FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4382363085> ?p ?o ?g. }

• W4382363085 abstract "The vacuolar H+-ATPase is a multisubunit enzyme which plays an essential role in the acidification and functions of lysosomes, endosomes, and synaptic vesicles. Many genes encoding subunits of V-ATPases, namely ATP6V0C, ATP6V1A, ATP6V0A1 and ATP6V1B2, have been associated with neurodevelopmental disorders and epilepsy. The autosomal dominant ATP6V1B2 p.Arg506* variant can cause both deafness, congenital, with onychodystrophy, autosomal dominant (DDOD) and deafness, onychodystrophy, osteodystrophy, mental retardation, and seizures syndromes (DOORS). Some but not all individuals with this truncating variant have intellectual disability and/or epilepsy, suggesting incomplete penetrance and/or variable expressivity. To further explore the impact of the p.Arg506* variant in neurodevelopment and epilepsy, we generated Atp6v1b2emR506* mutant mice and performed standardized phenotyping using the International Mouse Phenotyping Consortium (IMPC) pipeline. In addition, we assessed the EEG profile and seizure susceptibility of Atp6v1b2emR506* mice. Behavioral tests revealed that the mice present locomotor hyperactivity and show less anxiety-associated behaviors. Moreover, EEG analyses indicate that Atp6v1b2emR506* mutant mice have interictal epileptic activity and that both heterozygous (like patients) and homozygous mice have reduced seizure thresholds to pentylenetetrazol. Our results confirm that variants in ATP6V1B2 can cause seizures and that the Atp6v1b2emR506* heterozygous mouse model is a valuable tool to further explore the pathophysiology and potential treatments for vacuolar ATPases-associated epilepsy and disorders." @default.
• W4382363085 created "2023-06-29" @default.
• W4382363085 creator A5002939690 @default.
• W4382363085 creator A5018268251 @default.
• W4382363085 creator A5021333615 @default.
• W4382363085 creator A5025974364 @default.
• W4382363085 creator A5057582530 @default.
• W4382363085 creator A5058759078 @default.
• W4382363085 creator A5065502457 @default.
• W4382363085 creator A5076669629 @default.
• W4382363085 creator A5080134223 @default.
• W4382363085 creator A5092349018 @default.
• W4382363085 date "2023-06-28" @default.
• W4382363085 modified "2023-09-25" @default.
• W4382363085 title "The <em>ATP6V1B2 </em>DDOD/DOORS-Associated p.Arg506* Variant Causes Hyperactivity and Seizures in Mice" @default.
• W4382363085 doi "https://doi.org/10.20944/preprints202306.1970.v1" @default.
• W4382363085 hasPublicationYear "2023" @default.
• W4382363085 type Work @default.
• W4382363085 citedByCount "0" @default.
• W4382363085 crossrefType "posted-content" @default.
• W4382363085 hasAuthorship W4382363085A5002939690 @default.
• W4382363085 hasAuthorship W4382363085A5018268251 @default.
• W4382363085 hasAuthorship W4382363085A5021333615 @default.
• W4382363085 hasAuthorship W4382363085A5025974364 @default.
• W4382363085 hasAuthorship W4382363085A5057582530 @default.
• W4382363085 hasAuthorship W4382363085A5058759078 @default.
• W4382363085 hasAuthorship W4382363085A5065502457 @default.
• W4382363085 hasAuthorship W4382363085A5076669629 @default.
• W4382363085 hasAuthorship W4382363085A5080134223 @default.
• W4382363085 hasAuthorship W4382363085A5092349018 @default.
• W4382363085 hasBestOaLocation W43823630851 @default.
• W4382363085 hasConcept C104317684 @default.
• W4382363085 hasConcept C127716648 @default.
• W4382363085 hasConcept C169760540 @default.
• W4382363085 hasConcept C17755696 @default.
• W4382363085 hasConcept C200544954 @default.
• W4382363085 hasConcept C2775858608 @default.
• W4382363085 hasConcept C2776819090 @default.
• W4382363085 hasConcept C2778186239 @default.
• W4382363085 hasConcept C54355233 @default.
• W4382363085 hasConcept C551499885 @default.
• W4382363085 hasConcept C71924100 @default.
• W4382363085 hasConcept C86803240 @default.
• W4382363085 hasConceptScore W4382363085C104317684 @default.
• W4382363085 hasConceptScore W4382363085C127716648 @default.
• W4382363085 hasConceptScore W4382363085C169760540 @default.
• W4382363085 hasConceptScore W4382363085C17755696 @default.
• W4382363085 hasConceptScore W4382363085C200544954 @default.
• W4382363085 hasConceptScore W4382363085C2775858608 @default.
• W4382363085 hasConceptScore W4382363085C2776819090 @default.
• W4382363085 hasConceptScore W4382363085C2778186239 @default.
• W4382363085 hasConceptScore W4382363085C54355233 @default.
• W4382363085 hasConceptScore W4382363085C551499885 @default.
• W4382363085 hasConceptScore W4382363085C71924100 @default.
• W4382363085 hasConceptScore W4382363085C86803240 @default.
• W4382363085 hasLocation W43823630851 @default.
• W4382363085 hasOpenAccess W4382363085 @default.
• W4382363085 hasPrimaryLocation W43823630851 @default.
• W4382363085 hasRelatedWork W1973589190 @default.
• W4382363085 hasRelatedWork W1988764473 @default.
• W4382363085 hasRelatedWork W1990627463 @default.
• W4382363085 hasRelatedWork W2111461216 @default.
• W4382363085 hasRelatedWork W2914997480 @default.
• W4382363085 hasRelatedWork W2981333376 @default.
• W4382363085 hasRelatedWork W3035799378 @default.
• W4382363085 hasRelatedWork W3104061430 @default.
• W4382363085 hasRelatedWork W3184181491 @default.
• W4382363085 hasRelatedWork W4225276718 @default.
• W4382363085 isParatext "false" @default.
• W4382363085 isRetracted "false" @default.
• W4382363085 workType "article" @default.