Publication: Association of LRRK2 p.A419V with Parkinson’s Disease in East Asians and analysis of age at onset
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KU Authors
Co-Authors
Lim, Kai Shi
Periñan, Maria Teresa
Chew, Elaine Guo Yan
Lee, Paul Suhwan
Akçimen, Fulya
Lim, Jia Lun
Koretsky, Mathew J.
Funayama, Manabu
Yoshino, Hiroyo
Hattori, Nobutaka
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Date
Language
eng
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No
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Abstract
Common and rare variants in LRRK2 influence Parkinson’s disease (PD) risk across diverse populations, and in this study, the rare p.A419V variant was investigated across multiple ancestry cohorts comprising over 200,000 PD cases and controls. In cases of East Asian (EAS) ancestry, p.A419V was significantly associated with increased risk of PD (OR = 2.9
95% CI: 1.66–5.10
p = 0.0002), and was not in linkage disequilibrium with other LRRK2 coding variants. The variant was significantly associated with a lower age at PD onset in the study cohort, while a meta-analysis of the EAS cases indicated a similar, albeit non-significant trend. LRRK2 protein modelling prediction indicated that binding sites for RAB8A, RAB29 and RAB32 were in close proximity to the p.A419V variant within the ARM domain. Together, these findings confirm the p.A419V as a significant PD risk factor in EAS populations, as well as highlight disease-relevant variants in the ARM domain and the link with LRRK2-RAB signaling. (Figure presented.) © The Author(s) 2026.
95% CI: 1.66–5.10
p = 0.0002), and was not in linkage disequilibrium with other LRRK2 coding variants. The variant was significantly associated with a lower age at PD onset in the study cohort, while a meta-analysis of the EAS cases indicated a similar, albeit non-significant trend. LRRK2 protein modelling prediction indicated that binding sites for RAB8A, RAB29 and RAB32 were in close proximity to the p.A419V variant within the ARM domain. Together, these findings confirm the p.A419V as a significant PD risk factor in EAS populations, as well as highlight disease-relevant variants in the ARM domain and the link with LRRK2-RAB signaling. (Figure presented.) © The Author(s) 2026.
Source
Publisher
Nature Research
Subject
Neurology
Citation
Has Part
Source
npj Parkinson's Disease
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Edition
DOI
10.1038/s41531-026-01265-3
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