Your search keyword '"Jao Shwann Liang"' showing total 3 results

1. KCNQ2 mutations in childhood nonlesional epilepsy: Variable phenotypes and a novel mutation in a case series

Author

Inn‐Chi Lee, Tung‐Ming Chang, Jao‐Shwann Liang, and Shuan‐Yow Li

Subjects

childhood epilepsy, epileptic encephalopathy, KCNQ2, phenotypes, Genetics, QH426-470

Abstract

Abstract Background Epilepsy caused by a KCNQ2 gene mutation usually manifests as neonatal seizures during the first week of life. The genotypes and phenotypes of KCNQ2 mutations are noteworthy. Methods The KCNQ2 sequencings done were selected from 131 nonconsanguineous pediatric epileptic patients (age range: 2 days to 18 years) with nonlesional epilepsy. Results Seven (5%) index patients had verified KCNQ2 mutations: c.387+1 G>T (splicing), c.1741 C>T (p.Arg581*), c.740 C>T p.(Ser247Leu), c.853 C>A p.(Pro285Thr), c.860 C>T p.(Thr287Ile), c.1294 C>T p.(Arg432Cys), and c.1627 G>A p.(Val543Met). We found, after their paternity had been confirmed, that three patients had de novo p.(Ser247Leu), p.(Pro285Thr), and p.(Thr287Ile) mutations and neonatal‐onset epileptic encephalopathy; however, their frequent seizures remitted after they turned 6 months old. Those with the c.387+1G>T (splicing), (p.Arg581*), and p.(Val543Met) mutations presented with benign familial neonatal convulsions. In addition to their relatives, 14 patients had documented KCNQ2 mutations, and 12 (86%) had neonatal seizures. The seizures of all five patients treated with oxcarbazepine remitted. Conclusion KCNQ2‐related epilepsy led to varied outcomes (from benign to severe) in our patients. KCNQ2 mutations accounted for 13% of patients with seizure onset before 2 months old in our study. KCNQ2 mutations can cause different phenotypes in children. p.(Pro 285Thr) is a novel mutation, and the p.(Pro 285Thr), p.(Ser247Leu), and p.(Thr287Ile) variants can cause neonatal‐onset epileptic encephalopathy.

Published

2019

2. CDKL5 alterations lead to early epileptic encephalopathy in both genders

Author

Kaoru Imai, Keiko Shimojima, Makiko Osawa, Seiji Mizuno, Katsumi Imai, Jun Natsume, M. Shichiji, Akihisa Okumura, Tohru Okanishi, Hirokazu Oguni, Kyoko Hirasawa, Toshiyuki Yamamoto, Jao-Shwann Liang, Hiroko Ikeda, Yukitoshi Takahashi, Rumiko Takayama, Midori Sugawara, and Tomoshiro Ito

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, Seizure types, CDKL5, Physiology, Magnetic resonance imaging, Rett syndrome, Electroencephalography, Biology, medicine.disease, MECP2, Neurology, Frontal lobe, medicine, Clinical significance, Neurology (clinical)

Abstract

Summary Purpose: Genetic mutations of the cyclin-dependent kinase-like 5 gene (CDKL5) have been reported in patients with epileptic encephalopathy, which is characterized by intractable seizures and severe-to-profound developmental delay. We investigated the clinical relevance of CDKL5 alterations in both genders. Methods: A total of 125 patients with epileptic encephalopathy were examined for genomic copy number aberrations, and 119 patients with no such aberrations were further examined for CDKL5 mutations. Five patients with Rett syndrome, who did not show methyl CpG-binding protein 2 gene (MECP2) mutations, were also examined for CDKL5 mutations. Key Findings: One male and three female patients showed submicroscopic deletions including CDKL5, and two male and six female patients showed CDKL5 nucleotide alterations. Development of early onset seizure was a characteristic clinical feature for the patients with CDKL5 alterations in both genders despite polymorphous seizure types, including myoclonic seizures, tonic seizures, and spasms. Severe developmental delays and mild frontal lobe atrophies revealed by brain magnetic resonance imaging (MRI) were observed in almost all patients, and there was no gender difference in phenotypic features. Significance: We observed that 5% of the male patients and 14% of the female patients with epileptic encephalopathy had CDKL5 alterations. These findings indicate that alterations in CDKL5 are associated with early epileptic encephalopathy in both female and male patients.

Published

2011

3. STXBP1 mutations cause not only Ohtahara syndrome but also West syndrome-Result of Japanese cohort study

Author

Kaoru Imai, Hiroko Ikeda, Makiko Osawa, Toshiyuki Yamamoto, Jao-Shwann Liang, Motoko Otsuka, Hirokazu Oguni, Emiko Tachikawa, Kyoko Hirasawa, Katsumi Imai, and Keiko Shimojima

Subjects

Ohtahara syndrome, Pediatrics, medicine.medical_specialty, Pathology, business.industry, CDKL5, West Syndrome, medicine.disease, Central nervous system disease, Epilepsy, Neurology, medicine, Etiology, STXBP1, Neurology (clinical), business, Lennox–Gastaut syndrome

Abstract

Summary We performed STXBP1 mutation analyses in 86 patients with various types of epilepsies, including 10 patients with OS, 43 with West syndrome, 2 with Lennox-Gastaut syndrome, 12 with symptomatic generalized epilepsy, 14 with symptomatic partial epilepsy, and 5 with other undetermined types of epilepsy. In all patients, the etiology was unknown, but ARX and CDKL5 mutations were negative in all cases. All coding exons of STXBP1 were analyzed by direct-sequencing. Two de novo nucleotide alterations of STXBP1 were identified in two patients with Ohtahara and West syndrome, respectively. No de novo or deleterious mutations in STXBP1 were found in the remaining 84 patients with various types of symptomatic epilepsies. This is the first case report showing that STXBP1 mutations caused West syndrome from the onset of epilepsy. STXBP1 analysis should be considered as an etiology of symptomatic West syndrome without explainable cause.

Published

2010