The different clinical facets of SYN1-related neurodevelopmental disorders

Ilaria Parenti; Elsa Leitão; Alma Kuechler; Laurent Villard; Cyril Goizet; Cécile Courdier; Allan Bayat; Alessandra Rossi; Sophie Julia; Ange Line Bruel; Frédéric Tran Mau-Them; Sophie Nambot; Daphné Lehalle; Marjolaine Willems; James Lespinasse; Jamal Ghoumid; Roseline Caumes; Thomas Smol; Salima El Chehadeh; Elise Schaefer; Marie Thérèse Abi-Warde; Boris Keren; Alexandra Afenjar; Anne Claude Tabet; Jonathan Levy; Anna Maruani; Ángel Aledo-Serrano; Waltraud Garming; Clara Milleret-Pignot; Anna Chassevent; Marije Koopmans; Nienke E. Verbeek; Richard Person; Rebecca Belles; Gary Bellus; Bonnie A. Salbert; Frank J. Kaiser; Laure Mazzola; Philippe Convers; Laurine Perrin; Amélie Piton; Gert Wiegand; Andrea Accogli; Francesco Brancati; Fabio Benfenati; Nicolas Chatron; David Lewis-Smith; Rhys H. Thomas; Federico Zara; Pasquale Striano

doi:10.3389/fcell.2022.1019715

The different clinical facets of SYN1-related neurodevelopmental disorders

Ilaria Parenti, Elsa Leitão, Alma Kuechler, Laurent Villard, Cyril Goizet, Cécile Courdier, Allan Bayat, Alessandra Rossi, Sophie Julia, Ange Line Bruel, Frédéric Tran Mau-Them, Sophie Nambot, Daphné Lehalle, Marjolaine Willems, James Lespinasse, Jamal Ghoumid, Roseline Caumes, Thomas Smol, Salima El Chehadeh, Elise SchaeferMarie Thérèse Abi-Warde, Boris Keren, Alexandra Afenjar, Anne Claude Tabet, Jonathan Levy, Anna Maruani, Ángel Aledo-Serrano, Waltraud Garming, Clara Milleret-Pignot, Anna Chassevent, Marije Koopmans, Nienke E. Verbeek, Richard Person, Rebecca Belles, Gary Bellus, Bonnie A. Salbert, Frank J. Kaiser, Laure Mazzola, Philippe Convers, Laurine Perrin, Amélie Piton, Gert Wiegand, Andrea Accogli, Francesco Brancati, Fabio Benfenati, Nicolas Chatron, David Lewis-Smith, Rhys H. Thomas, Federico Zara, Pasquale Striano

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

16 Citationer (Scopus)

Abstract

Synapsin-I (SYN1) is a presynaptic phosphoprotein crucial for synaptogenesis and synaptic plasticity. Pathogenic SYN1 variants are associated with variable X-linked neurodevelopmental disorders mainly affecting males. In this study, we expand on the clinical and molecular spectrum of the SYN1-related neurodevelopmental disorders by describing 31 novel individuals harboring 22 different SYN1 variants. We analyzed newly identified as well as previously reported individuals in order to define the frequency of key features associated with these disorders. Specifically, behavioral disturbances such as autism spectrum disorder or attention deficit hyperactivity disorder are observed in 91% of the individuals, epilepsy in 82%, intellectual disability in 77%, and developmental delay in 70%. Seizure types mainly include tonic-clonic or focal seizures with impaired awareness. The presence of reflex seizures is one of the most representative clinical manifestations related to SYN1. In more than half of the cases, seizures are triggered by contact with water, but other triggers are also frequently reported, including rubbing with a towel, fever, toothbrushing, fingernail clipping, falling asleep, and watching others showering or bathing. We additionally describe hyperpnea, emotion, lighting, using a stroboscope, digestive troubles, and defecation as possible triggers in individuals with SYN1 variants. The molecular spectrum of SYN1 variants is broad and encompasses truncating variants (frameshift, nonsense, splicing and start-loss variants) as well as non-truncating variants (missense substitutions and in-frame duplications). Genotype-phenotype correlation revealed that epileptic phenotypes are enriched in individuals with truncating variants. Furthermore, we could show for the first time that individuals with early seizures onset tend to present with severe-to-profound intellectual disability, hence highlighting the existence of an association between early seizure onset and more severe impairment of cognitive functions. Altogether, we present a detailed clinical description of the largest series of individuals with SYN1 variants reported so far and provide the first genotype-phenotype correlations for this gene. A timely molecular diagnosis and genetic counseling are cardinal for appropriate patient management and treatment.

