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Burden of variants in Parkinson’s disease-associated genes in GBA mutation carriers

Y.L Sosero, E. Yu, P. Saini, L. Krohn, U. Rudakou, J. Ruskey, F. Asayesh, M. Estiar, S. Fahn, C. Waters, O. Monchi, Y. Dauvilliers, A. Espay, N. Dupré, L. Greenbaum, G. Rouleau, S. Hassin-Baer, E. Fon, R. Alcalay, Z. Gan-Or (Montreal, QC, Canada)

Meeting: MDS Virtual Congress 2020

Abstract Number: 508

Keywords:

Category: Parkinson's Disease: Genetics

Objective: The main objective of this study is to examine the burden of variants in genes that are known or suspected to be involved in PD in GBA-associated PD, as potential modifiers of risk among these patients.

Background: GBA variants are among the most common genetic risk factors associated with Parkinson’s disease (PD), present in up to 20% of patients with PD in different populations. The majority of GBA variant carriers do not develop PD, and there is a large heterogeneity in its clinical presentation. It is therefore clear that other factors, genetic and/or environmental, affect the development of GBA-associated PD.

Method: We compared the frequency of rare (minor allele frequency < 0.01) variants in 42 genes that are known or suspected to be involved in PD between 309 PD patients carrying a GBA variant (GBA-PD) and 2074 PD patients without GBA variants. Burden and optimized sequence Kernel association tests (SKAT-O) have been performed for each of the 42 genes.

Results: After Bonferroni correction for multiple testing, no significant association between GBA-PD and variants in the tested genes was observed. However, a nominally significant burden of GAK variants (p=0.00054) was found in the burden analysis of variants predicted to be pathogenic by Combined Annotation Dependent Depletion (CADD) score. One GAK nonsynonymous variant with a higher frequency in the GBA-PD group was located in a tensin phosphatase domain.

Conclusion: Based on these results, there is no strong evidence for burden of variants in PD-associated genes among GBA variant carriers. The nominally significant results suggest that larger studies are required to determine the potential role of these variants in GBA-PD

References: 1. Gan-Or Z, Amshalom I, Kilarski LL, et al. Differential effects of severe vs mild GBA mutations on Parkinson disease. Neurology 2015;84(9):880-887. 2. Alcalay RN, Levy OA, Waters CC, et al. Glucocerebrosidase activity in Parkinson’s disease with and without GBA mutations. Brain 2015;138(Pt 9):2648-2658. 3. Gan-Or Z, Giladi N, Rozovski U, et al. Genotype-phenotype correlations between GBA mutations and Parkinson disease risk and onset. Neurology 2008;70(24):2277-2283.

To cite this abstract in AMA style:

Y.L Sosero, E. Yu, P. Saini, L. Krohn, U. Rudakou, J. Ruskey, F. Asayesh, M. Estiar, S. Fahn, C. Waters, O. Monchi, Y. Dauvilliers, A. Espay, N. Dupré, L. Greenbaum, G. Rouleau, S. Hassin-Baer, E. Fon, R. Alcalay, Z. Gan-Or. Burden of variants in Parkinson’s disease-associated genes in GBA mutation carriers [abstract]. Mov Disord. 2020; 35 (suppl 1). https://www.mdsabstracts.org/abstract/burden-of-variants-in-parkinsons-disease-associated-genes-in-gba-mutation-carriers/. Accessed November 22, 2024.

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