lysosomal storage disorder Gaucher disease (GD). They are also risk factors for Parkinson's disease (PD), and modify the expression of the PD phenotype.
The penetrance of GBA1 variants in PD is incomplete, and the ability to determine who among GBA1 variant carriers are at higher risk of developing PD, would represent an advantage for prognostic and trial design purposes.
Objectives
To compare the motor and non-motor phenotype of GBA1 carriers and non-carriers.
Methods
We present the cross-sectional results of the baseline assessment from the RAPSODI study, an online assessment tool for PD patients and GBA1 variant carriers. The assessment includes clinically validated questionnaires, a tap-test, the University of Pennsyllvania Smell Identification Test and cognitive tests. Additional, homogeneous data from the PREDICT-PD cohort were included.
Results
A total of 379 participants completed all parts of the RAPSODI assessment (89 GBA1-negative controls, 169 GBA1-negative PD, 47 GBA1-positive PD, 47 non-affected GBA1 carriers, 27 GD). Eighty-six participants were recruited through PREDICT-PD (43 non-affected GBA1 carriers and 43 GBA1-negative controls). GBA1-positive PD patients showed worse performance in visual cognitive tasks and olfaction compared to GBA1-negative PD patients. No differences were detected between non-affected GBA1 carriers carriers and GBA1-negative controls. No phenotypic differences were observed between any of the non-PD groups.
Conclusions
Our results support previous evidence that GBA1-positive PD has a specific phenotype with more severe non-motor symptoms. However, we did not reproduce previous findings of more frequent prodromal PD signs in non-affected GBA1 carriers.
AB - Background
Variants in the GBA1 gene cause the lysosomal storage disorder Gaucher disease (GD). They are also risk factors for Parkinson's disease (PD), and modify the expression of the PD phenotype.
The penetrance of GBA1 variants in PD is incomplete, and the ability to determine who among GBA1 variant carriers are at higher risk of developing PD, would represent an advantage for prognostic and trial design purposes.
Objectives
To compare the motor and non-motor phenotype of GBA1 carriers and non-carriers.
Methods
We present the cross-sectional results of the baseline assessment from the RAPSODI study, an online assessment tool for PD patients and GBA1 variant carriers. The assessment includes clinically validated questionnaires, a tap-test, the University of Pennsyllvania Smell Identification Test and cognitive tests. Additional, homogeneous data from the PREDICT-PD cohort were included.
Results
A total of 379 participants completed all parts of the RAPSODI assessment (89 GBA1-negative controls, 169 GBA1-negative PD, 47 GBA1-positive PD, 47 non-affected GBA1 carriers, 27 GD). Eighty-six participants were recruited through PREDICT-PD (43 non-affected GBA1 carriers and 43 GBA1-negative controls). GBA1-positive PD patients showed worse performance in visual cognitive tasks and olfaction compared to GBA1-negative PD patients. No differences were detected between non-affected GBA1 carriers carriers and GBA1-negative controls. No phenotypic differences were observed between any of the non-PD groups.
Conclusions
Our results support previous evidence that GBA1-positive PD has a specific phenotype with more severe non-motor symptoms. However, we did not reproduce previous findings of more frequent prodromal PD signs in non-affected GBA1 carriers.
U2 - 10.1016/j.nbd.2023.106343
DO - 10.1016/j.nbd.2023.106343
M3 - Article
SN - 0969-9961
VL - 188
JO - Neurobiology of Disease
JF - Neurobiology of Disease
IS - 0
ER -