Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings

Cheng Yen Kuo; Meng Han Tsai; Hsi Hsien Lin; Yu Chi Wang; Abhishek Kumar Singh; Chin Chen Chang; Jainn Jim Lin; Po Cheng Hung; Kuang Lin Lin

doi:10.1002/epi4.12685

Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings

Cheng Yen Kuo, Meng Han Tsai, Hsi Hsien Lin, Yu Chi Wang, Abhishek Kumar Singh, Chin Chen Chang, Jainn Jim Lin, Po Cheng Hung, Kuang Lin Lin^*

^*Corresponding author for this work

Research output: Contribution to journal › Journal Article › peer-review

8 Scopus citations

Abstract

Objective: Bilateral frontoparietal polymicrogyria (BFPP) is a rare genetic-related migration disorder. It has been attributed to loss-of-function of the ADGRG1 gene, which encodes an adhesion G protein-coupled receptor, ADGRG1/GPR56. We report the EEG findings of BFPP in three Asian patients, and confirmed that change in protein function was caused by the novel missense variant (p.Leu290Pro). Methods: We reviewed the medical records of three siblings with BFPP including one elder girl and two identical twin boys from birth to adulthood. The clinical symptoms, electroencephalography (EEG), brain MRI, whole-exome sequencing, treatment including medications, neuromodulation, and epilepsy surgery, and clinical outcomes were reviewed. The protein structure of a novel missense variant (p.Leu290Pro) was predicted by in silico studies, and molecular analysis was performed via typical flow cytometry and Western blotting. Results: The elder girl (Patient 1) was 22 years old and the twin boys (Patients 2 and 3) were 20 years old at the time of publication. All of them presented with typical clinical symptoms/signs and MRI findings of BFPP. Whole-exome sequencing followed by Sanger confirmation showed that all three patients had compound heterozygous variants in the ADGRG1 gene. The missense variant (p.Leu290Pro) was confirmed to be related to a reduction in cell surface GPR56 expression. High-amplitude rhythmic activity was noted in sleep EEG during infancy, which may have been due to excessive sleep spindle, and the rhythm disappeared when they were of pre-school age. Partial callosotomy provided short-term benefits in seizure control in Patients 1 and 2, and combined vagus nerve stimulation and partial callosotomy provided longer benefits in Patient 3. Significance: Sleep EEG findings of high-amplitude rhythmic activity in our BFPP cases were only noted during infancy and childhood. We also confirmed that the missense variant (p.Leu290Pro) led to loss of function due to a reduction in cell surface GPR56 expression.

Original language	English
Pages (from-to)	154-164
Number of pages	11
Journal	Epilepsia Open
Volume	8
Issue number	1
DOIs	https://doi.org/10.1002/epi4.12685
State	Published - 03 2023

Bibliographical note

Keywords

congenital CNS malformation
epilepsy
genetic
polymicrogyria
Humans
Child, Preschool
Polymicrogyria
Male
Infant
Mutation, Missense
Young Adult
Receptors, G-Protein-Coupled/genetics
Female
Adult
Child
Siblings

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Kuo, C. Y., Tsai, M. H., Lin, H. H., Wang, Y. C., Singh, A. K., Chang, C. C., Lin, J. J., Hung, P. C., & Lin, K. L. (2023). Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings. Epilepsia Open, 8(1), 154-164. https://doi.org/10.1002/epi4.12685

