Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder

Holly Melland; Fabian Bumbak; Anna Kolesnik-Taylor; Elise Ng-Cordell; Abinayah John; Panayiotis Constantinou; Shelagh Joss; Martin Larsen; Christina Fagerberg; Lone Walentin Laulund; Jenny Thies; Frances Emslie; Marjolein Willemsen; Tjitske Kleefstra; Rolf Pfundt; Rebekah Barrick; Richard Chang; Lucy Loong; Majid Alfadhel; Jasper van der Smagt; Mathilde Nizon; Manju Kurian; Daniel J Scott; Joshua J Ziarek; Sarah L Gordon; Kate Baker

doi:10.1016/j.gim.2021.12.002

Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder

Holly Melland, Fabian Bumbak, Anna Kolesnik-Taylor, Elise Ng-Cordell, Abinayah John, Panayiotis Constantinou, Shelagh Joss, Martin Larsen, Christina Fagerberg, Lone Walentin Laulund, Jenny Thies, Frances Emslie, Marjolein Willemsen, Tjitske Kleefstra, Rolf Pfundt, Rebekah Barrick, Richard Chang, Lucy Loong, Majid Alfadhel, Jasper van der SmagtMathilde Nizon, Manju Kurian, Daniel J Scott, Joshua J Ziarek, Sarah L Gordon, Kate Baker^*

^*Kontaktforfatter

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

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Abstract

PURPOSE: Synaptotagmin-1 (SYT1) is a critical mediator of neurotransmitter release in the central nervous system. Previously reported missense SYT1 variants in the C2B domain are associated with severe intellectual disability, movement disorders, behavioral disturbances, and electroencephalogram abnormalities. In this study, we expand the genotypes and phenotypes and identify discriminating features of this disorder.

METHODS: We describe 22 individuals with 15 de novo missense SYT1 variants. The evidence for pathogenicity is discussed, including the American College of Medical Genetics and Genomics/Association for Molecular Pathology criteria, known structure-function relationships, and molecular dynamics simulations. Quantitative behavioral data for 14 cases were compared with other monogenic neurodevelopmental disorders.

RESULTS: Four variants were located in the C2A domain with the remainder in the C2B domain. We classified 6 variants as pathogenic, 4 as likely pathogenic, and 5 as variants of uncertain significance. Prevalent clinical phenotypes included delayed developmental milestones, abnormal eye physiology, movement disorders, and sleep disturbances. Discriminating behavioral characteristics were severity of motor and communication impairment, presence of motor stereotypies, and mood instability.

CONCLUSION: Neurodevelopmental disorder-associated SYT1 variants extend beyond previously reported regions, and the phenotypic spectrum encompasses a broader range of severities than initially reported. This study guides the diagnosis and molecular understanding of this rare neurodevelopmental disorder and highlights a key role for SYT1 function in emotional regulation, motor control, and emergent cognitive function.

Originalsprog	Engelsk
Tidsskrift	Genetics in Medicine
Vol/bind	24
Udgave nummer	4
Sider (fra-til)	880-893
ISSN	1098-3600
DOI	https://doi.org/10.1016/j.gim.2021.12.002
Status	Udgivet - apr. 2022

Bibliografisk note

Dokumenter og links

10.1016/j.gim.2021.12.002Licens: CC BY

Open access versionForlagets udgivne version, 1,91 MBLicens: CC BY

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Tjek adgangen til materialet i Syddansk Universitetsbiblioteks søgemaskine

Citationsformater

Melland, H., Bumbak, F., Kolesnik-Taylor, A., Ng-Cordell, E., John, A., Constantinou, P., Joss, S., Larsen, M., Fagerberg, C., Laulund, L. W., Thies, J., Emslie, F., Willemsen, M., Kleefstra, T., Pfundt, R., Barrick, R., Chang, R., Loong, L., Alfadhel, M., ... Baker, K. (2022). Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder. Genetics in Medicine, 24(4), 880-893. https://doi.org/10.1016/j.gim.2021.12.002

@article{86a56958854348cb8dc52b9c3b64a4a5,

title = "Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder",

abstract = "PURPOSE: Synaptotagmin-1 (SYT1) is a critical mediator of neurotransmitter release in the central nervous system. Previously reported missense SYT1 variants in the C2B domain are associated with severe intellectual disability, movement disorders, behavioral disturbances, and electroencephalogram abnormalities. In this study, we expand the genotypes and phenotypes and identify discriminating features of this disorder.METHODS: We describe 22 individuals with 15 de novo missense SYT1 variants. The evidence for pathogenicity is discussed, including the American College of Medical Genetics and Genomics/Association for Molecular Pathology criteria, known structure-function relationships, and molecular dynamics simulations. Quantitative behavioral data for 14 cases were compared with other monogenic neurodevelopmental disorders.RESULTS: Four variants were located in the C2A domain with the remainder in the C2B domain. We classified 6 variants as pathogenic, 4 as likely pathogenic, and 5 as variants of uncertain significance. Prevalent clinical phenotypes included delayed developmental milestones, abnormal eye physiology, movement disorders, and sleep disturbances. Discriminating behavioral characteristics were severity of motor and communication impairment, presence of motor stereotypies, and mood instability.CONCLUSION: Neurodevelopmental disorder-associated SYT1 variants extend beyond previously reported regions, and the phenotypic spectrum encompasses a broader range of severities than initially reported. This study guides the diagnosis and molecular understanding of this rare neurodevelopmental disorder and highlights a key role for SYT1 function in emotional regulation, motor control, and emergent cognitive function.",