Originalsprog	Engelsk
Artikelnummer	1019715
Tidsskrift	Frontiers in Cell and Developmental Biology
Vol/bind	10
ISSN	2296-634X
DOI	https://doi.org/10.3389/fcell.2022.1019715
Status	Udgivet - 8 dec. 2022
Udgivet eksternt	Ja

Bibliografisk note

Funding Information:
This research was funded in whole, or in part, by the Wellcome Trust [203914/Z/16/Z] supporting DL-S. For the purpose of Open Access, the author has applied a CC BY public copyright license to any Author Accepted Manuscript version arising from this submission. CD is supported by Universitätsklinikum Essen and received grants from the Deutsche Forschungsgemeinschaft (DFG). AB is funded by a BRIDGE—Translational Excellence Programme grant funded by the Novo Nordisk Foundation, grant agreement number: NNF20SA0064340. FB received funding from the Italian Ministry of Health.

Funding Information:
We thank the patients and their families for participating to this study. We acknowledge support from the Open Access Publication Fund of the University of Duisburg-Essen. One patient included in this study was diagnosed thanks to Defidiag (NCT04154891), a study supported by The French Ministry of Health and the Agence Nationale de la Recherche (ANR-10-IAHU-01).

Publisher Copyright:
Copyright © 2022 Parenti, Leitão, Kuechler, Villard, Goizet, Courdier, Bayat, Rossi, Julia, Bruel, Tran Mau-Them, Nambot, Lehalle, Willems, Lespinasse, Ghoumid, Caumes, Smol, El Chehadeh, Schaefer, Abi-Warde, Keren, Afenjar, Tabet, Levy, Maruani, Aledo-Serrano, Garming, Milleret-Pignot, Chassevent, Koopmans, Verbeek, Person, Belles, Bellus, Salbert, Kaiser, Mazzola, Convers, Perrin, Piton, Wiegand, Accogli, Brancati, Benfenati, Chatron, Lewis-Smith, Thomas, Zara, Striano, Lesca and Depienne.

Adgang til dokumentet

10.3389/fcell.2022.1019715

Citationsformater

Parenti, I., Leitão, E., Kuechler, A., Villard, L., Goizet, C., Courdier, C., Bayat, A., Rossi, A., Julia, S., Bruel, A. L., Tran Mau-Them, F., Nambot, S., Lehalle, D., Willems, M., Lespinasse, J., Ghoumid, J., Caumes, R., Smol, T., El Chehadeh, S., ... Striano, P. (2022). The different clinical facets of SYN1-related neurodevelopmental disorders. Frontiers in Cell and Developmental Biology, 10, Artikel 1019715. https://doi.org/10.3389/fcell.2022.1019715

Parenti, I, Leitão, E, Kuechler, A, Villard, L, Goizet, C, Courdier, C, Bayat, A, Rossi, A, Julia, S, Bruel, AL, Tran Mau-Them, F, Nambot, S, Lehalle, D, Willems, M, Lespinasse, J, Ghoumid, J, Caumes, R, Smol, T, El Chehadeh, S, Schaefer, E, Abi-Warde, MT, Keren, B, Afenjar, A, Tabet, AC, Levy, J, Maruani, A, Aledo-Serrano, Á, Garming, W, Milleret-Pignot, C, Chassevent, A, Koopmans, M, Verbeek, NE, Person, R, Belles, R, Bellus, G, Salbert, BA, Kaiser, FJ, Mazzola, L, Convers, P, Perrin, L, Piton, A, Wiegand, G, Accogli, A, Brancati, F, Benfenati, F, Chatron, N, Lewis-Smith, D, Thomas, RH, Zara, F & Striano, P 2022, 'The different clinical facets of SYN1-related neurodevelopmental disorders', Frontiers in Cell and Developmental Biology, bind 10, 1019715. https://doi.org/10.3389/fcell.2022.1019715

