FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2970748251> ?p ?o ?g. }

• W2970748251 endingPage "82" @default.
• W2970748251 startingPage "77" @default.
• W2970748251 abstract "Background Mutations in the elongation factor 1 alpha 2 (EEF1A2) gene have been recently shown to cause epileptic encephalopathy (MIM # 616409 EIEE33) associated with neurodevelopmental disorders such as intellectual disability, autistic spectrum disorder, hypotonia and dysmorphic facial features. EEF1A2 protein is involved in protein synthesis, suppression of apoptosis, regulation of actin function and cytoskeletal structure. To date, only sixteen patients with EEF1A2 mutations have been reported. Case report We described a new case, a boy with severe intellectual disability with absent speech, autistic spectrum disorder, mild dysmorphic facial features, failure to thrive and epilepsy associated to a de novo heterozygous missense mutation in EEF1A2 (c.364G>A; p.Glu122Lys) identified by next generation sequencing; it was already reported in other studies. Most clinical features are shared by all individuals with EEF1A2 mutation, but unlike others reports our patient showed a mild epileptic phenotype: epilepsy developed in late infancy and was well-controlled with antiepileptic drugs. Moreover, at the onset of epilepsy, interictal wake/sleep electroencephalograms showed typical pattern that disappeared with age. Conclusion This report focused that EEF1A2 mutations should be considered not only in patients with epileptic encephalopathy, but also in those with less severe epilepsy. A typical EEG pattern may be a biomarker for EEF1A2 mutation, but further investigations and longitudinal clinical observations are required." @default.
• W2970748251 created "2019-09-05" @default.
• W2970748251 creator A5002075087 @default.
• W2970748251 creator A5037817203 @default.
• W2970748251 creator A5040918424 @default.
• W2970748251 date "2020-01-01" @default.
• W2970748251 modified "2023-10-02" @default.
• W2970748251 title "Mild epileptic phenotype associates with de novo eef1a2 mutation: Case report and review" @default.
• W2970748251 cites W1503441328 @default.
• W2970748251 cites W1590977598 @default.
• W2970748251 cites W1974558715 @default.
• W2970748251 cites W2023228765 @default.
• W2970748251 cites W2052394197 @default.
• W2970748251 cites W2074481290 @default.
• W2970748251 cites W2115558586 @default.
• W2970748251 cites W2143891161 @default.
• W2970748251 cites W2205158010 @default.
• W2970748251 cites W2312616498 @default.
• W2970748251 cites W2677301288 @default.
• W2970748251 doi "https://doi.org/10.1016/j.braindev.2019.08.001" @default.
• W2970748251 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31477274" @default.
• W2970748251 hasPublicationYear "2020" @default.
• W2970748251 type Work @default.
• W2970748251 sameAs 2970748251 @default.
• W2970748251 citedByCount "10" @default.
• W2970748251 countsByYear W29707482512020 @default.
• W2970748251 countsByYear W29707482512021 @default.
• W2970748251 countsByYear W29707482512022 @default.
• W2970748251 countsByYear W29707482512023 @default.
• W2970748251 crossrefType "journal-article" @default.
• W2970748251 hasAuthorship W2970748251A5002075087 @default.
• W2970748251 hasAuthorship W2970748251A5037817203 @default.
• W2970748251 hasAuthorship W2970748251A5040918424 @default.
• W2970748251 hasConcept C104317684 @default.
• W2970748251 hasConcept C118552586 @default.
• W2970748251 hasConcept C127716648 @default.
• W2970748251 hasConcept C16568411 @default.
• W2970748251 hasConcept C187212893 @default.
• W2970748251 hasConcept C2778186239 @default.
• W2970748251 hasConcept C2778201146 @default.
• W2970748251 hasConcept C2779546488 @default.
• W2970748251 hasConcept C2779674439 @default.
• W2970748251 hasConcept C2910479173 @default.
• W2970748251 hasConcept C501734568 @default.
• W2970748251 hasConcept C54355233 @default.
• W2970748251 hasConcept C551499885 @default.
• W2970748251 hasConcept C71924100 @default.
• W2970748251 hasConcept C75563809 @default.
• W2970748251 hasConcept C86803240 @default.
• W2970748251 hasConceptScore W2970748251C104317684 @default.
• W2970748251 hasConceptScore W2970748251C118552586 @default.
• W2970748251 hasConceptScore W2970748251C127716648 @default.
• W2970748251 hasConceptScore W2970748251C16568411 @default.
• W2970748251 hasConceptScore W2970748251C187212893 @default.
• W2970748251 hasConceptScore W2970748251C2778186239 @default.
• W2970748251 hasConceptScore W2970748251C2778201146 @default.
• W2970748251 hasConceptScore W2970748251C2779546488 @default.
• W2970748251 hasConceptScore W2970748251C2779674439 @default.
• W2970748251 hasConceptScore W2970748251C2910479173 @default.
• W2970748251 hasConceptScore W2970748251C501734568 @default.
• W2970748251 hasConceptScore W2970748251C54355233 @default.
• W2970748251 hasConceptScore W2970748251C551499885 @default.
• W2970748251 hasConceptScore W2970748251C71924100 @default.
• W2970748251 hasConceptScore W2970748251C75563809 @default.
• W2970748251 hasConceptScore W2970748251C86803240 @default.
• W2970748251 hasIssue "1" @default.
• W2970748251 hasLocation W29707482511 @default.
• W2970748251 hasLocation W29707482512 @default.
• W2970748251 hasOpenAccess W2970748251 @default.
• W2970748251 hasPrimaryLocation W29707482511 @default.
• W2970748251 hasRelatedWork W1892224228 @default.
• W2970748251 hasRelatedWork W2472188752 @default.
• W2970748251 hasRelatedWork W2970748251 @default.
• W2970748251 hasRelatedWork W3040790123 @default.
• W2970748251 hasRelatedWork W3124002180 @default.
• W2970748251 hasRelatedWork W3185393103 @default.
• W2970748251 hasRelatedWork W4207081885 @default.
• W2970748251 hasRelatedWork W4377093572 @default.
• W2970748251 hasRelatedWork W4385294592 @default.
• W2970748251 hasRelatedWork W4385973395 @default.
• W2970748251 hasVolume "42" @default.
• W2970748251 isParatext "false" @default.
• W2970748251 isRetracted "false" @default.
• W2970748251 magId "2970748251" @default.
• W2970748251 workType "article" @default.