Novel mutations in <i>ATP1A3</i> associated with catastrophic early life epilepsy, episodic prolonged apnea, and postnatal microcephaly

Paciorkowski, Alex R.; McDaniel, Sharon S.; Jansen, Laura A.; Tully, Hannah M.; Tuttle, Emily; Ghoneim, Dalia; Tupal, Srinivasan; Gunter, Sonya A.; Vasta, Valeria; Zhang, Qing; Tran, Thao; Liu, Yi B.; Ozelius, Laurie J.; Brashear, Allison; Sweadner, Kathleen J.; Dobyns, William B.; Hahn, Si Houn

doi:10.1111/epi.12914

Cited by 105 publications

(102 citation statements)

References 35 publications

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“…ATP1A2 , together with ATP1A3 , belongs to a family of genes coding for catalytic subunits of Na/K‐ATPase. The relevance of these genes in genetic epilepsies is also supported by the report of a child with catastrophic early life epilepsy and shortened survival carrying a mutation in ATP1A3 [Paciorkowski et al., ].…”

Section: Discussionmentioning

confidence: 99%

Diagnostic Targeted Resequencing in 349 Patients with Drug-Resistant Pediatric Epilepsies Identifies Causative Mutations in 30 Different Genes

et al. 2016

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Targeted resequencing gene panels are used in the diagnostic setting to identify gene defects in epilepsy. We performed targeted resequencing using a 30-genes panel and a 95-genes panel in 349 patients with drugresistant epilepsies beginning in the first years of life. We identified 71 pathogenic variants, 42 of which novel, in 30 genes, corresponding to 20.3% of the probands. In 66% of mutation positive patients, epilepsy onset occurred before the age of 6 months. The 95-genes panel allowed a genetic diagnosis in 22 (6.3%) patients that would have otherwise been missed using the 30-gene panel. About 50% of mutations were identified in genes coding for sodium and potassium channel components. SCN2A was the most frequently mutated gene followed by SCN1A, KCNQ2, STXBP1, SCN8A, CDKL5, and MECP2. Twenty-nine mutations were identified in 23 additional genes, most of them recently associated with epilepsy. Our data show that panels targeting about 100 genes represent the best cost-effective diagnostic option in pediatric drug-resistant epilepsies. They enable molecular diagnosis of atypical phenotypes, allowing to broaden phenotype-genotype correlations. Molecular diagnosis might influence patients' management and translate into better and specific treatment recommendations in some conditions. Hum Mutat 38:216-225, 2017. C 2016 Wiley Periodicals, Inc.

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Section: Discussionmentioning

confidence: 99%

Diagnostic Targeted Resequencing in 349 Patients with Drug-Resistant Pediatric Epilepsies Identifies Causative Mutations in 30 Different Genes

et al. 2016

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“…After assessing the conventional brain MRI findings and genotypes of our patients, we have shown for the first time that similar abnormal findings exist in patients with severe deterioration. Progressive brain atrophy and cerebellar atrophy/ataxia have been reported in a spectrum of ATP1A3 ‐related disorders other than AHC …”

Section: Discussionmentioning

confidence: 99%

Progressive Brain Atrophy in Alternating Hemiplegia of Childhood

Sasaki

Ishii

Saito

et al. 2017

Movement Disord Clin Pract

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Background Alternating hemiplegia of childhood (AHC) is a rare neurodevelopmental disorder that includes involuntary movements, paroxysmal symptoms, and various severities of nonparoxysmal symptoms. Objective To investigate the occurrence of structural brain abnormalities in patients with AHC during clinical courses. Methods Conventional brain magnetic resonance imaging findings and clinical courses were retrospectively investigated in 14 patients with AHC confirmed by ATP1A3 mutations. Results Progressive frontal dominant cerebral, diffuse cerebellar cortical, and severe hippocampal atrophy were observed in seven patients with irreversible severe motor and intellectual deterioration. All of these seven patients exhibited status epilepticus and required transient respiratory care. Isolated diffuse cerebellar cortical atrophy was observed in two adult patients with mild motor regression. Five patients without apparent deterioration displayed almost normal brain findings. Conclusions The areas of atrophy were consistent with the areas of increased expression of the Na+/K+‐ATPase α3 subunit encoded by ATP1A3. Some of paroxysmal and nonparoxysmal neurological symptoms are considered as related to the areas of brain atrophy.

