Entry - #614306 - COGNITIVE IMPAIRMENT WITH OR WITHOUT CEREBELLAR ATAXIA; CIAT - OMIM

 
 
# 614306

COGNITIVE IMPAIRMENT WITH OR WITHOUT CEREBELLAR ATAXIA; CIAT


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
12q13.13 Cognitive impairment with or without cerebellar ataxia 614306 AD 3 SCN8A 600702
Clinical Synopsis
 

INHERITANCE
- Autosomal dominant
HEAD & NECK
Eyes
- Optic nerve hypoplasia (1 patient)
- Gaze-evoked nystagmus (1 patient)
- Esophoria (1 patient)
- Amblyopia (1 patient)
MUSCLE, SOFT TISSUES
- Hypotonia (in some patients)
NEUROLOGIC
Central Nervous System
- Global developmental delay
- Impaired intellectual development
- Ataxia (in some patients)
- Language delay
- Dysmetria (1 patient)
- Dysarthria (1 patient)
- Cerebellar atrophy seen on MRI (1 patient)
Behavioral Psychiatric Manifestations
- Attention deficit-hyperactivity disorder
- Emotional lability
MOLECULAR BASIS
- Caused by mutation in the voltage-gated sodium channel, type VIII, alpha subunit gene (SCN8A, 600702.0001)
▲ Close

TEXT

A number sign (#) is used with this entry because of evidence that cognitive impairment with or without cerebellar ataxia (CIAT) is caused by heterozygous mutation in the SCN8A gene (600702) on chromosome 12q13.

Clinical Features

Trudeau et al. (2006) reported a family of Swedish and Norwegian origin with highly variable neurologic deficits. The proband was a 9-year-old boy with markedly delayed psychomotor development, attention deficit disorder, and cerebellar ataxia. Features included ataxic wide-based gait, dysmetria in the upper limbs, and dysarthria, with normal strength, tone, and reflexes. He also had esophoria, amblyopia, and gaze-evoked nystagmus. Brain MRI showed moderate pancerebellar atrophy, accentuated in the vermal and parasagittal regions, as well as optic nerve hypoplasia. There were no cerebral abnormalities. His mother and maternal aunt had a history of emotional instability and mild cognitive impairment, and a first cousin had attention deficit-hyperactivity disorder (ADHD; 143465). A brother of the proband was noted to have impaired cognition and another cousin was noted to have ADHD, but they were not studied at the molecular level. In addition, none of the family members besides the proband was available for formal clinical evaluation or brain imaging studies. The proband was ascertained during a study of 151 patients with ataxia who were screened specifically for mutations in the SCN8A gene.

Wagnon et al. (2017) reported 2 unrelated children, a 7-year-old girl and a 10-year-old boy, with global developmental delay and impaired intellectual development (IQ of 73 and 56, respectively). The girl had delayed language, hypotonia that resolved with time, and ADHD; she was able to attend a special school. The boy had severe speech delay, temper tantrums, and a history of unsteady gait. Neither patient had seizures, and brain imaging performed in 1 patient was normal.


Inheritance

The transmission pattern of CIAT in the family reported by Trudeau et al. (2006) was consistent with autosomal dominant inheritance with variable expressivity.


Molecular Genetics

Trudeau et al. (2006) screened the 26 coding exons of SCN8A in 151 patients with inherited or sporadic ataxia and no mutations in known ataxia-related genes. The SCN8A gene was chosen for study because it is widely expressed in neurons of the central and peripheral nervous systems, and because mutations in the mouse ortholog result in ataxia and other movement disorders. A heterozygous 2-bp deletion in exon 24 (600702.0001) was identified in 1 patient, a 9-year-old boy with mental retardation, pancerebellar atrophy, and ataxia. Three additional family members who were heterozygous for the mutation exhibited milder cognitive behavioral deficits including ADHD. However, Trudeau et al. (2006) noted that it was unclear whether the relatives of the proband had a milder version of the neurologic abnormalities seen in the proband due to haploinsufficiency for SCN8A, or if the proband's symptoms were caused by an unrelated developmental disorder.

In 2 unrelated children with CIAT, Wagnon et al. (2017) identified de novo heterozygous missense mutations in the SCN8A gene (G964R, 600702.0013 and E1218K, 600702.0014). The mutations, which were found by exome sequencing, occurred at highly conserved residues in transmembrane domains. Neither mutation was present in the ExAC database. The mutation occurred de novo in 1 patient; it was not found in the unaffected mother of the other patient, but DNA from the father was not available. In vitro functional expression studies in transfected cells showed that both mutations caused a complete loss of channel activity. Wagnon et al. (2017) suggested that loss of neuronal activity due to the mutation may alter the dynamics of synaptic plasticity during maturation and lead to aberrant cerebral circuitry and impaired intellectual development.


