De Novo Missense Variants in SLC32A1 Cause a Developmental and Epileptic Encephalopathy Due to Impaired GABAergic Neurotransmission

被引：10

作者：

Platzer, Konrad ^{[1
]}

Sticht, Heinrich ^{[2
]}

Bupp, Caleb ^{[3
]}

Ganapathi, Mythily ^{[4
]}

Pereira, Elaine M. ^{[5
]}

Le Guyader, Gwenael ^{[6
]}

Bilan, Frederic ^{[6
,7
]}

Henderson, Lindsay B. ^{[8
]}

Lemke, Johannes R. ^{[1
,9
]}

Taschenberger, Holger ^{[10
]}

Brose, Nils ^{[10
]}

Abou Jamra, Rami ^{[1
]}

Wojcik, Sonja M. ^{[10
]}

机构：

[1] Univ Leipzig, Inst Human Genet, Med Ctr, Leipzig, Germany

[2] Friedrich Alexander Univ Erlangen Nurnberg, Inst Biochem, Erlangen, Germany

[3] Spectrum Hlth Med Genet, Grand Rapids, MI USA

[4] Columbia Univ, Dept Pathol & Cell Biol, Med Ctr, New York, NY USA

[5] Columbia Univ, Dept Pediat, Irving Med Ctr, New York, NY USA

[6] Poitiers Univ Hosp Ctr, Dept Genet, Poitiers, France

[7] Univ Poitiers, Lab Expt & Clin Neurosci LNEC, INSERM, U1084, Poitiers, France

[8] GeneDx, Gaithersburg, MD USA

[9] Univ Leipzig, Ctr Rare Dis, Med Ctr, Leipzig, Germany

[10] Max Planck Inst Multidisciplinary Sci, Dept Mol Neurobiol, Gottingen, Germany

来源：

ANNALS OF NEUROLOGY | 2022年 / 92卷 / 06期

关键词：

VESICULAR GABA TRANSPORTER; FEBRILE SEIZURES; FAMILIES SLC32; RELEASE; PATHOGENICITY; TRANSMISSION; EXPRESSION; CA2+;

D O I：

10.1002/ana.26485

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Objective Rare inherited missense variants in SLC32A1, the gene that encodes the vesicular gamma-aminobutyric acid (GABA) transporter, have recently been shown to cause genetic epilepsy with febrile seizures plus. We aimed to clarify if de novo missense variants in SLC32A1 can also cause epilepsy with impaired neurodevelopment. Methods Using exome sequencing, we identified four individuals with a developmental and epileptic encephalopathy and de novo missense variants in SLC32A1. To assess causality, we performed functional evaluation of the identified variants in a murine neuronal cell culture model. Results The main phenotype comprises moderate-to-severe intellectual disability, infantile-onset epilepsy within the first 18 months of life, and a choreiform, dystonic, or dyskinetic movement disorder. In silico modeling and functional analyses reveal that three of these variants, which are located in helices that line the putative GABA transport pathway, result in reduced quantal size, consistent with impaired filling of synaptic vesicles with GABA. The fourth variant, located in the vesicular gamma-aminobutyric acid N-terminus, does not affect quantal size, but increases presynaptic release probability, leading to more severe synaptic depression during high-frequency stimulation. Thus, variants in vesicular gamma-aminobutyric acid can impair GABAergic neurotransmission through at least two mechanisms, by affecting synaptic vesicle filling and by altering synaptic short-term plasticity. Interpretation This work establishes de novo missense variants in SLC32A1 as a novel cause of a developmental and epileptic encephalopathy. Summary for Social Media If Published @platzer_k @lemke_johannes @RamiJamra @Nirgalito @GeneDx The SLC family 32 Member 1 (SLC32A1) is the only protein identified to date, that loads gamma-aminobutyric acid (GABA) and glycine into synaptic vesicles, and is therefore also known as the vesicular GABA transporter (VGAT) or vesicular inhibitory amino acid transporter (VIAAT). Rare inherited missense variants in SLC32A1, the gene that encodes VGAT/vesicular inhibitory amino acid transporter, have recently been shown to cause genetic epilepsy with febrile seizures plus. We aimed to clarify if de novo missense variants in SLC32A1 can also cause epilepsy with impaired neurodevelopment. We report on four individuals with de novo missense variants in SLC32A1 and a developmental and epileptic encephalopathy with infantile onset epilepsy. We establish causality of the variants via in silico modeling and their functional evaluation in a murine neuronal cell culture model. SLC32A1 variants represent a novel genetic etiology in neurodevelopmental disorders with epilepsy and a new GABA-related disease mechanism. ANN NEUROL 2022

