Leigh syndrome with developmental regression and ataxia due to a novel splicing variant in the PMPCB gene

Leigh syndrome with developmental regression and ataxia due to a novel splicing variant in the PMPCB gene

Only five children with pathogenic PMPCB gene variants have been described and all carried missense variants. Clinical features included a Leigh-like syndrome of developmental regression, basal ganglia lesions and ataxia with or without dystonia and epilepsy. Three of the five died in childhood and...

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Veröffentlicht in:Journal of human genetics 2024-06, Vol.69 (6), p.283-285
Hauptverfasser: Matthews, Emma, Whittle, Ella F, Khan, Faraan, McEntagart, Meriel, Carroll, Christopher J
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Age
Ataxia
Ataxia - genetics
Ataxia - pathology
Atrophy
Basal ganglia
Brain research
Brief Communication
Children
Crystal structure
Dystonia
Ear diseases
Epilepsy
Female
Genes
Genetics
Humans
Illnesses
Leigh Disease - genetics
Leigh Disease - pathology
Leigh-like syndrome
Male
Medical imaging
Neuroimaging
Otitis media
Proteins
RNA Splicing - genetics
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Zusammenfassung:Only five children with pathogenic PMPCB gene variants have been described and all carried missense variants. Clinical features included a Leigh-like syndrome of developmental regression, basal ganglia lesions and ataxia with or without dystonia and epilepsy. Three of the five died in childhood and none was older than age six when described. We report the first splice site variant in the PMPCB gene in a 39-year old individual who experienced developmental regression and ataxia following otitis media in childhood. A minigene assay confirms this variant results in aberrant splicing and skipping of exon 12.
ISSN:1434-5161
1435-232X
DOI:10.1038/s10038-024-01226-9