@article{e30d47126c3e4e348738f21b76804720,

title = "Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings",

abstract = "Objective: Bilateral frontoparietal polymicrogyria (BFPP) is a rare genetic-related migration disorder. It has been attributed to loss-of-function of the ADGRG1 gene, which encodes an adhesion G protein-coupled receptor, ADGRG1/GPR56. We report the EEG findings of BFPP in three Asian patients, and confirmed that change in protein function was caused by the novel missense variant (p.Leu290Pro). Methods: We reviewed the medical records of three siblings with BFPP including one elder girl and two identical twin boys from birth to adulthood. The clinical symptoms, electroencephalography (EEG), brain MRI, whole-exome sequencing, treatment including medications, neuromodulation, and epilepsy surgery, and clinical outcomes were reviewed. The protein structure of a novel missense variant (p.Leu290Pro) was predicted by in silico studies, and molecular analysis was performed via typical flow cytometry and Western blotting. Results: The elder girl (Patient 1) was 22 years old and the twin boys (Patients 2 and 3) were 20 years old at the time of publication. All of them presented with typical clinical symptoms/signs and MRI findings of BFPP. Whole-exome sequencing followed by Sanger confirmation showed that all three patients had compound heterozygous variants in the ADGRG1 gene. The missense variant (p.Leu290Pro) was confirmed to be related to a reduction in cell surface GPR56 expression. High-amplitude rhythmic activity was noted in sleep EEG during infancy, which may have been due to excessive sleep spindle, and the rhythm disappeared when they were of pre-school age. Partial callosotomy provided short-term benefits in seizure control in Patients 1 and 2, and combined vagus nerve stimulation and partial callosotomy provided longer benefits in Patient 3. Significance: Sleep EEG findings of high-amplitude rhythmic activity in our BFPP cases were only noted during infancy and childhood. We also confirmed that the missense variant (p.Leu290Pro) led to loss of function due to a reduction in cell surface GPR56 expression.",

keywords = "congenital CNS malformation, epilepsy, genetic, polymicrogyria, Humans, Child, Preschool, Polymicrogyria, Male, Infant, Mutation, Missense, Young Adult, Receptors, G-Protein-Coupled/genetics, Female, Adult, Child, Siblings",

author = "Kuo, \{Cheng Yen\} and Tsai, \{Meng Han\} and Lin, \{Hsi Hsien\} and Wang, \{Yu Chi\} and Singh, \{Abhishek Kumar\} and Chang, \{Chin Chen\} and Lin, \{Jainn Jim\} and Hung, \{Po Cheng\} and Lin, \{Kuang Lin\}",

note = "{\textcopyright} 2022 The Authors. Epilepsia Open published by Wiley Periodicals LLC on behalf of International League Against Epilepsy.",

year = "2023",

month = mar,

doi = "10.1002/epi4.12685",

language = "英语",

volume = "8",

pages = "154--164",

journal = "Epilepsia Open",

issn = "2470-9239",

publisher = "Wiley-Blackwell Publishing Ltd",

number = "1",

}

Kuo, CY, Tsai, MH , Lin, HH, Wang, YC, Singh, AK, Chang, CC, Lin, JJ, Hung, PC & Lin, KL 2023, 'Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings', Epilepsia Open, vol. 8, no. 1, pp. 154-164. https://doi.org/10.1002/epi4.12685

Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings. / Kuo, Cheng Yen; Tsai, Meng Han ; Lin, Hsi Hsien et al.
In: Epilepsia Open, Vol. 8, No. 1, 03.2023, p. 154-164.

Research output: Contribution to journal › Journal Article › peer-review

TY - JOUR

T1 - Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria

T2 - The electroclinical change from infancy to adulthood after Callosotomy in three siblings

