Expanding the phenotypic spectrum of GABRG2 variants: a recurrent GABRG2 missense variant associated with a severe phenotype

Fanggeng Zou; Kirsty McWalter; Lindsay Schmidt; Amy Decker; Jonathan D Picker; Sharyn Lincoln; David A Sweetser; Lauren C Briere; Chellamani Harini; Eric Marsh; Livija Medne; Raymond Y Wang; Karen Leydiker; Andrew Mower; Gepke Visser; Inge Cuppen; Koen L van Gassen; Jasper van der Smagt; Adeel Yousaf; Michael Tennison; Anita Shanmugham; Elizabeth Butler; Gabriele Richard; Dianalee McKnight

doi:10.1080/01677063.2017.1315417

Expanding the phenotypic spectrum of GABRG2 variants: a recurrent GABRG2 missense variant associated with a severe phenotype

Fanggeng Zou
, Kirsty McWalter
, Lindsay Schmidt
, Amy Decker
, Jonathan D Picker
, Sharyn Lincoln
, David A Sweetser
, Lauren C Briere
, Chellamani Harini
, Eric Marsh
, Livija Medne
, Raymond Y Wang
, Karen Leydiker
, Andrew Mower
, Gepke Visser
, Inge Cuppen
, Koen L van Gassen
, Jasper van der Smagt
, Adeel Yousaf
, Michael Tennison

Anita Shanmugham, Elizabeth Butler, Gabriele Richard, Dianalee McKnight^*,

^*Corresponding author for this work

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

Abstract

Pathogenic missense and truncating variants in the GABRG2 gene cause a spectrum of epilepsies, from Dravet syndrome to milder simple febrile seizures. In most cases, pathogenic missense variants in the GABRG2 gene segregate with a febrile seizure phenotype. In this case series, we report a recurrent, de novo missense variant (c0.316 G > A; p.A106T) in the GABRG2 gene that was identified in five unrelated individuals. These patients were described to have a more severe phenotype than previously reported for GABRG2 missense variants. Common features include variable early-onset seizures, significant motor and speech delays, intellectual disability, hypotonia, movement disorder, dysmorphic features and vision/ocular issues. Our report further explores a recurrent pathogenic missense variant within the GABRG2 variant family and broadens the spectrum of associated phenotypes for GABRG2-associated disorders.

Original language	English
Pages (from-to)	30-36
Number of pages	7
Journal	Journal of Neurogenetics
Volume	31
Issue number	1-2
DOIs	https://doi.org/10.1080/01677063.2017.1315417
Publication status	Published - 4 May 2017

Keywords

Epilepsy
GABRG2
genetics
missense
phenotype
seizures

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Zou, F., McWalter, K., Schmidt, L., Decker, A., Picker, J. D., Lincoln, S., Sweetser, D. A., Briere, L. C., Harini, C., Marsh, E., Medne, L., Wang, R. Y., Leydiker, K., Mower, A., Visser, G., Cuppen, I., van Gassen, K. L., van der Smagt, J., Yousaf, A. (2017). Expanding the phenotypic spectrum of GABRG2 variants: a recurrent GABRG2 missense variant associated with a severe phenotype. Journal of Neurogenetics, 31(1-2), 30-36. https://doi.org/10.1080/01677063.2017.1315417

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title = "Expanding the phenotypic spectrum of GABRG2 variants: a recurrent GABRG2 missense variant associated with a severe phenotype",

abstract = "Pathogenic missense and truncating variants in the GABRG2 gene cause a spectrum of epilepsies, from Dravet syndrome to milder simple febrile seizures. In most cases, pathogenic missense variants in the GABRG2 gene segregate with a febrile seizure phenotype. In this case series, we report a recurrent, de novo missense variant (c0.316 G > A; p.A106T) in the GABRG2 gene that was identified in five unrelated individuals. These patients were described to have a more severe phenotype than previously reported for GABRG2 missense variants. Common features include variable early-onset seizures, significant motor and speech delays, intellectual disability, hypotonia, movement disorder, dysmorphic features and vision/ocular issues. Our report further explores a recurrent pathogenic missense variant within the GABRG2 variant family and broadens the spectrum of associated phenotypes for GABRG2-associated disorders.",