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title = "The different clinical facets of SYN1-related neurodevelopmental disorders",

abstract = "Synapsin-I (SYN1) is a presynaptic phosphoprotein crucial for synaptogenesis and synaptic plasticity. Pathogenic SYN1 variants are associated with variable X-linked neurodevelopmental disorders mainly affecting males. In this study, we expand on the clinical and molecular spectrum of the SYN1-related neurodevelopmental disorders by describing 31 novel individuals harboring 22 different SYN1 variants. We analyzed newly identified as well as previously reported individuals in order to define the frequency of key features associated with these disorders. Specifically, behavioral disturbances such as autism spectrum disorder or attention deficit hyperactivity disorder are observed in 91% of the individuals, epilepsy in 82%, intellectual disability in 77%, and developmental delay in 70%. Seizure types mainly include tonic-clonic or focal seizures with impaired awareness. The presence of reflex seizures is one of the most representative clinical manifestations related to SYN1. In more than half of the cases, seizures are triggered by contact with water, but other triggers are also frequently reported, including rubbing with a towel, fever, toothbrushing, fingernail clipping, falling asleep, and watching others showering or bathing. We additionally describe hyperpnea, emotion, lighting, using a stroboscope, digestive troubles, and defecation as possible triggers in individuals with SYN1 variants. The molecular spectrum of SYN1 variants is broad and encompasses truncating variants (frameshift, nonsense, splicing and start-loss variants) as well as non-truncating variants (missense substitutions and in-frame duplications). Genotype-phenotype correlation revealed that epileptic phenotypes are enriched in individuals with truncating variants. Furthermore, we could show for the first time that individuals with early seizures onset tend to present with severe-to-profound intellectual disability, hence highlighting the existence of an association between early seizure onset and more severe impairment of cognitive functions. Altogether, we present a detailed clinical description of the largest series of individuals with SYN1 variants reported so far and provide the first genotype-phenotype correlations for this gene. A timely molecular diagnosis and genetic counseling are cardinal for appropriate patient management and treatment.",

keywords = "autism spectrum disorders, genotype-phenotype correlation, neurodevelopmental disorders, reflex epilepsy, SYN1, synapsins",

author = "Ilaria Parenti and Elsa Leit{\~a}o and Alma Kuechler and Laurent Villard and Cyril Goizet and C{\'e}cile Courdier and Allan Bayat and Alessandra Rossi and Sophie Julia and Bruel, {Ange Line} and {Tran Mau-Them}, Fr{\'e}d{\'e}ric and Sophie Nambot and Daphn{\'e} Lehalle and Marjolaine Willems and James Lespinasse and Jamal Ghoumid and Roseline Caumes and Thomas Smol and {El Chehadeh}, Salima and Elise Schaefer and Abi-Warde, {Marie Th{\'e}r{\`e}se} and Boris Keren and Alexandra Afenjar and Tabet, {Anne Claude} and Jonathan Levy and Anna Maruani and {\'A}ngel Aledo-Serrano and Waltraud Garming and Clara Milleret-Pignot and Anna Chassevent and Marije Koopmans and Verbeek, {Nienke E.} and Richard Person and Rebecca Belles and Gary Bellus and Salbert, {Bonnie A.} and Kaiser, {Frank J.} and Laure Mazzola and Philippe Convers and Laurine Perrin and Am{\'e}lie Piton and Gert Wiegand and Andrea Accogli and Francesco Brancati and Fabio Benfenati and Nicolas Chatron and David Lewis-Smith and Thomas, {Rhys H.} and Federico Zara and Pasquale Striano",

