WARS2 mutations cause dopa-responsive early-onset parkinsonism and progressive myoclonus ataxia

Matej Skorvanek; Irena Rektorova; Wim Mandemakers; Matias Wagner; Robert Steinfeld; Laura Orec; Vladimir Han; Petra Pavelekova; Alexandra Lackova; Kristina Kulcsarova; Miriam Ostrozovicova; Zuzana Gdovinova; Barbara Plecko; Theresa Brunet; Riccardo Berutti; Demy J S Kuipers; Valerie Boumeester; Petra Havrankova; M A J Tijssen; Rauan Kaiyrzhanov; Mie Rizig; Henry Houlden; Juliane Winkelmann; Vincenzo Bonifati; Michael Zech; Robert Jech

doi:10.1016/j.parkreldis.2021.11.030

WARS2 mutations cause dopa-responsive early-onset parkinsonism and progressive myoclonus ataxia

Parkinsonism Relat Disord. 2022 Jan:94:54-61. doi: 10.1016/j.parkreldis.2021.11.030. Epub 2021 Dec 2.

Authors

Matej Skorvanek¹, Irena Rektorova², Wim Mandemakers³, Matias Wagner⁴, Robert Steinfeld⁵, Laura Orec⁶, Vladimir Han⁷, Petra Pavelekova⁷, Alexandra Lackova⁷, Kristina Kulcsarova⁷, Miriam Ostrozovicova⁷, Zuzana Gdovinova⁷, Barbara Plecko⁸, Theresa Brunet⁹, Riccardo Berutti⁴, Demy J S Kuipers³, Valerie Boumeester³, Petra Havrankova¹⁰, M A J Tijssen¹¹, Rauan Kaiyrzhanov¹², Mie Rizig¹², Henry Houlden¹², Juliane Winkelmann¹³, Vincenzo Bonifati³, Michael Zech⁴, Robert Jech¹⁰

Affiliations

¹ Department of Neurology, P.J. Safarik University, Kosice, Slovak Republic; Department of Neurology, University Hospital of L. Pasteur, Kosice, Slovak Republic. Electronic address: mskorvanek@gmail.com.
² First Department of Neurology, Faculty of Medicine, St. Anne's University Hospital, and CEITEC, Masaryk University, Brno, Czech Republic.
³ Erasmus MC, University Medical Center Rotterdam, Department of Clinical Genetics, Rotterdam, Netherlands.
⁴ Institute of Neurogenomics, Helmholtz Zentrum München, Munich, Germany; Institute of Human Genetics, Technical University of Munich, Munich, Germany.
⁵ Division of Pediatric Neurology, University Children's Hospital Zurich, Zurich, Switzerland.
⁶ Division of Pediatric Neurology and Metabolic Medicine, Centre for Child and Adolescent Medicine, University Hospital Heidelberg, Heidelberg, Germany.
⁷ Department of Neurology, P.J. Safarik University, Kosice, Slovak Republic; Department of Neurology, University Hospital of L. Pasteur, Kosice, Slovak Republic.
⁸ Department of Pediatrics and Adolescent Medicine, Division of General Pediatrics, Medical University of Graz, Graz, Austria.
⁹ Institute of Human Genetics, Technical University of Munich, Munich, Germany.
¹⁰ Department of Neurology, Charles University, First Faculty of Medicine and General University Hospital in Prague, Prague, Czech Republic.
¹¹ Expertise Center Movement Disorders Groningen, University Medical Center Groningen, University of Groningen, Groningen, Netherlands.
¹² University College London, Institute of Neurology, Department of Neuromuscular Disorders, Queen Square, WC1N 3BG, London, UK.
¹³ Institute of Human Genetics, Technical University of Munich, Munich, Germany; Lehrstuhl für Neurogenetik, Technische Universität München, Munich, Germany; Munich Cluster for Systems Neurology, SyNergy, Munich, Germany.

PMID: 34890876
DOI: 10.1016/j.parkreldis.2021.11.030

Abstract

Introduction: Sixteen subjects with biallelic WARS2 variants encoding the tryptophanyl mitochondrial aminoacyl-tRNA synthetase, presenting with a neonatal- or infantile-onset mitochondrial disease, have been reported to date. Here we present six novel cases with WARS2-related diseases and expand the spectrum to later onset phenotypes including dopa-responsive early-onset parkinsonism and progressive myoclonus-ataxia.

Methods: Six individuals from four families underwent whole-exome sequencing within research and diagnostic settings. Following the identification of a genetic defect, in-depth phenotyping and protein expression studies were performed.

Results: A relatively common (gnomAD MAF = 0.0033) pathogenic p.(Trp13Gly) missense variant in WARS2 was detected in trans in all six affected individuals in combination with different pathogenic alleles (exon 2 deletion in family 1; p.(Leu100del) in family 2; p.(Gly50Asp) in family 3; and p.(Glu208*) in family 4). Two subjects presented with action tremor around age 10-12 years and developed tremor-dominant parkinsonism with prominent neuropsychiatric features later in their 20s. Two subjects presented with a progressive myoclonus-ataxia dominant phenotype. One subject presented with spasticity, choreo-dystonia, myoclonus, and speech problems. One subject presented with speech problems, ataxia, and tremor. Western blotting analyses in patient-derived fibroblasts showed a markedly decreased expression of the full-length WARS2 protein in both subjects carrying p.(Trp13Gly) and an exon-2 deletion in compound heterozygosity.

Conclusions: This study expands the spectrum of the disease to later onset phenotypes of early-onset tremor-dominant parkinsonism and progressive myoclonus-ataxia phenotypes.

Keywords: Early onset parkinsonism; Progressive myoclonus ataxia; WARS2; Whole exome sequencing.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Ataxia
Dihydroxyphenylalanine
Humans
Mutation
Myoclonus*
Parkinsonian Disorders* / drug therapy
Parkinsonian Disorders* / genetics
Phenotype
Spinocerebellar Degenerations*
Tremor
Tryptophan-tRNA Ligase* / genetics

Substances

Dihydroxyphenylalanine
Tryptophan-tRNA Ligase