ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities

OBJECTIVE: ADGRV1 gene encodes adhesion G protein-coupled receptor-V1 that is involved in synaptic function. ADGRV1 mutations are associated with audio-visual disorders. Although previous experimental studies suggested that ADGRV1 variants were associated with epilepsy, clinical evidence is limited...

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Autores principales: Zhou, Peng, Meng, Heng, Liang, Xiaoyu, Lei, Xiaoyun, Zhang, Jingwen, Bian, Wenjun, He, Na, Lin, Zhijian, Song, Xingwang, Zhu, Weiwen, Hu, Bin, Li, Bingmei, Yan, Limin, Tang, Bin, Su, Tao, Liu, Hankui, Mao, Yong, Zhai, Qiongxiang, Yi, Yonghong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Molecular Neuroscience
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9262510/
https://www.ncbi.nlm.nih.gov/pubmed/35813073
http://dx.doi.org/10.3389/fnmol.2022.864074
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author Zhou, Peng
Meng, Heng
Liang, Xiaoyu
Lei, Xiaoyun
Zhang, Jingwen
Bian, Wenjun
He, Na
Lin, Zhijian
Song, Xingwang
Zhu, Weiwen
Hu, Bin
Li, Bingmei
Yan, Limin
Tang, Bin
Su, Tao
Liu, Hankui
Mao, Yong
Zhai, Qiongxiang
Yi, Yonghong
author_facet Zhou, Peng
Meng, Heng
Liang, Xiaoyu
Lei, Xiaoyun
Zhang, Jingwen
Bian, Wenjun
He, Na
Lin, Zhijian
Song, Xingwang
Zhu, Weiwen
Hu, Bin
Li, Bingmei
Yan, Limin
Tang, Bin
Su, Tao
Liu, Hankui
Mao, Yong
Zhai, Qiongxiang
Yi, Yonghong
author_sort Zhou, Peng
collection PubMed
description OBJECTIVE: ADGRV1 gene encodes adhesion G protein-coupled receptor-V1 that is involved in synaptic function. ADGRV1 mutations are associated with audio-visual disorders. Although previous experimental studies suggested that ADGRV1 variants were associated with epilepsy, clinical evidence is limited and the phenotype spectrum is to be defined. METHODS: Trio-based targeting sequencing was performed in a cohort of 101 cases with febrile seizure (FS) and epilepsy with antecedent FS. Protein modeling was used to assess the damaging effects of variants. The genotype-phenotype correlations of the ADGRV1 variants in epilepsy and audio-visual disorders were analyzed. RESULTS: ADGRV1 variants were identified in nine unrelated cases (8.91%), including two heterozygous frameshift variants, six heterozygous missense variants, and a pair of compound heterozygous variants. These variants presented a statistically higher frequency in this cohort than that in control populations. Most missense variants were located at CalX-β motifs and changed the hydrogen bonds. These variants were inherited from the asymptomatic parents, indicating an incomplete penetrance. We also identified SCN1A variants in 25 unrelated cases (24.75%) and SCN9A variants in 3 unrelated cases (2.97%) in this cohort. Contrary to SCN1A variant-associated epilepsy that revealed seizure was aggravated by sodium channel blockers, ADGRV1 variants were associated with mild epilepsy with favorable responses to antiepileptic drugs. The patients denied problems with audio-visual-vestibular abilities in daily life. However, audio-visual tests revealed auditory and visual impairment in the patient with compound heterozygous variants, auditory or vestibular impairment in the patients with heterozygous frameshift, or hydrogen-bond changed missense variants but no abnormalities in the patients with missense variants without hydrogen-bond changes. Previously reported ADGRV1 variants that were associated with audio-visual disorders were mostly biallelic/destructive variants, which were significantly more frequent in the severe phenotype of audio-visual disorders (Usher syndrome 2) than in other mild phenotypes. In contrast, the variants identified in epilepsy were monoallelic, missense mainly located at CalX-β, or affected isoforms VLGR1b/1c. SIGNIFICANCE: ADGRV1 is potentially associated with FS-related epilepsy as a susceptibility gene. The genotype, submolecular implication, isoforms, and damaging severity of the variants explained the phenotypical variations. ADGRV1 variant-associated FS/epilepsy presented favorable responses to antiepileptic drugs, implying a clinical significance.