note = "Publisher Copyright: Copyright {\textcopyright} 2022 Parenti, Leit{\~a}o, Kuechler, Villard, Goizet, Courdier, Bayat, Rossi, Julia, Bruel, Tran Mau-Them, Nambot, Lehalle, Willems, Lespinasse, Ghoumid, Caumes, Smol, El Chehadeh, Schaefer, Abi-Warde, Keren, Afenjar, Tabet, Levy, Maruani, Aledo-Serrano, Garming, Milleret-Pignot, Chassevent, Koopmans, Verbeek, Person, Belles, Bellus, Salbert, Kaiser, Mazzola, Convers, Perrin, Piton, Wiegand, Accogli, Brancati, Benfenati, Chatron, Lewis-Smith, Thomas, Zara, Striano, Lesca and Depienne.",

year = "2022",

month = dec,

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doi = "10.3389/fcell.2022.1019715",

language = "English",

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journal = "Frontiers in Cell and Developmental Biology",

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T1 - The different clinical facets of SYN1-related neurodevelopmental disorders

AU - Parenti, Ilaria

AU - Leitão, Elsa

AU - Kuechler, Alma

AU - Villard, Laurent

AU - Goizet, Cyril

AU - Courdier, Cécile

AU - Bayat, Allan

AU - Rossi, Alessandra

AU - Julia, Sophie

AU - Bruel, Ange Line

AU - Tran Mau-Them, Frédéric

AU - Nambot, Sophie

AU - Lehalle, Daphné

AU - Willems, Marjolaine

AU - Lespinasse, James

AU - Ghoumid, Jamal

AU - Caumes, Roseline

AU - Smol, Thomas

AU - El Chehadeh, Salima

AU - Schaefer, Elise

AU - Abi-Warde, Marie Thérèse

AU - Keren, Boris

AU - Afenjar, Alexandra

AU - Tabet, Anne Claude

AU - Levy, Jonathan

AU - Maruani, Anna

AU - Aledo-Serrano, Ángel

AU - Garming, Waltraud

AU - Milleret-Pignot, Clara

AU - Chassevent, Anna

AU - Koopmans, Marije

AU - Verbeek, Nienke E.

AU - Person, Richard

AU - Belles, Rebecca

AU - Bellus, Gary

AU - Salbert, Bonnie A.

AU - Kaiser, Frank J.

AU - Mazzola, Laure

AU - Convers, Philippe

AU - Perrin, Laurine

AU - Piton, Amélie

AU - Wiegand, Gert

AU - Accogli, Andrea

AU - Brancati, Francesco

AU - Benfenati, Fabio

AU - Chatron, Nicolas

AU - Lewis-Smith, David

AU - Thomas, Rhys H.

AU - Zara, Federico

AU - Striano, Pasquale

N1 - Publisher Copyright: Copyright © 2022 Parenti, Leitão, Kuechler, Villard, Goizet, Courdier, Bayat, Rossi, Julia, Bruel, Tran Mau-Them, Nambot, Lehalle, Willems, Lespinasse, Ghoumid, Caumes, Smol, El Chehadeh, Schaefer, Abi-Warde, Keren, Afenjar, Tabet, Levy, Maruani, Aledo-Serrano, Garming, Milleret-Pignot, Chassevent, Koopmans, Verbeek, Person, Belles, Bellus, Salbert, Kaiser, Mazzola, Convers, Perrin, Piton, Wiegand, Accogli, Brancati, Benfenati, Chatron, Lewis-Smith, Thomas, Zara, Striano, Lesca and Depienne.