引用

页码：958 / 973

页数：16

共 50 条

[21] De novo variants in the alternative exon 5 of SCN8A cause epileptic encephalopathy
Berkovic, Samuel F.
Dixon-Salazar, Tracy
Goldstein, David B.
Heinzen, Erin L.
Laughlin, Brandon L.
Lowenstein, Daniel H.
Lubbers, Laura
Milder, Julie
Stewart, Randall
Whittemore, Vicky
Angione, Kaitlin
Bazil, Carl W.
Bier, Louise
Bluvstein, Judith
Brimble, Elise
Campbell, Colleen
Chambers, Chelsea
Choi, Hyunmi
Cilio, Maria Roberta
Ciliberto, Michael
Cornes, Susannah
Delanty, Norman
Demarest, Scott
Devinsky, Orrin
Dlugos, Dennis
Dubbs, Holly
Dugan, Patricia
Ernst, Michelle E.
Gallentine, William
Gibbons, Melissa
Goodkin, Howard
Grinton, Bronwyn
Helbig, Ingo
Jansen, Laura
Johnson, Kaleas
Joshi, Charuta
Lippa, Natalie C.
Makati, Mohamad A.
Marsh, Eric
Martinez, Alejandro
Millichap, John
Moskovich, Yuliya
Mulhern, Maureen S.
Numis, Adam
Park, Kristen
Poduri, Annapurna
Porter, Brenda
Sands, Tristan T.
Scheffer, Ingrid E.
Sheidley, Beth
GENETICS IN MEDICINE, 2018, 20 (02) : 275 - 281
[22] De novo missense variants in KDM1A cause a neurodevelopmental disorder
Berking, Ann-Cathrine
Pabst, Brigitte
Kordes, Uwe R.
Muntnich, Lucas
Kratz, Christian
Bohne, Jens
Auber, Bernd
Ripperger, Tim
EUROPEAN JOURNAL OF HUMAN GENETICS, 2024, 32 : 1198 - 1199
[23] A de novo heterozygous missense BSCL2 variant in 2 siblings with intractable developmental and epileptic encephalopathy
Fernandez-Marmiesse, Ana
Sanchez-Iglesias, Sofia
Darling, Alejandra
O'Callaghan, Maria M.
Tonda, Raul
Jou, Cristina
Araujo-Vilar, David
SEIZURE-EUROPEAN JOURNAL OF EPILEPSY, 2019, 71 : 161 - 165
[24] Missense Variants in RHOBTB2 Cause a Developmental and Epileptic Encephalopathy in Humans, and Altered Levels Cause Neurological Defects in Drosophila
Straub, Jonas
Konrad, Enrico D. H.
Gruener, Johanna
Toutain, Annick
Bok, Levinus A.
Cho, Megan T.
Crawford, Heather P.
Dubbs, Holly
Douglas, Ganka
Jobling, Rebekah
Johnson, Diana
Krock, Bryan
Mikati, Mohamad A.
Nesbitt, Addie
Nicolai, Joost
Phillips, Meredith
Poduri, Annapurna
Ortiz-Gonzalez, Xilma R.
Powis, Zoe
Santani, Avni
Smith, Lacey
Stegmann, Alexander P. A.
Stumpel, Constance
Vreeburg, Maaike
Fliedner, Anna
Gregor, Anne
Sticht, Heinrich
Zweier, Christiane
AMERICAN JOURNAL OF HUMAN GENETICS, 2018, 102 (01) : 44 - 57
[25] De novo truncating variants in the intronless IRF2BPL are responsible for developmental epileptic encephalopathy
Mau-Them, F. Tran
Guibaud, L.
Duplomb, L.
Keren, B.
Lindstrom, K.
Marey, I
Mochel, F.
van den Boogaard, M. J.
Oegema, R.
Nava, C.
Masurel, A.
Jouan, T.
Jansen, F. E.
Au, M.
Chen, Agnes H.
Cho, M.
Duffourd, Y.
Lozier, E.
Konovalov, F.
Sharkov, A.
Korostelev, S.
Urteaga, B.
Dickson, P.
Vera, M.
Martinez-Agosto, Julian A.
Begemann, A.
Zweier, M.
Schmitt-Mechelke, T.
Rauch, A.
Philippe, C.
van Gassen, K.
Nelson, S.
Graham, J. M., Jr.
Friedman, J.
Faivre, L.
Lin, H. J.
Thauvin-Robinet, C.
Vitobello, A.
GENETICS IN MEDICINE, 2019, 21 (04) : 1008 - 1014
