Clinical and functional evidence for the pathogenicity of the LRRK2 p.Arg1067Gln variant

IF 6.7 1区医学 Q1 NEUROSCIENCES

NPJ Parkinson's Disease Pub Date : 2025-02-23 DOI:10.1038/s41531-025-00884-6

Shen-Yang Lim, Tzi Shin Toh, Jia Wei Hor, Jia Lun Lim, Lei Cheng Lit, Azlina Ahmad-Annuar, Yi Wen Tay, Jia Nee Foo, Ebonne Yulin Ng, Kalai Arasu Muthusamy, Norlinah Mohamed Ibrahim, Khairul Azmi Ibrahim, Louis Chew Seng Tan, Jannah Zulkefli, Anis Nadhirah Khairul Anuar, Kirsten Black, Pawel Lis, Fei Xie, Zhidong Cen, Kai Shi Lim, Katja Lohmann, Shalini Padmanabhan, Dario R. Alessi, Wei Luo, Eng King Tan, Esther Sammler, Ai Huey Tan

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引用次数: 0

Abstract

LRRK2-related Parkinson’s disease (LRRK2-PD) is the most frequent form of monogenic PD worldwide, with important therapeutic opportunities, exemplified by the advancement in LRRK2 kinase inhibition studies/trials. However, many LRRK2 variants, especially those found in underrepresented populations, remain classified as variants of uncertain significance (VUS). Leveraging on Malaysian, Singaporean, and mainland Chinese PD datasets (n = 4901), we describe 12 Chinese-ancestry patients harboring the LRRK2 p.Arg1067Gln variant, more than doubling the number of previously reported cases (total n = 23, 87% East Asian, mean age of onset: 53.9 years). We determine that this variant is enriched in East Asian PD patients compared to population controls (OR = 8.0, 95% CI: 3.0–20.9), and provide supportive data for its co-segregation with PD, albeit with incomplete penetrance. Utilizing established experimental workflows, this variant showed increased LRRK2 kinase activity, by ~2-fold compared to wildtype and higher than the p.Gly2019Ser variant. Taken together, p.Arg1067Gln should be reclassified from a VUS to pathogenic for causing LRRK2-PD.

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LRRK2 相关帕金森病（LRRK2-PD）是全球最常见的单基因帕金森病，具有重要的治疗机会，LRRK2 激酶抑制剂研究/试验的进展就是例证。然而，许多 LRRK2 变异，尤其是在代表性不足的人群中发现的 LRRK2 变异，仍被归类为意义不确定的变异 (VUS)。利用马来西亚、新加坡和中国大陆的帕金森病数据集（n = 4901），我们描述了 12 例携带 LRRK2 p.Arg1067Gln 变异的中国裔患者，比之前报告的病例数增加了一倍多（总人数 n = 23，87% 为东亚人，平均发病年龄：53.9 岁）。我们确定，与人群对照相比，该变异在东亚帕金森病患者中富集（OR = 8.0，95% CI：3.0-20.9），并提供了该变异与帕金森病共分离的支持性数据，尽管该变异具有不完全的渗透性。利用已建立的实验工作流程，该变异显示 LRRK2 激酶活性增加，与野生型相比增加了约 2 倍，高于 p.Gly2019Ser 变异。综上所述，p.Arg1067Gln 应从导致 LRRK2-PD 的 VUS 变异重新归类为致病性变异。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

NPJ Parkinson's Disease Medicine-Neurology (clinical)

CiteScore

9.80

自引率

5.70%

发文量

156

审稿时长

11 weeks

期刊介绍： npj Parkinson's Disease is a comprehensive open access journal that covers a wide range of research areas related to Parkinson's disease. It publishes original studies in basic science, translational research, and clinical investigations. The journal is dedicated to advancing our understanding of Parkinson's disease by exploring various aspects such as anatomy, etiology, genetics, cellular and molecular physiology, neurophysiology, epidemiology, and therapeutic development. By providing free and immediate access to the scientific and Parkinson's disease community, npj Parkinson's Disease promotes collaboration and knowledge sharing among researchers and healthcare professionals.