PY - 2022/12/8

Y1 - 2022/12/8

N2 - Synapsin-I (SYN1) is a presynaptic phosphoprotein crucial for synaptogenesis and synaptic plasticity. Pathogenic SYN1 variants are associated with variable X-linked neurodevelopmental disorders mainly affecting males. In this study, we expand on the clinical and molecular spectrum of the SYN1-related neurodevelopmental disorders by describing 31 novel individuals harboring 22 different SYN1 variants. We analyzed newly identified as well as previously reported individuals in order to define the frequency of key features associated with these disorders. Specifically, behavioral disturbances such as autism spectrum disorder or attention deficit hyperactivity disorder are observed in 91% of the individuals, epilepsy in 82%, intellectual disability in 77%, and developmental delay in 70%. Seizure types mainly include tonic-clonic or focal seizures with impaired awareness. The presence of reflex seizures is one of the most representative clinical manifestations related to SYN1. In more than half of the cases, seizures are triggered by contact with water, but other triggers are also frequently reported, including rubbing with a towel, fever, toothbrushing, fingernail clipping, falling asleep, and watching others showering or bathing. We additionally describe hyperpnea, emotion, lighting, using a stroboscope, digestive troubles, and defecation as possible triggers in individuals with SYN1 variants. The molecular spectrum of SYN1 variants is broad and encompasses truncating variants (frameshift, nonsense, splicing and start-loss variants) as well as non-truncating variants (missense substitutions and in-frame duplications). Genotype-phenotype correlation revealed that epileptic phenotypes are enriched in individuals with truncating variants. Furthermore, we could show for the first time that individuals with early seizures onset tend to present with severe-to-profound intellectual disability, hence highlighting the existence of an association between early seizure onset and more severe impairment of cognitive functions. Altogether, we present a detailed clinical description of the largest series of individuals with SYN1 variants reported so far and provide the first genotype-phenotype correlations for this gene. A timely molecular diagnosis and genetic counseling are cardinal for appropriate patient management and treatment.

AB - Synapsin-I (SYN1) is a presynaptic phosphoprotein crucial for synaptogenesis and synaptic plasticity. Pathogenic SYN1 variants are associated with variable X-linked neurodevelopmental disorders mainly affecting males. In this study, we expand on the clinical and molecular spectrum of the SYN1-related neurodevelopmental disorders by describing 31 novel individuals harboring 22 different SYN1 variants. We analyzed newly identified as well as previously reported individuals in order to define the frequency of key features associated with these disorders. Specifically, behavioral disturbances such as autism spectrum disorder or attention deficit hyperactivity disorder are observed in 91% of the individuals, epilepsy in 82%, intellectual disability in 77%, and developmental delay in 70%. Seizure types mainly include tonic-clonic or focal seizures with impaired awareness. The presence of reflex seizures is one of the most representative clinical manifestations related to SYN1. In more than half of the cases, seizures are triggered by contact with water, but other triggers are also frequently reported, including rubbing with a towel, fever, toothbrushing, fingernail clipping, falling asleep, and watching others showering or bathing. We additionally describe hyperpnea, emotion, lighting, using a stroboscope, digestive troubles, and defecation as possible triggers in individuals with SYN1 variants. The molecular spectrum of SYN1 variants is broad and encompasses truncating variants (frameshift, nonsense, splicing and start-loss variants) as well as non-truncating variants (missense substitutions and in-frame duplications). Genotype-phenotype correlation revealed that epileptic phenotypes are enriched in individuals with truncating variants. Furthermore, we could show for the first time that individuals with early seizures onset tend to present with severe-to-profound intellectual disability, hence highlighting the existence of an association between early seizure onset and more severe impairment of cognitive functions. Altogether, we present a detailed clinical description of the largest series of individuals with SYN1 variants reported so far and provide the first genotype-phenotype correlations for this gene. A timely molecular diagnosis and genetic counseling are cardinal for appropriate patient management and treatment.

KW - autism spectrum disorders

KW - genotype-phenotype correlation

KW - neurodevelopmental disorders

KW - reflex epilepsy

KW - SYN1

KW - synapsins

U2 - 10.3389/fcell.2022.1019715

DO - 10.3389/fcell.2022.1019715

M3 - Journal article

AN - SCOPUS:85144967645

SN - 2296-634X

VL - 10

JO - Frontiers in Cell and Developmental Biology

JF - Frontiers in Cell and Developmental Biology

M1 - 1019715

ER -