keywords = "Epilepsy, GABRG2, genetics, missense, phenotype, seizures",

author = "Fanggeng Zou and Kirsty McWalter and Lindsay Schmidt and Amy Decker and Picker, \{Jonathan D\} and Sharyn Lincoln and Sweetser, \{David A\} and Briere, \{Lauren C\} and Chellamani Harini and Eric Marsh and Livija Medne and Wang, \{Raymond Y\} and Karen Leydiker and Andrew Mower and Gepke Visser and Inge Cuppen and \{van Gassen\}, \{Koen L\} and \{van der Smagt\}, Jasper and Adeel Yousaf and Michael Tennison and Anita Shanmugham and Elizabeth Butler and Gabriele Richard and Dianalee McKnight",

year = "2017",

month = may,

day = "4",

doi = "10.1080/01677063.2017.1315417",

language = "English",

volume = "31",

pages = "30--36",

journal = "Journal of Neurogenetics",

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Zou, F, McWalter, K, Schmidt, L, Decker, A, Picker, JD, Lincoln, S, Sweetser, DA, Briere, LC, Harini, C, Marsh, E, Medne, L, Wang, RY, Leydiker, K, Mower, A, Visser, G, Cuppen, I, van Gassen, KL, van der Smagt, J, Yousaf, A, Tennison, M, Shanmugham, A, Butler, E, Richard, G, McKnight, D 2017, 'Expanding the phenotypic spectrum of GABRG2 variants: a recurrent GABRG2 missense variant associated with a severe phenotype', Journal of Neurogenetics, vol. 31, no. 1-2, pp. 30-36. https://doi.org/10.1080/01677063.2017.1315417

TY - JOUR

T1 - Expanding the phenotypic spectrum of GABRG2 variants

T2 - a recurrent GABRG2 missense variant associated with a severe phenotype

AU - Zou, Fanggeng

AU - McWalter, Kirsty

AU - Schmidt, Lindsay

AU - Decker, Amy

AU - Picker, Jonathan D

AU - Lincoln, Sharyn

AU - Sweetser, David A

AU - Briere, Lauren C

AU - Harini, Chellamani

AU - Marsh, Eric

AU - Medne, Livija

AU - Wang, Raymond Y

AU - Leydiker, Karen

AU - Mower, Andrew

AU - Visser, Gepke

AU - Cuppen, Inge

AU - van Gassen, Koen L

AU - van der Smagt, Jasper

AU - Yousaf, Adeel

AU - Tennison, Michael

AU - Shanmugham, Anita

AU - Butler, Elizabeth

AU - Richard, Gabriele

AU - McKnight, Dianalee

PY - 2017/5/4

Y1 - 2017/5/4

N2 - Pathogenic missense and truncating variants in the GABRG2 gene cause a spectrum of epilepsies, from Dravet syndrome to milder simple febrile seizures. In most cases, pathogenic missense variants in the GABRG2 gene segregate with a febrile seizure phenotype. In this case series, we report a recurrent, de novo missense variant (c0.316 G > A; p.A106T) in the GABRG2 gene that was identified in five unrelated individuals. These patients were described to have a more severe phenotype than previously reported for GABRG2 missense variants. Common features include variable early-onset seizures, significant motor and speech delays, intellectual disability, hypotonia, movement disorder, dysmorphic features and vision/ocular issues. Our report further explores a recurrent pathogenic missense variant within the GABRG2 variant family and broadens the spectrum of associated phenotypes for GABRG2-associated disorders.

AB - Pathogenic missense and truncating variants in the GABRG2 gene cause a spectrum of epilepsies, from Dravet syndrome to milder simple febrile seizures. In most cases, pathogenic missense variants in the GABRG2 gene segregate with a febrile seizure phenotype. In this case series, we report a recurrent, de novo missense variant (c0.316 G > A; p.A106T) in the GABRG2 gene that was identified in five unrelated individuals. These patients were described to have a more severe phenotype than previously reported for GABRG2 missense variants. Common features include variable early-onset seizures, significant motor and speech delays, intellectual disability, hypotonia, movement disorder, dysmorphic features and vision/ocular issues. Our report further explores a recurrent pathogenic missense variant within the GABRG2 variant family and broadens the spectrum of associated phenotypes for GABRG2-associated disorders.

KW - Epilepsy

KW - GABRG2

KW - genetics

KW - missense

KW - phenotype

KW - seizures

UR - https://www.scopus.com/pages/publications/85018457577

U2 - 10.1080/01677063.2017.1315417

DO - 10.1080/01677063.2017.1315417

M3 - Article

C2 - 28460589

AN - SCOPUS:85018457577

SN - 0167-7063

VL - 31

SP - 30

EP - 36

JO - Journal of Neurogenetics

JF - Journal of Neurogenetics

IS - 1-2

ER -

Expanding the phenotypic spectrum of GABRG2 variants: a recurrent GABRG2 missense variant associated with a severe phenotype

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Keywords

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