AU - Kuo, Cheng Yen

AU - Tsai, Meng Han

AU - Lin, Hsi Hsien

AU - Wang, Yu Chi

AU - Singh, Abhishek Kumar

AU - Chang, Chin Chen

AU - Lin, Jainn Jim

AU - Hung, Po Cheng

AU - Lin, Kuang Lin

PY - 2023/3

Y1 - 2023/3

N2 - Objective: Bilateral frontoparietal polymicrogyria (BFPP) is a rare genetic-related migration disorder. It has been attributed to loss-of-function of the ADGRG1 gene, which encodes an adhesion G protein-coupled receptor, ADGRG1/GPR56. We report the EEG findings of BFPP in three Asian patients, and confirmed that change in protein function was caused by the novel missense variant (p.Leu290Pro). Methods: We reviewed the medical records of three siblings with BFPP including one elder girl and two identical twin boys from birth to adulthood. The clinical symptoms, electroencephalography (EEG), brain MRI, whole-exome sequencing, treatment including medications, neuromodulation, and epilepsy surgery, and clinical outcomes were reviewed. The protein structure of a novel missense variant (p.Leu290Pro) was predicted by in silico studies, and molecular analysis was performed via typical flow cytometry and Western blotting. Results: The elder girl (Patient 1) was 22 years old and the twin boys (Patients 2 and 3) were 20 years old at the time of publication. All of them presented with typical clinical symptoms/signs and MRI findings of BFPP. Whole-exome sequencing followed by Sanger confirmation showed that all three patients had compound heterozygous variants in the ADGRG1 gene. The missense variant (p.Leu290Pro) was confirmed to be related to a reduction in cell surface GPR56 expression. High-amplitude rhythmic activity was noted in sleep EEG during infancy, which may have been due to excessive sleep spindle, and the rhythm disappeared when they were of pre-school age. Partial callosotomy provided short-term benefits in seizure control in Patients 1 and 2, and combined vagus nerve stimulation and partial callosotomy provided longer benefits in Patient 3. Significance: Sleep EEG findings of high-amplitude rhythmic activity in our BFPP cases were only noted during infancy and childhood. We also confirmed that the missense variant (p.Leu290Pro) led to loss of function due to a reduction in cell surface GPR56 expression.

AB - Objective: Bilateral frontoparietal polymicrogyria (BFPP) is a rare genetic-related migration disorder. It has been attributed to loss-of-function of the ADGRG1 gene, which encodes an adhesion G protein-coupled receptor, ADGRG1/GPR56. We report the EEG findings of BFPP in three Asian patients, and confirmed that change in protein function was caused by the novel missense variant (p.Leu290Pro). Methods: We reviewed the medical records of three siblings with BFPP including one elder girl and two identical twin boys from birth to adulthood. The clinical symptoms, electroencephalography (EEG), brain MRI, whole-exome sequencing, treatment including medications, neuromodulation, and epilepsy surgery, and clinical outcomes were reviewed. The protein structure of a novel missense variant (p.Leu290Pro) was predicted by in silico studies, and molecular analysis was performed via typical flow cytometry and Western blotting. Results: The elder girl (Patient 1) was 22 years old and the twin boys (Patients 2 and 3) were 20 years old at the time of publication. All of them presented with typical clinical symptoms/signs and MRI findings of BFPP. Whole-exome sequencing followed by Sanger confirmation showed that all three patients had compound heterozygous variants in the ADGRG1 gene. The missense variant (p.Leu290Pro) was confirmed to be related to a reduction in cell surface GPR56 expression. High-amplitude rhythmic activity was noted in sleep EEG during infancy, which may have been due to excessive sleep spindle, and the rhythm disappeared when they were of pre-school age. Partial callosotomy provided short-term benefits in seizure control in Patients 1 and 2, and combined vagus nerve stimulation and partial callosotomy provided longer benefits in Patient 3. Significance: Sleep EEG findings of high-amplitude rhythmic activity in our BFPP cases were only noted during infancy and childhood. We also confirmed that the missense variant (p.Leu290Pro) led to loss of function due to a reduction in cell surface GPR56 expression.

KW - congenital CNS malformation

KW - epilepsy

KW - genetic

KW - polymicrogyria

KW - Humans

KW - Child, Preschool

KW - Polymicrogyria

KW - Male

KW - Infant

KW - Mutation, Missense

KW - Young Adult

KW - Receptors, G-Protein-Coupled/genetics

KW - Female

KW - Adult

KW - Child

KW - Siblings

UR - https://www.scopus.com/pages/publications/85146159967

U2 - 10.1002/epi4.12685

DO - 10.1002/epi4.12685

M3 - 文章

C2 - 36524291

AN - SCOPUS:85146159967

SN - 2470-9239

VL - 8

SP - 154

EP - 164

JO - Epilepsia Open

JF - Epilepsia Open

IS - 1

ER -

Identification and clinical characteristics of a novel missense ADGRG1 variant in bilateral Frontoparietal Polymicrogyria: The electroclinical change from infancy to adulthood after Callosotomy in three siblings

Abstract

Bibliographical note

Keywords

Access to Document

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