Rare but Relevant: Assessing Variants in Dystonia-linked Genes in Parkinson’s Disease

Lara M. Lange
Zih-Hua Fang
Laurel Screven
Ai Huey Tan
Roy N. Alcalay
Rim Amouri
Roberta Bovenzi
Matilda Fenn
Joshua L. I. Frost
Joseph Jankovic
Simona Jasaityte
Zane Jaunmuktane
Beomseok Jeon
Ignacio Juan Keller Sarmiento
Rejko Krüger
Gregor Kuhlenbäumer
Chin-Hsien Lin
Lukas Pavelka
Maria Teresa Periñan
Samia Ben Sassi
Tommaso Schirinzi
Jung Hwan Shin
Joshua M. Shulman
Yi Wen Tay
Ryan Uitti
Tom Warner
Zbigniew K. Wszolek
Lesley Wu
Ruey-Meei Wu
Kirsten E. Zeuner
Cornelis Blauwendraat
Andrew Singleton
Niccolò E. Mencacci
Huw R. Morris
Shen-Yang Lim
Katja Lohmann
Christine Klein
Global Parkinson’s Genetics Program (GP2)

0 evaluations Published on Jul 11, 2025

This article on Sciety

Abstract

Background

Dystonia and Parkinson’s disease (PD) show clinical and genetic overlap, but the relevance of dystonia gene variants in PD remains unclear.

Objective

To assess the frequency of dystonia-linked pathogenic variants in PD.

Methods

We screened sequencing data from 15,738 individuals (7,851 PD, 4,287 atypical parkinsonism, and 3,600 unaffected) from GP2 and AMP-PD for variants in genes linked to isolated dystonia, dystonia-parkinsonism, and myoclonus-dystonia.

Results

Pathogenic variants were only identified in PD patients. Forty-five PD individuals (0.57%) carried 26 distinct (likely) pathogenic variants in nine dystonia-linked genes, most frequently in GCH1, followed by VPS16.

Conclusion

Though rare, pathogenic variants in dystonia-linked genes are present in clinically and pathologically diagnosed PD. Our results reinforce GCH1 as a PD-relevant gene with clinical implications, while variants identified in other genes are rare and of sometimes uncertain relation to the PD phenotype.

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