Novel Homozygous Truncating Variant Widens the Spectrum of Early-Onset Multisystemic SYNE1 Ataxia

William Kristian Karlsson; Joan Lilja Sunnleyg Højgaard; Anna Vilhelmsen; Clarissa Crone; Birgit Andersen; Ian Law; Lisbeth Birk Møller; Troels Tolstrup Nielsen; Emilie Neerup Nielsen; Thomas Krag; Kirsten Svenstrup; Jørgen Erik Nielsen

doi:10.1007/s12311-021-01308-w

Novel Homozygous Truncating Variant Widens the Spectrum of Early-Onset Multisystemic SYNE1 Ataxia

Cerebellum. 2022 Jun;21(3):514-519. doi: 10.1007/s12311-021-01308-w. Epub 2021 Jul 28.

Authors

Affiliations

¹ Department of Neurology, University of Copenhagen, Rigshospitalet, Inge Lehmanns Vej 8, 2100, Copenhagen, Denmark. wkarlsson@dadlnet.dk.
² Department of Neurology, University of Copenhagen, Rigshospitalet, Inge Lehmanns Vej 8, 2100, Copenhagen, Denmark.
³ Department of Psychiatry, National Hospital of the Faroe Islands, Tórshavn, Faroe Islands.
⁴ Department of Neurophysiology, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark.
⁵ Department of Clinical Physiology, Nuclear Medicine & PET, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark.
⁶ Department of Clinical Genetics, Rigshospitalet Glostrup, University of Copenhagen, Copenhagen, Denmark.
⁷ Neurogenetics Clinic & Research Lab, Danish Dementia Research Centre, University of Copenhagen, Rigshospitalet, Copenhagen, Denmark.
⁸ Department of Neurology, Copenhagen Neuromuscular Center, University of Copenhagen, Copenhagen, Denmark.

PMID: 34318393
DOI: 10.1007/s12311-021-01308-w

Abstract

Pathogenic variants in the SYNE1 gene are associated with a phenotypic spectrum spanning from late-onset, slowly progressive, relatively pure ataxia to early-onset, fast progressive multisystemic disease. Since its first description in 2007 as an adult-onset ataxia in French Canadian families, subsequent identification of patients worldwide has widened the clinical spectrum and increased the number of identified pathogenic variants. We report a 20-year-old Faroese female with early-onset progressive gait problems, weakness, dysphagia, slurred speech, orthostatic dizziness, and urge incontinence. Neurological examination revealed mild cognitive deficits, dysarthria, broken slow pursuit, hypometric saccades, weakness with spasticity, hyperreflexia, absent ankle reflexes, ataxia, and wide-based, spastic gait. Magnetic resonance imaging displayed atrophy of the cerebellum, brainstem, and spinal cord. Severely prolonged central motor conduction time and lower motor neuron involvement was demonstrated electrophysiologically. Fluorodeoxyglucose-positron emission tomography (FDG-PET) scan showed hypometabolism of the cerebellum and right frontal lobe. Muscle biopsy revealed chronic neurogenic changes and near-absent immunostaining for Nesprin-1. Next-generation sequencing revealed a previously undescribed homozygous truncating, likely pathogenic variant in the SYNE1 gene. The patient's mother and paternal grandfather were heterozygous carriers of the variant. Her father's genotype was unobtainable. We expand the list of likely pathogenic variants in SYNE1 ataxia with a novel homozygous truncating variant with proximity to the C-terminus and relate it to a phenotype comprising early-onset cerebellar deficits, upper and lower motor neuron involvement and cognitive deficits. Also, we report novel findings of focally reduced frontal lobe FDG-PET uptake and motor evoked potential abnormalities suggestive of central demyelination.

Keywords: Ataxia; Autosomal recessive; Cerebellum; Nesprin; SYNE1; Spinocerebellar ataxia.

Publication types

Case Reports

MeSH terms

Canada
Cerebellar Ataxia* / complications
Cerebellar Ataxia* / diagnostic imaging
Cerebellar Ataxia* / genetics
Cytoskeletal Proteins* / genetics
Female
Fluorodeoxyglucose F18
Humans
Muscle Spasticity / genetics
Mutation
Nerve Tissue Proteins / genetics
Young Adult

Substances

Cytoskeletal Proteins
Nerve Tissue Proteins
SYNE1 protein, human
Fluorodeoxyglucose F18