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spelling pubmed-92625102022-07-08 ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities Zhou, Peng Meng, Heng Liang, Xiaoyu Lei, Xiaoyun Zhang, Jingwen Bian, Wenjun He, Na Lin, Zhijian Song, Xingwang Zhu, Weiwen Hu, Bin Li, Bingmei Yan, Limin Tang, Bin Su, Tao Liu, Hankui Mao, Yong Zhai, Qiongxiang Yi, Yonghong Front Mol Neurosci Molecular Neuroscience OBJECTIVE: ADGRV1 gene encodes adhesion G protein-coupled receptor-V1 that is involved in synaptic function. ADGRV1 mutations are associated with audio-visual disorders. Although previous experimental studies suggested that ADGRV1 variants were associated with epilepsy, clinical evidence is limited and the phenotype spectrum is to be defined. METHODS: Trio-based targeting sequencing was performed in a cohort of 101 cases with febrile seizure (FS) and epilepsy with antecedent FS. Protein modeling was used to assess the damaging effects of variants. The genotype-phenotype correlations of the ADGRV1 variants in epilepsy and audio-visual disorders were analyzed. RESULTS: ADGRV1 variants were identified in nine unrelated cases (8.91%), including two heterozygous frameshift variants, six heterozygous missense variants, and a pair of compound heterozygous variants. These variants presented a statistically higher frequency in this cohort than that in control populations. Most missense variants were located at CalX-β motifs and changed the hydrogen bonds. These variants were inherited from the asymptomatic parents, indicating an incomplete penetrance. We also identified SCN1A variants in 25 unrelated cases (24.75%) and SCN9A variants in 3 unrelated cases (2.97%) in this cohort. Contrary to SCN1A variant-associated epilepsy that revealed seizure was aggravated by sodium channel blockers, ADGRV1 variants were associated with mild epilepsy with favorable responses to antiepileptic drugs. The patients denied problems with audio-visual-vestibular abilities in daily life. However, audio-visual tests revealed auditory and visual impairment in the patient with compound heterozygous variants, auditory or vestibular impairment in the patients with heterozygous frameshift, or hydrogen-bond changed missense variants but no abnormalities in the patients with missense variants without hydrogen-bond changes. Previously reported ADGRV1 variants that were associated with audio-visual disorders were mostly biallelic/destructive variants, which were significantly more frequent in the severe phenotype of audio-visual disorders (Usher syndrome 2) than in other mild phenotypes. In contrast, the variants identified in epilepsy were monoallelic, missense mainly located at CalX-β, or affected isoforms VLGR1b/1c. SIGNIFICANCE: ADGRV1 is potentially associated with FS-related epilepsy as a susceptibility gene. The genotype, submolecular implication, isoforms, and damaging severity of the variants explained the phenotypical variations. ADGRV1 variant-associated FS/epilepsy presented favorable responses to antiepileptic drugs, implying a clinical significance. Frontiers Media S.A. 2022-06-23 /pmc/articles/PMC9262510/ /pubmed/35813073 http://dx.doi.org/10.3389/fnmol.2022.864074 Text en Copyright © 2022 Zhou, Meng, Liang, Lei, Zhang, Bian, He, Lin, Song, Zhu, Hu, Li, Yan, Tang, Su, Liu, Mao, Zhai and Yi. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Molecular Neuroscience
Zhou, Peng
Meng, Heng
Liang, Xiaoyu
Lei, Xiaoyun
Zhang, Jingwen
Bian, Wenjun
He, Na
Lin, Zhijian
Song, Xingwang
Zhu, Weiwen
Hu, Bin
Li, Bingmei
Yan, Limin
Tang, Bin
Su, Tao
Liu, Hankui
Mao, Yong
Zhai, Qiongxiang
Yi, Yonghong
ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities
title ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities
title_full ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities
title_fullStr ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities
title_full_unstemmed ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities
title_short ADGRV1 Variants in Febrile Seizures/Epilepsy With Antecedent Febrile Seizures and Their Associations With Audio-Visual Abnormalities
title_sort adgrv1 variants in febrile seizures/epilepsy with antecedent febrile seizures and their associations with audio-visual abnormalities
topic Molecular Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9262510/
https://www.ncbi.nlm.nih.gov/pubmed/35813073
http://dx.doi.org/10.3389/fnmol.2022.864074
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