Abstract
Hereditary ataxia and spastic paraplegia are heterogeneous monogenic neurodegenerative disorders. To date, a large number of individuals with such disorders remain undiagnosed. Here, we have assessed molecular diagnosis by gene panel sequencing in 105 early and late-onset hereditary ataxia and spastic paraplegia probands, in whom extensive previous investigations had failed to identify the genetic cause of disease. Pathogenic and likely-pathogenic variants were identified in 20 probands (19%) and variants of uncertain significance in ten probands (10%). Together these accounted for 30 probands (29%) and involved 18 different genes. Among several interesting findings, dominantly inherited KIF1A variants, p.(Val8Met) and p.(Ile27Thr) segregated in two independent families, both presenting with a pure spastic paraplegia phenotype. Two homozygous missense variants, p.(Gly4230Ser) and p.(Leu4221Val) were found in SACS in one consanguineous family, presenting with spastic ataxia and isolated cerebellar atrophy. The average disease duration in probands with pathogenic and likely-pathogenic variants was 31 years, ranging from 4 to 51 years. In conclusion, this study confirmed and expanded the clinical phenotypes associated with known disease genes. The results demonstrate that gene panel sequencing and similar sequencing approaches can serve as efficient diagnostic tools for different heterogeneous disorders. Early use of such strategies may help to reduce both costs and time of the diagnostic process.
Highlights
The spinocerebellar degenerative disorders; hereditary ataxias (HA) and hereditary spastic paraplegias (HSP) are heterogeneous disorders causing progressive gait difficulties due to degeneration of the cerebellum, corticospinal tracts, brainstem, and/or spinal cord [1]
We have evaluated the use of Gene panel sequencing (GPS) in 105 clinically well-characterized probands affected with HA or HSP in whom previous extensive investigations had failed to identify a genetic cause
A small perturbation in the expression of genes in the brain could lead to serious consequences and a number of neurological disorders including HA and HSP
Summary
The spinocerebellar degenerative disorders; hereditary ataxias (HA) and hereditary spastic paraplegias (HSP) are heterogeneous disorders causing progressive gait difficulties due to degeneration of the cerebellum, corticospinal tracts, brainstem, and/or spinal cord [1]. These disorders are relatively rare with an estimated total prevalence of 13.9/100,000 in southeast Norway [2]. HA is characterized by progressive limb and gait ataxia, loss of coordination and disturbances of speech and oculomotor control. Genetic diagnosis in neurodegenerative disorders decision to publish, or preparation of the manuscript
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