| Literature DB >> 33224018 |
Masashi Ogasawara1,2,3, Eiji Nakagawa1, Eri Takeshita1, Kohei Hamanaka4, Satoko Miyatake4, Naomichi Matsumoto4, Masayuki Sasaki1.
Abstract
The NEXMIF (KIAA2022) gene is located in the X chromosome, and hemizygous mutations in NEXMIF cause X-linked intellectual disability in male patients. Female patients with heterozygous mutations in NEXMIF also show similar, but milder, intellectual disability. Most female patients demonstrate intractable epilepsy compared with male patients, and the treatment strategy for epilepsy is still uncertain. Thus far, 24 female patients with NEXMIF mutations have been reported. Of these 24 patients, 20 also have epilepsy. Until now, epilepsy has been controlled in only 2 of these female patients. We report a female patient with a heterozygous de novo mutation, NM_001008537.2:c.1123del (p.Glu375Argfs*21), in NEXMIF. The patient showed mild intellectual disability, facial dysmorphism, obesity, generalized tonic-clonic seizures, and nonconvulsive status epilepticus. Sodium valproate was effective but caused secondary amenorrhea. We successfully treated her epilepsy with clonazepam without side effects, indicating that clonazepam might be a good choice to treat epilepsy in patients with NEXMIF mutations.Entities:
Keywords: Epilepsy; Facial dysmorphism; Intellectual disability; Obesity; X-linked inheritance
Year: 2020 PMID: 33224018 PMCID: PMC7675231 DOI: 10.1159/000510172
Source DB: PubMed Journal: Mol Syndromol ISSN: 1661-8769