[26] De novo variants in RHOBTB2, an atypical Rho GTPase gene, cause epileptic encephalopathy
Belal, Hazrat
Nakashima, Mitsuko
Matsumoto, Hiroshi
Yokochi, Kenji
Taniguchi-Ikeda, Mariko
Aoto, Kazushi
Amin, Mohammed Badrul
Maruyama, Azusa
Nagase, Hiroaki
Mizuguchi, Takeshi
Miyatake, Satoko
Miyake, Noriko
Iijima, Kazumoto
Nonoyama, Shigeaki
Matsumoto, Naomichi
Saitsu, Hirotomo
HUMAN MUTATION, 2018, 39 (08) : 1070 - 1075
[27] De novo hotspot variants in CYFIP2 cause early-onset epileptic encephalopathy
Nakashima, Mitsuko
Kato, Mitsuhiro
Aoto, Kazushi
Shiina, Masaaki
Belal, Hazrat
Mukaida, Souichi
Kumada, Satoko
Sato, Atsushi
Zerem, Ayelet
Lerman-Sagie, Tally
Lev, Dorit
Leong, Huey Yin
Tsurusaki, Yoshinori
Mizuguchi, Takeshi
Miyatake, Satoko
Miyake, Noriko
Ogata, Kazuhiro
Saitsu, Hirotomo
Matsumoto, Naomichi
ANNALS OF NEUROLOGY, 2018, 83 (04) : 794 - 806
[28] De Novo Pathogenic Variants in CACNA1E Cause Developmental and Epileptic Encephalopathy with Contractures, Macrocephaly, and Dyskinesias (vol 103, pg 666, 2018)
Helbig, Katherine L.
Lauerer, Robert J.
Bahr, Jacqueline C.
Souza, Ivana A.
Myers, Candace T.
Uysal, Betul
Schwarz, Niklas
Gandini, Maria A.
Huang, Sun
Keren, Boris
Mignot, Cyril
Afenjar, Alexandra
de Villemeur, Thierry Billette
Heron, Delphine
Nava, Caroline
Valence, Stephanie
Buratti, Julien
Fagerberg, Christina R.
Soerensen, Kristina P.
Kibaek, Maria
Kamsteeg, Erik-Jan
Koolen, David A.
Gunning, Boudewijn
Schelhaas, H. Jurgen
Kruer, Michael C.
Fox, Jordana
Bakhtiari, Somayeh
Jarrar, Randa
Padilla-Lopez, Sergio
Lindstrom, Kristin
Jin, Sheng Chih
Zeng, Xue
Bilguvar, Kaya
Papavasileiou, Antigone
Xing, Qinghe
Zhu, Changlian
Boysen, Katja
Vairo, Filippo
Lanpher, Brendan C.
Klee, Eric W.
Tillema, Jan-Mendelt
Payne, Eric T.
Cousin, Margot A.
Kruisselbrink, Teresa M.
Wick, Myra J.
Baker, Joshua
Haan, Eric
Smith, Nicholas
Sadeghpour, Azita
Davis, Erica E.
AMERICAN JOURNAL OF HUMAN GENETICS, 2019, 104 (03) : 562 - 562
[29] Homozygous variants of PACS1cause an autosomal recessive developmental and epileptic encephalopathy
Chatron, N.
Rad, A.
Efthymiou, S.
Labalme, A.
Vona, B.
Carneiro, M.
Saeidi, K.
Houlden, H.
Sultan, T.
Maroofian, R.
Lesca, G.
EUROPEAN JOURNAL OF HUMAN GENETICS, 2020, 28 (SUPPL 1) : 409 - 410
[30] De novo mutations in HCN1 cause early infantile epileptic encephalopathy
Nava, Caroline
Dalle, Carine
Rastetter, Agnes
Striano, Pasquale
de Kovel, Carolien G. F.
Nabbout, Rima
Cances, Claude
Ville, Dorothee
Brilstra, Eva H.
Gobbi, Giuseppe
Raffo, Emmanuel
Bouteiller, Delphine
Marie, Yannick
Trouillard, Oriane
Robbiano, Angela
Keren, Boris
Agher, Dahbia
Roze, Emmanuel
Lesage, Suzanne
Nicolas, Aude
Brice, Alexis
Baulac, Michel
Vogt, Cornelia
El Hajj, Nady
Schneiderr, Eberhard
Suls, Arvid
Weckhuysen, Sarah
Gormley, Padhraig
Lehesjoki, Anna-Elina
De Jonghe, Peter
Helbig, Ingo
Baulac, Stephanie
Zara, Federico
Koeleman, Bobby P. C.
Haaf, Thomas
LeGuern, Eric
Depienne, Christel
NATURE GENETICS, 2014, 46 (06) : 640 - 645

← 1 2 3 4 5 →