Michiko Torio scite author profile

Three recessive mutations in the sodium leak channel, nonselective (NALCN) have been reported to cause intellectual disability and hypotonia. In addition, 14 de novo heterozygous mutations have been identified in 15 patients with arthrogryposis and neurodevelopmental impairment. Here, we report three patients with neurodevelopmental disease and hypotonia, harboring one recurrent (p.R1181Q) and two novel mutations (p.L312V and p.V1020F) occurring de novo in NALCN. Mutation p.L312 is located in the pore forming S6 region of domain I and p.V1020F in the S5 region of domain III. Mutation p.R1181Q is in a linker region. Mapping these three mutations to a model of NALCN showed p.Leu312 and p.Val1020 positioned in the hydrophobic core of the pore modules, indicating these two mutations may affect the gating function of NALCN. Although p.R1181Q is unlikely to affect the ion channel structure, previous studies have shown that an analogous mutation in Caenorhabditis elegans produced a phenotype with a coiling locomotion, suggesting that p.R1181Q could also affect NALCN function. Our three patients showed profound intellectual disability and growth delay, facial dysmorphologies and hypotonia. The present data support previous work suggesting heterozygous NALCN mutations lead to syndromic neurodevelopmental impairment.

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Fetal hydrocephalus and neonatal stroke as the first presentation of protein C deficiency

Ichiyama

Ohga

Ochiai

et al. 2016

Brain and Development

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Association of perinatal factors of epilepsy in very low birth weight infants, using a nationwide database in Japan

et al. 2019

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ObjectiveTo determine clinical features of very low birth weight infants (VLBWIs) who had developed epilepsy by age 3 years.Study designMulticenter cohort study using the Neonatal Research Network of Japan database. We analyzed clinical variables of 8431 VLBWIs who had recorded data of neurological sequelae at age 3 years. Logistic regression identified the association between variables and development of epilepsy.ResultOne hundred and forty-three (1.7%) infants developed epilepsy, 683 (8.1%) showed cerebral palsy (CP), and 1114 (13.2%) had psychomotor delay. Epilepsy was associated with history of sepsis [adjusted odds ratio (AOR) 3.23], severe intraventricular hemorrhage (IVH; AOR 5.13), and cystic periventricular leukomalacia (PVL; AOR 12.7). Severe IVH and cystic PVL were also frequently associated with CP and psychomotor delay.ConclusionSevere IVH and cystic PVL are strongly associated with development of epilepsy, as well as other neurological sequelae, and are potential critical therapeutic targets.

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De Novo Truncating Mutation of TRIM8 Causes Early‐Onset Epileptic Encephalopathy

Sakai

Fukai

Matsushita

et al. 2016

Annals of Human Genetics

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Michiko Torio

Phenotypic spectrum of GNAO1 variants: epileptic encephalopathy to involuntary movements with severe developmental delay

De novo missense mutations in NALCN cause developmental and intellectual impairment with hypotonia

Fetal hydrocephalus and neonatal stroke as the first presentation of protein C deficiency

Association of perinatal factors of epilepsy in very low birth weight infants, using a nationwide database in Japan

De Novo Truncating Mutation of TRIM8 Causes Early‐Onset Epileptic Encephalopathy

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