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Disease
Symptom
Drug
Enzyme
Compound
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Target Concepts:
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Query: UMLS:C0002736 (
amyotrophic lateral sclerosis
)
19,048
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The frequency of
amyotrophic lateral sclerosis
(
ALS
) mutations has been extensively investigated in several populations; however, a systematic analysis in Turkish cases has not been reported so far. In this study, we screened 477
ALS
patients for mutations, including 116 familial
ALS
patients from 82 families and 361 sporadic
ALS
(sALS) cases. Patients were genotyped for C9orf72 (18.3%), SOD1 (12.2%), FUS (5%), TARDBP (3.7%), and UBQLN2 (2.4%) gene mutations, which together account for approximately 40% of familial
ALS
in Turkey. No SOD1 mutations were detected in sALS patients; however, C9orf72 (3.1%) and UBQLN2 (0.6%) explained 3.7% of sALS in the population. Exome sequencing revealed mutations in OPTN, SPG11, DJ1, PLEKHG5,
SYNE1
, TRPM7, and SQSTM1 genes, many of them novel. The spectrum of mutations reflect both the distinct genetic background and the heterogeneous nature of the Turkish
ALS
population.
...
PMID:The distinct genetic pattern of ALS in Turkey and novel mutations. 2568 89
Mutations in
SYNE1
have been originally described to cause a slowly progressive, pure cerebellar ataxia (spinocerebellar ataxia, autosomal-recessive 8; SCAR8). Notably, recent studies revealed that affected patients with
SYNE1
-associated ataxia can present with complex phenotypes rather than pure cerebellar ataxia, including motor neuron and brainstem dysfunctions. We herein report a Japanese patient diagnosed with juvenile
amyotrophic lateral sclerosis
(
ALS
) with a complex phenotype, who carried compound heterozygous pathogenic variants in
SYNE1
. Of the variants, one was a novel frameshift variant and the other was a nonsense variant previously reported as pathogenic for SCAR8. The patient showed an early age at onset with a relatively slow but progressive course of
ALS
, accompanied by cognitive decline. Our findings suggest that the clinical spectrum of patients carrying pathogenic
SYNE1
variants is broader than expected, and
SYNE1
variants should be considered in patients diagnosed with juvenile
ALS
, even without prominent cerebellar ataxia.
...
PMID:Juvenile amyotrophic lateral sclerosis with complex phenotypes associated with novel
SYNE1
mutations. 3287 32
A 24-year-old female presented with wasting and weakness of both hands and fasciculations over the chin since 12 years, followed by imbalance while walking and speech changes since 10 years. Her 12-year-old sister also had a similar clinical presentation. There were fasciculations over the chin, tongue, hands, back, thighs with wasting and weakness in tongue, and C7, C8, T1 segments in both upper limbs along with bipyramidal signs. There was limb and gait ataxia. Magnetic resonance imaging brain showed pancerebellar atrophy, and electromyography was suggestive of anterior horn cell involvement in bulbar, cervical, thoracic, and lumbar segments. Next-generation sequencing identified a novel likely pathogenic deletion mutation: chr6:152527389_152527399del, c.22711_22721del, and p.Ala7571ArgfsTer4 in exon 125 of synaptic nuclear envelope protein 1 (
SYNE1
) gene. This mutation leads to frameshift and premature termination of the protein 'Nesprin 1'.
Amyotrophic lateral sclerosis
-like presentation followed by cerebellar ataxia have been described with
SYNE1
ataxia. This unique phenotype and novel deletion mutation of
SYNE1
gene is the first case reported from India.
...
PMID:Synaptic Nuclear Envelope Protein 1 (SYNE 1) Ataxia with Amyotrophic Lateral Sclerosis-like Presentation: A Novel Synaptic Nuclear Envelope Protein 1 (SYNE 1) Gene Deletion Mutation from India. 3322 74
