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Mono and biallelic variants in HCN2 cause severe neurodevelopmental disorders

Authors :: Houdayer, Clara
Phillips, A Marie
Chabbert, Marie
Bourreau, Jennifer
Maroofian, Reza
Houlden, Henry
Richards, Kay
Saadi, Nebal Waill
Dad'ová, Eliška
Van Bogaert, Patrick
Rupin, Mailys
Keren, Boris
Charles, Perrine
Smol, Thomas
Riquet, Audrey
Pais, Lynn
O'Donnell-Luria, Anne
VanNoy, Grace E
Bayat, Allan
Møller, Rikke S
Olofsson, Kern
Abou Jamra, Rami
Syrbe, Steffen
Dasouki, Majed
Seaver, Laurie H
Sullivan, Jennifer A
Shashi, Vandana
Alkuraya, Fowzan S
Poss, Alexis F
Spence, J Edward
Schnur, Rhonda E
Forster, Ian C
Mckenzie, Chaseley E
Simons, Cas
Wang, Min
Snell, Penny
Kothur, Kavitha
Buckley, Michael
Roscioli, Tony
Elserafy, Noha
Dauriat, Benjamin
Procaccio, Vincent
Henrion, Daniel
Lenaers, Guy
Colin, Estelle
Verbeek, Nienke E
Van Gassen, Koen L
Legendre, Claire
Bonneau, Dominique
Reid, Christopher A
Howell, Katherine B
Ziegler, Alban
Legros, Christian
Houdayer, Clara
Phillips, A Marie
Chabbert, Marie
Bourreau, Jennifer
Maroofian, Reza
Houlden, Henry
Richards, Kay
Saadi, Nebal Waill
Dad'ová, Eliška
Van Bogaert, Patrick
Rupin, Mailys
Keren, Boris
Charles, Perrine
Smol, Thomas
Riquet, Audrey
Pais, Lynn
O'Donnell-Luria, Anne
VanNoy, Grace E
Bayat, Allan
Møller, Rikke S
Olofsson, Kern
Abou Jamra, Rami
Syrbe, Steffen
Dasouki, Majed
Seaver, Laurie H
Sullivan, Jennifer A
Shashi, Vandana
Alkuraya, Fowzan S
Poss, Alexis F
Spence, J Edward
Schnur, Rhonda E
Forster, Ian C
Mckenzie, Chaseley E
Simons, Cas
Wang, Min
Snell, Penny
Kothur, Kavitha
Buckley, Michael
Roscioli, Tony
Elserafy, Noha
Dauriat, Benjamin
Procaccio, Vincent
Henrion, Daniel
Lenaers, Guy
Colin, Estelle
Verbeek, Nienke E
Van Gassen, Koen L
Legendre, Claire
Bonneau, Dominique
Reid, Christopher A
Howell, Katherine B
Ziegler, Alban
Legros, Christian
Source :: Houdayer , C , Phillips , A M , Chabbert , M , Bourreau , J , Maroofian , R , Houlden , H , Richards , K , Saadi , N W , Dad'ová , E , Van Bogaert , P , Rupin , M , Keren , B , Charles , P , Smol , T , Riquet , A , Pais , L , O'Donnell-Luria , A , VanNoy , G E , Bayat , A , Møller , R S , Olofsson , K , Abou Jamra , R , Syrbe , S , Dasouki , M , Seaver , L H , Sullivan , J A , Shashi , V , Alkuraya , F S , Poss , A F , Spence , J E , Schnur , R E , Forster , I C , Mckenzie , C E , Simons , C , Wang , M , Snell , P , Kothur , K , Buckley , M , Roscioli , T , Elserafy , N , Dauriat , B , Procaccio , V , Henrion , D , Lenaers , G , Colin , E , Verbeek , N E , Van Gassen , K L , Legendre , C , Bonneau , D , Reid , C A , Howell , K B , Ziegler , A & Legros , C 2024 ' Mono and biallelic variants in HCN2 cause severe neurodevelopmental disorders ' medRxiv .
Publication Year :: 2024
Abstract: Hyperpolarization activated Cyclic Nucleotide (HCN) gated channels are crucial for various neurophysiological functions, including learning and sensory functions, and their dysfunction are responsible for brain disorders, such as epilepsy. To date, HCN2 variants have only been associated with mild epilepsy and recently, one monoallelic missense variant has been linked to developmental and epileptic encephalopathy. Here, we expand the phenotypic spectrum of HCN2- related disorders by describing twenty-one additional individuals from fifteen unrelated families carrying HCN2 variants. Seventeen individuals had developmental delay/intellectual disability (DD/ID), two had borderline DD/ID, and one had borderline DD. Ten individuals had epilepsy with DD/ID, with median age of onset of 10 months, and one had epilepsy with normal development. Molecular diagnosis identified thirteen different pathogenic HCN2 variants, including eleven missense variants affecting highly conserved amino acids, one frameshift variant, and one in-frame deletion. Seven variants were monoallelic of which five occurred de novo, one was not maternally inherited, one was inherited from a father with mild learning disabilities, and one was of unknown inheritance. The remaining six variants were biallelic, with four homozygous and two compound heterozygous variants. Functional studies using two-electrode voltage-clamp recordings in Xenopus laevis oocytes were performed on three monoallelic variants, p.(Arg324His), p.(Ala363Val), and p.(Met374Leu), and three biallelic variants, p.(Leu377His), p.(Pro493Leu) and p.(Gly587Asp). The p.(Arg324His) variant induced a strong increase of HCN2 conductance, while p.(Ala363Val) and p.(Met374Leu) displayed dominant negative effects, leading to a partial loss of HCN2 channel function. By confocal imaging, we found that the p.(Leu377His), p.(Pro493Leu) and p.(Gly587Asp) pathogenic variants impaired membrane trafficking, resulting in a complete loss of HCN2 elicited

Details

Database :: OAIster
Journal :: Houdayer , C , Phillips , A M , Chabbert , M , Bourreau , J , Maroofian , R , Houlden , H , Richards , K , Saadi , N W , Dad'ová , E , Van Bogaert , P , Rupin , M , Keren , B , Charles , P , Smol , T , Riquet , A , Pais , L , O'Donnell-Luria , A , VanNoy , G E , Bayat , A , Møller , R S , Olofsson , K , Abou Jamra , R , Syrbe , S , Dasouki , M , Seaver , L H , Sullivan , J A , Shashi , V , Alkuraya , F S , Poss , A F , Spence , J E , Schnur , R E , Forster , I C , Mckenzie , C E , Simons , C , Wang , M , Snell , P , Kothur , K , Buckley , M , Roscioli , T , Elserafy , N , Dauriat , B , Procaccio , V , Henrion , D , Lenaers , G , Colin , E , Verbeek , N E , Van Gassen , K L , Legendre , C , Bonneau , D , Reid , C A , Howell , K B , Ziegler , A & Legros , C 2024 ' Mono and biallelic variants in HCN2 cause severe neurodevelopmental disorders ' medRxiv .
Notes :: application/pdf, English
Publication Type :: Electronic Resource
Accession number :: edsoai.on1439557228
Document Type :: Electronic Resource