Penetrance of Parkinson’s disease in GBA1 carriers is depending on the variant severity and polygenic background

Emadeldin Hassanin
Zied Landoulsi
Sinthuja Pachchek
NCER-PD Consortium
Peter Krawitz
Carlo Maj
Rejko Krüger
Patrick May
Dheeraj Reddy Bobbili

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Abstract

Background

Heterozygous variants in the GBA1 gene cause Parkinson’s disease (PD) with variable penetrance and have been classified into severe, mild, and PD-specific risk variants based on their association with Gaucher’s disease (GD; mild and severe) or PD (risk variants). Polygenic risk scores (PRS) further modify PD susceptibility and may influence the age of onset in GBA1 variant carriers. Our study investigates the interaction between a genome wide PRS and pathogenic GBA1 variants ( GBA1 _PVs ), focusing on how established combined PD risk polymorphisms may influence GBA1 -related PD risk across different levels of GBA1 -mediated pathogenicity.

Methods

GBA1 variants were identified from whole exome sequencing data in the UK Biobank (UKB) cohort and from GBA1 -targeted PacBio sequencing in the Luxembourg Parkinson’s Study (LuxPark). PRSs were calculated for all participants using established genome-wide significant SNPs, excluding variants within the GBA1 locus, and then categorized based on both PRS levels and GBA1 _PVs carrier status. Carriers of GBA1 _PVs were further divided into ‘severe (Gaucher-related) +mild (PD-related)’ and ‘risk’ groups. To evaluate the relationship between PRS, GBA1 _PVs carrier status or severity, and PD risk, logistic regression and Cox proportional hazards regression were conducted with disease presence as the dependent variable.

Results

We identified GBA1 _PVs in 8.8% of PD patients in the UKB discovery cohort and 9.9% in the LuxPark replication cohort. GBA1 _PVs carriers had consistently higher PD risk compared to non-carriers across all PRS categories. In UKB, GBA1 _PVs carriers in the highest PRS category had a 2.3-fold increased risk of PD (OR: 2.34; 95% CI, 2.08-2.63) and cumulative incidence of 67% by the age of 75, while those in LuxPark had a 1.6-fold higher risk (OR: 1.64; 95% CI, 1.52-1.76), and cumulative incidence of 81% at the age of 75. Carriers of “severe+mild” GBA1 variants had nearly double the risk of PD compared to “risk” variant carriers, with ORs ranging from 2.05 to 3.69 in UKB and 1.73 to 1.98 in LuxPark. The interaction between the PRSs and GBA1 _PVs severity was similar in the two cohorts.

Conclusions

Our findings demonstrate that GBA1 _PVs carrier status and severity significantly impact PD risk, with severe variants conferring higher risk than risk ones. Additionally, PRS consistently increases both PD risk and GBA1 _PVs penetrance in an additive manner across all variant types, defining a genetic background that influences PD penetrance in GBA1 _PVs carriers. The presence of additional PD-associated risk variants in GBA1 carriers defines new avenues to incorporate PRS and genetic risk data into future clinical trial design and genetic counselling in GBA1 -associated PD.

Version published to 10.1101/2025.01.23.25320896v1 on medRxiv
Jan 28, 2025

An improved polygenic score for Parkinson’s disease partly explains variable penetrance of genetic Parkinson’s disease

This article has 37 authors:
1. Sebastian Sendel
2. Zied Landoulsi
3. Katja Lohmann
4. Björn-Hergen Laabs
5. Meike Kasten
6. Eva-Juliane Vollstedt
7. Tatiana Usnich
8. Alexander Balck
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11. Max Borsche
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14. Henrike Hanssen
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16. Andrew A. Hicks
17. Ulrike M. Krämer
18. Rejko Krüger
19. Gregor Kuhlenbäumer
20. Lara M. Lange
21. Wolfgang Lieb
22. Brit Mollenhauer
23. NCER-PD Consortium
24. Miriam Neis
25. Peter P. Pramstaller
26. Jannik Prasuhn
27. Eva Schaeffer
28. Manu Sharma
29. Meike Steinbach
30. Claudia Trenkwalder
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81. Rufus Akinyemi
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83. Laksh Malik
84. Raymond Owolabi
85. Yakub Nyandaiti
86. Hampton L. Leonard
87. Kolawole Wahab
88. Kathryn Step
89. Oladunni Abiodun
90. Carlos F. Hernandez
91. Fatima Abdulai
92. Hirotaka Iwaki
93. Soraya Bardien
94. Christine Klein
95. John Hardy
96. Henry Houlden
97. Kamalini Ghosh Galvelis
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