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3 research outputs found

Disruptive variants of CSDE1 associate with autism and interfere with neuronal development and synaptic transmission

Author: Adams D.J. (Darius J.)
Azamian M. (Mahshid)
Bai T. (Ting)
Ball S. (Susie)
Bernier R.A. (Raphael A.)
Calabrese G. (Giuseppe)
Chen M. (Meilin)
Eichler Evan
Galesi O.
Gecz Jozef
Gillentine M.A. (Madelyn A.)
Guo H. (Hui)
Haan Eric
Han L. (Lin)
Hasselt Peter
Hoekzema K. (Kendra)
Hopkin R.
Hu Z. (Zhengmao)
Hufnagel R.B. (Robert B.)
Jia X. (Xiangbin)
Kvarnung M. (Malin)
Lalani S.R. (Seema R.)
Li H. (Honghui)
Li K. (Kuokuo)
Li Y. (Ying)
Lindstrand A. (Anna)
Liu C. (Cenying)
Liu L. (Lijuan)
Liu P. (Pengfei)
Liu Y. (Yaning)
Long M. (Min)
Madan-Khetarpal Suneeta
Mancini Grazia
McWalter K. (Kirsty)
Monaghan K.G. (Kristin G.)
Ni H. (Hailun)
Nordenskjöld M.
Nordgren Ann
Osei-Owusu I.A. (Ikeoluwa A.)
Ou M. (Mengzhu)
Pang N. (Nan)
Peng J. (Jing)
Peng P. (Pengwei)
Pevsner J. (Jonathan)
Phornphutkul C. (Chanika)
Prada C.
Quan Y. (Yingting)
Racobaldo M. (Melissa)
Ranells J. (Judith)
Romano Corrado
Rosenfeld Jill
Scott D.A.
Sebastian Jessica
Shen L. (Lu)
Shieh J.T. (Joseph T.)
Stegmann A.P.A. (Alexander P.A.)
Tan J. (Jieqiong)
van Gassen K. (Koen)
Vries Boukje
Wang T. (Tianyun)
Wu H. (Huidan)
Xia F. (Fan)
Xia K. (Kun)
Xie W. (Wei)
Xu T. (Tao)
Xu Z.-Q.D. (Zhi-Qing David)
Zhang Q. (Qiumeng)
Zhang Y. (Yaowen)
Zhang Y. (Yu)
Zhao J. (Jingping)
Zhao R. (Rongjuan)
Zhu T. (Tengfei)
Zou X. (Xiaobing)
Publication venue: 'American Association for the Advancement of Science (AAAS)'
Publication date: 25/09/2019
Field of study

textabstractRNA binding proteins are key players in posttranscriptional regulation and have been implicated in neurodevelopmental and neuropsychiatric disorders. Here, we report a significant burden of heterozygous, likely genedisrupting variants in CSDE1 (encoding a highly constrained RNA binding protein) among patients with autism and related neurodevelopmental disabilities. Analysis of 17 patients identifies common phenotypes including autism, intellectual disability, language and motor delay, seizures, macrocephaly, and variable ocular abnormalities. HITSCLIP revealed that Csde1binding targets are enriched in autismassociated gene sets, especially FMRP targets, and in neuronal development and synaptic plasticity–related pathways. Csde1 knockdown in primary mouse cortical neurons leads to an overgrowth of the neurites and abnormal dendritic spine morphology/synapse formation and impaired synaptic transmission, whereas mutant and knockdown experiments in Drosophila result in defects in synapse growth and synaptic transmission. Our study defines a new autismrelated syndrome and highlights the functional role of CSDE1 in synapse development and synaptic transmission

Erasmus University Digital Repository

Disruptive variants of CSDE1 associate with autism and interfere with neuronal development and synaptic transmission

Author: Adams Darius J.
Azamian Mahshid
Bai Ting
Ball Susie
Bernier Raphael A.
Calabrese Giuseppe
Chen Meilin
de Vries Bert B. A.
Eichler Evan E.
Galesi Ornella
Gecz Jozef
Gillentine Madelyn A.
Guo Hui
Haan Eric
Han Lin
Hoekzema Kendra
Hopkin Robert J.
Hu Zhengmao
Hufnagel Robert B.
Jia Xiangbin
Kvarnung Malin
Lalani Seema R.
Li Honghui
Li Kuokuo
Li Ying
Lindstrand Anna
Liu Cenying
Liu Lijuan
Liu Pengfei
Liu Yaning
Long Min
Madan-Khetarpal Suneeta
Mancini Grazia M. S.
McWalter Kirsty
Monaghan Kristin G.
Ni Hailun
Nordenskjold Magnus
Nordgren Ann
Osei-Owusu Ikeoluwa A.
Ou Mengzhu
Pang Nan
Peng Jing
Peng Pengwei
Pevsner Jonathan
Phornphutkul Chanika
Prada Carlos E.
Quan Yingting
Racobaldo Melissa
Ranells Judith
Romano Corrado
Rosenfeld Jill A.
Scott Daryl A.
Sebastian Jessica
Shen Lu
Shieh Joseph T.
Stegmann Alexander P. A.
Tan Jieqiong
van Gassen Koen
van Hasselt Peter M.
Wang Tianyun
Wu Huidan
Xia Fan
Xia Kun
Xie Wei
Xu Tao
Xu Zhi-Qing David
Zhang Qiumeng
Zhang Yaowen
Zhang Yu
Zhao Jingping
Zhao Rongjuan
Zhu Tengfei
Zou Xiaobing
Publication venue: 'American Association for the Advancement of Science (AAAS)'
Publication date: 01/09/2019
Field of study