REFERENCES

  1. Trudeau, M. M., Dalton, J. C., Day, J. W., Ranum, L. P. W., Meisler, M. H. Heterozygosity for a protein truncation mutation of sodium channel SCN8A in a patient with cerebellar atrophy, ataxia, and mental retardation. (Letter) J. Med. Genet. 43: 527-530, 2006. [PubMed: 16236810, images, related citations] [Full Text]

  2. Wagnon, J. L., Barker, B. S., Ottolini, M., Park, Y., Volkheimer, A., Valdez, P., Swinkels, M. E. M., Patel, M. K., Meisler, M. H. Loss-of-function variants of SCN8A in intellectual disability without seizures. Neurol. Genet. 3: e170, 2017. Note: Electronic Article. [PubMed: 28702509, images, related citations] [Full Text]


Contributors:
Cassandra L. Kniffin - updated : 03/25/2019
Creation Date:
Cassandra L. Kniffin : 10/25/2011
Edit History:
carol : 08/23/2022
carol : 08/22/2022
carol : 04/02/2019
carol : 03/29/2019
ckniffin : 03/25/2019
carol : 09/22/2014
carol : 10/31/2011
ckniffin : 10/31/2011

# 614306

COGNITIVE IMPAIRMENT WITH OR WITHOUT CEREBELLAR ATAXIA; CIAT


Phenotype-Gene Relationships

Location Phenotype Phenotype
MIM number 		Inheritance Phenotype
mapping key 		Gene/Locus Gene/Locus
MIM number
12q13.13 Cognitive impairment with or without cerebellar ataxia 614306 Autosomal dominant 3 SCN8A 600702

TEXT

A number sign (#) is used with this entry because of evidence that cognitive impairment with or without cerebellar ataxia (CIAT) is caused by heterozygous mutation in the SCN8A gene (600702) on chromosome 12q13.

Clinical Features

Trudeau et al. (2006) reported a family of Swedish and Norwegian origin with highly variable neurologic deficits. The proband was a 9-year-old boy with markedly delayed psychomotor development, attention deficit disorder, and cerebellar ataxia. Features included ataxic wide-based gait, dysmetria in the upper limbs, and dysarthria, with normal strength, tone, and reflexes. He also had esophoria, amblyopia, and gaze-evoked nystagmus. Brain MRI showed moderate pancerebellar atrophy, accentuated in the vermal and parasagittal regions, as well as optic nerve hypoplasia. There were no cerebral abnormalities. His mother and maternal aunt had a history of emotional instability and mild cognitive impairment, and a first cousin had attention deficit-hyperactivity disorder (ADHD; 143465). A brother of the proband was noted to have impaired cognition and another cousin was noted to have ADHD, but they were not studied at the molecular level. In addition, none of the family members besides the proband was available for formal clinical evaluation or brain imaging studies. The proband was ascertained during a study of 151 patients with ataxia who were screened specifically for mutations in the SCN8A gene.

Wagnon et al. (2017) reported 2 unrelated children, a 7-year-old girl and a 10-year-old boy, with global developmental delay and impaired intellectual development (IQ of 73 and 56, respectively). The girl had delayed language, hypotonia that resolved with time, and ADHD; she was able to attend a special school. The boy had severe speech delay, temper tantrums, and a history of unsteady gait. Neither patient had seizures, and brain imaging performed in 1 patient was normal.


Inheritance

The transmission pattern of CIAT in the family reported by Trudeau et al. (2006) was consistent with autosomal dominant inheritance with variable expressivity.


Molecular Genetics

Trudeau et al. (2006) screened the 26 coding exons of SCN8A in 151 patients with inherited or sporadic ataxia and no mutations in known ataxia-related genes. The SCN8A gene was chosen for study because it is widely expressed in neurons of the central and peripheral nervous systems, and because mutations in the mouse ortholog result in ataxia and other movement disorders. A heterozygous 2-bp deletion in exon 24 (600702.0001) was identified in 1 patient, a 9-year-old boy with mental retardation, pancerebellar atrophy, and ataxia. Three additional family members who were heterozygous for the mutation exhibited milder cognitive behavioral deficits including ADHD. However, Trudeau et al. (2006) noted that it was unclear whether the relatives of the proband had a milder version of the neurologic abnormalities seen in the proband due to haploinsufficiency for SCN8A, or if the proband's symptoms were caused by an unrelated developmental disorder.

In 2 unrelated children with CIAT, Wagnon et al. (2017) identified de novo heterozygous missense mutations in the SCN8A gene (G964R, 600702.0013 and E1218K, 600702.0014). The mutations, which were found by exome sequencing, occurred at highly conserved residues in transmembrane domains. Neither mutation was present in the ExAC database. The mutation occurred de novo in 1 patient; it was not found in the unaffected mother of the other patient, but DNA from the father was not available. In vitro functional expression studies in transfected cells showed that both mutations caused a complete loss of channel activity. Wagnon et al. (2017) suggested that loss of neuronal activity due to the mutation may alter the dynamics of synaptic plasticity during maturation and lead to aberrant cerebral circuitry and impaired intellectual development.


REFERENCES

  1. Trudeau, M. M., Dalton, J. C., Day, J. W., Ranum, L. P. W., Meisler, M. H. Heterozygosity for a protein truncation mutation of sodium channel SCN8A in a patient with cerebellar atrophy, ataxia, and mental retardation. (Letter) J. Med. Genet. 43: 527-530, 2006. [PubMed: 16236810] [Full Text: https://doi.org/10.1136/jmg.2005.035667]

  2. Wagnon, J. L., Barker, B. S., Ottolini, M., Park, Y., Volkheimer, A., Valdez, P., Swinkels, M. E. M., Patel, M. K., Meisler, M. H. Loss-of-function variants of SCN8A in intellectual disability without seizures. Neurol. Genet. 3: e170, 2017. Note: Electronic Article. [PubMed: 28702509] [Full Text: https://doi.org/10.1212/NXG.0000000000000170]


Contributors:
Cassandra L. Kniffin - updated : 03/25/2019

Creation Date:
Cassandra L. Kniffin : 10/25/2011

Edit History:
carol : 08/23/2022
carol : 08/22/2022
carol : 04/02/2019
carol : 03/29/2019
ckniffin : 03/25/2019
carol : 09/22/2014
carol : 10/31/2011
ckniffin : 10/31/2011



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2025 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2025 Johns Hopkins University.
Printed: March 5, 2025