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“…Recently, sudden unexpected death in epilepsy, cardiac structural abnormalities, episodic prolonged apnea, and postnatal microcephaly have been reported in patients with ATP1A3 -related disorders (Dard et al, 2015; Paciorkowski et al, 2015; Rosewich et al, 2012; Rosewich, Weise, Ohlenbusch, Gärtner, and Brockmann, 2014). Atypical and overlapping features of AHC, RDP, and CAPOS syndrome with intermediate phenotypes have been reported in patients with novel variants p.Arg756His and p.Arg756Cys in ATP1A3 (Jaffer et al, 2017; Kanemasa et al, 2016).…”

Section: Discussionmentioning

confidence: 99%

“…Pathogenic variants in ATP1A3 have been implicated in a phenotypic spectrum of autosomal dominant disorders including Alternating Hemiplegia of Childhood (AHC, OMIM 614820), Rapid-onset Dystonia-Parkinsonism (RDP, OMIM 128235) and Cerebellar ataxia, Areflexia, Pes cavus, Optic atrophy, and Sensorineural hearing loss syndrome (CAPOS syndrome, OMIM 601338) (de Carvalho Aguiar et al, 2004; Demos et al, 2014; Heinzen et al, 2014; Paciorkowski et al, 2015; Rosewich et al, 2012; Sweney, Newcomb, & Swoboda, 2015). Marked genetic heterogeneity exists for AHC and RDP, including possible genotype-phenotype correlation (Yang et al, 2014) and mosaicism (Hully et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Novel pregnancy‐triggered episodes of CAPOS syndrome

Chang

Adam

Jayadev

et al. 2017

American J of Med Genetics Pt A

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Cerebellar ataxia, areflexia, pes cavus, optic atrophy, and sensorineural hearing loss (CAPOS) syndrome (OMIM# 601338) is a rare autosomal dominant disorder characterized by episodic, fever-induced ataxic encephalopathy in childhood with residual symptoms. All identified patients have the same heterozygous missense variant c.2452G>A (p.Glu818Lys) in the ATP1A3 gene, encoding Na /K ATPase α3. We describe a large CAPOS pedigree with three generations of affected members, the first ascertained in the United States. Deafness, optic atrophy, and pes cavus were present in all three members of the family evaluated. In addition, one of the affected individuals experienced markedly worsening features during her three pregnancies and in the immediate postpartum period, a potential element of the natural history of CAPOS previously unreported. We conclude that the triggering factors and clinical spectrum of pathogenic ATP1A3 variants may be broader than previously described. Targeted sequencing of ATP1A3 should be considered in any patient presenting with cerebellar ataxia triggered by febrile illness, or pregnancy and delivery, especially in the presence of sensorineural hearing loss, optic atrophy, pes cavus, or early childhood history of acute encephalopathic ataxia. Prophylactic administration of acetazolamide or flunarizine may prevent acute episodes of ataxia or mitigate neurologic symptoms, although their efficacies have not been well studied.

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Novel mutations in ATP1A3 associated with catastrophic early life epilepsy, episodic prolonged apnea, and postnatal microcephaly

Cited by 105 publications

References 35 publications

Diagnostic Targeted Resequencing in 349 Patients with Drug-Resistant Pediatric Epilepsies Identifies Causative Mutations in 30 Different Genes

Diagnostic Targeted Resequencing in 349 Patients with Drug-Resistant Pediatric Epilepsies Identifies Causative Mutations in 30 Different Genes

Progressive Brain Atrophy in Alternating Hemiplegia of Childhood

Novel pregnancy‐triggered episodes of CAPOS syndrome

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