RNA binding proteins are key players in posttranscriptional regulation and have been implicated in neuro-developmental and neuropsychiatric disorders. Here, we report a significant burden of heterozygous, likely gene-disrupting variants in CSDE1 (encoding a highly constrained RNA binding protein) among patients with autism and related neurodevelopmental disabilities. Analysis of 17 patients identifies common phenotypes including autism, intellectual disability, language and motor delay, seizures, macrocephaly, and variable ocular abnormalities. HITS-CLIP revealed that Csde1-binding targets are enriched in autism-associated gene sets, especially FMRP targets, and in neuronal development and synaptic plasticity-related pathways. Csde1 knockdown in primary mouse cortical neurons leads to an overgrowth of the neurites and abnormal dendritic spine morphology/synapse formation and impaired synaptic transmission, whereas mutant and knockdown experiments in Drosophila result in defects in synapse growth and synaptic transmission. Our study defines a new autism-related syndrome and highlights the functional role of CSDE1 in synapse development and synaptic transmission

Maastricht University Research Portal

Germline variants in tumor suppressor FBXW7 lead to impaired ubiquitination and a neurodevelopmental syndrome

Author: Accogli Andrea
Agre Katherine E.
Alhuzaimi Dana E.
Amburgey Kimberly
Amor David J.
Ascher David B.
Au P.Y. Billie
Bahlo Melanie
Baker Joshua J.
Barel Ortal
Besnard Thomas
Björnsson Hans Tómas
Blok Laura E.R.
Boyce Jessica O.
Broad Center for Mendelian Genomics
Bruel Ange-Line
Burns Wechsler Stephanie
Capra Valeria
Carmignac Virginie
Chilton Ilana
Christodoulou John
Chung Wendy K.
Cogné Benjamin
Cornaton Jenny
Costain Gregory
Crunk Amy
de Haan Hugoline
Devinsky Orrin
Dias Kerith-Rae
Dong Xiaomin
Dowling James J.
Evans Carey-Anne
Friðriksdóttir Rún
Gardiner Fiona J.
Griffith Christopher
Gupta Aditi
Hainline Bryan E.
Hayeems Robin Z.
Heise Elizabeth M.
Hildebrand Michael S.
Isidor Bertrand
Jansen Sandra
Kaspi Antony
Kato Kohji
Katrínardóttir Hildigunnur
Klee Eric W.
Koyama Norihisa
Lim Sze Chern
Lockhart Paul J.
Lynch Sally A.
Mandelstam Simone
Marcelis Carlo
Mariani Milena
Marle Nathalie
Mefford Heather C.
Millan Francisca
Monaghan Kristin G.
Morgan Angela T.
Morice-Picard Fanny
Morleo Manuela
Moutton Sebastien
Muir Alison M.
Nguyen Thanh Binh
Niu Zhiyv
Nizon Mathilde
Ogi Tomoo
Person Richard
Picker Jonathan
Piton Amelie
Raas-Rothschild Annick
Racobaldo Melissa
Rasmussen Kristen J.
Revah-Politi Anya
Rhodes Lindsay
Richards Sarah
Richmond Christopher
Rodan Lance H.
Roscioli Tony
Sachdev Rani
Sadedin Simon
Sapp Katie
Scala Marcello
Scheffer Ingrid E.
Schenck Annette
Schimmenti Lisa A.
Schneider Amy L.
Schwartz Marc A.
Silk Michael A.
Stefánsson Kári
Stephenson Sarah E.M.
Stimach Chandler
Suk-Ying Goh Elaine
Sulem Patrick
Tan Tiong Yang
Temple Suzanna E.L.
Torella Annalaura
TUDP Study Group
Vincent Marie
Walker Susan
Wallis Mathew
Weisfisz Quinten
Wentzensen Ingrid M.
White Susan M.
Willems Marjolaine
Zeev Bruria Ben
Zhu Ying
Publication venue: Elsevier
Publication date: 01/01/2022
Field of study

Neurodevelopmental disorders are highly heterogenous conditions resulting from abnormalities of brain architecture and/or function. FBXW7 (F-box and WD-repeat-domain-containing 7), a recognized developmental regulator and tumor suppressor, has been shown to regulate cell-cycle progression and cell growth and survival by targeting substrates including CYCLIN E1/2 and NOTCH for degradation via the ubiquitin proteasome system. We used a genotype-first approach and global data-sharing platforms to identify 35 individuals harboring de novo and inherited FBXW7 germline monoallelic chromosomal deletions and nonsense, frameshift, splice-site, and missense variants associated with a neurodevelopmental syndrome. The FBXW7 neurodevelopmental syndrome is distinguished by global developmental delay, borderline to severe intellectual disability, hypotonia, and gastrointestinal issues. Brain imaging detailed variable underlying structural abnormalities affecting the cerebellum, corpus collosum, and white matter. A crystal-structure model of FBXW7 predicted that missense variants were clustered at the substrate-binding surface of the WD40 domain and that these might reduce FBXW7 substrate binding affinity. Expression of recombinant FBXW7 missense variants in cultured cells demonstrated impaired CYCLIN E1 and CYCLIN E2 turnover. Pan-neuronal knockdown of the Drosophila ortholog, archipelago, impaired learning and neuronal function. Collectively, the data presented herein provide compelling evidence of an F-Box protein-related, phenotypically variable neurodevelopmental disorder associated with monoallelic variants in FBXW7

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PubMed Central