keywords = "Intellectual disability, Neurotransmission, Synapse, Synaptic vesicle, Synaptotagmin, Movement Disorders/genetics, Humans, Genotype, Calcium/metabolism, Intellectual Disability/genetics, Phenotype, Neurodevelopmental Disorders/genetics, Synaptotagmin I/genetics",

author = "Holly Melland and Fabian Bumbak and Anna Kolesnik-Taylor and Elise Ng-Cordell and Abinayah John and Panayiotis Constantinou and Shelagh Joss and Martin Larsen and Christina Fagerberg and Laulund, \{Lone Walentin\} and Jenny Thies and Frances Emslie and Marjolein Willemsen and Tjitske Kleefstra and Rolf Pfundt and Rebekah Barrick and Richard Chang and Lucy Loong and Majid Alfadhel and \{van der Smagt\}, Jasper and Mathilde Nizon and Manju Kurian and Scott, \{Daniel J\} and Ziarek, \{Joshua J\} and Gordon, \{Sarah L\} and Kate Baker",

year = "2022",

month = apr,

doi = "10.1016/j.gim.2021.12.002",

language = "English",

volume = "24",

pages = "880--893",

journal = "Genetics in Medicine",

issn = "1098-3600",

publisher = "Elsevier",

number = "4",

}

Melland, H, Bumbak, F, Kolesnik-Taylor, A, Ng-Cordell, E, John, A, Constantinou, P, Joss, S, Larsen, M , Fagerberg, C, Laulund, LW, Thies, J, Emslie, F, Willemsen, M, Kleefstra, T, Pfundt, R, Barrick, R, Chang, R, Loong, L, Alfadhel, M, van der Smagt, J, Nizon, M, Kurian, M, Scott, DJ, Ziarek, JJ, Gordon, SL & Baker, K 2022, 'Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder', Genetics in Medicine, bind 24, nr. 4, s. 880-893. https://doi.org/10.1016/j.gim.2021.12.002

TY - JOUR

T1 - Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder

AU - Melland, Holly

AU - Bumbak, Fabian

AU - Kolesnik-Taylor, Anna

AU - Ng-Cordell, Elise

AU - John, Abinayah

AU - Constantinou, Panayiotis

AU - Joss, Shelagh

AU - Larsen, Martin

AU - Fagerberg, Christina

AU - Laulund, Lone Walentin

AU - Thies, Jenny

AU - Emslie, Frances

AU - Willemsen, Marjolein

AU - Kleefstra, Tjitske

AU - Pfundt, Rolf

AU - Barrick, Rebekah

AU - Chang, Richard

AU - Loong, Lucy

AU - Alfadhel, Majid

AU - van der Smagt, Jasper

AU - Nizon, Mathilde

AU - Kurian, Manju

AU - Scott, Daniel J

AU - Ziarek, Joshua J

AU - Gordon, Sarah L

AU - Baker, Kate

PY - 2022/4

Y1 - 2022/4

N2 - PURPOSE: Synaptotagmin-1 (SYT1) is a critical mediator of neurotransmitter release in the central nervous system. Previously reported missense SYT1 variants in the C2B domain are associated with severe intellectual disability, movement disorders, behavioral disturbances, and electroencephalogram abnormalities. In this study, we expand the genotypes and phenotypes and identify discriminating features of this disorder.METHODS: We describe 22 individuals with 15 de novo missense SYT1 variants. The evidence for pathogenicity is discussed, including the American College of Medical Genetics and Genomics/Association for Molecular Pathology criteria, known structure-function relationships, and molecular dynamics simulations. Quantitative behavioral data for 14 cases were compared with other monogenic neurodevelopmental disorders.RESULTS: Four variants were located in the C2A domain with the remainder in the C2B domain. We classified 6 variants as pathogenic, 4 as likely pathogenic, and 5 as variants of uncertain significance. Prevalent clinical phenotypes included delayed developmental milestones, abnormal eye physiology, movement disorders, and sleep disturbances. Discriminating behavioral characteristics were severity of motor and communication impairment, presence of motor stereotypies, and mood instability.CONCLUSION: Neurodevelopmental disorder-associated SYT1 variants extend beyond previously reported regions, and the phenotypic spectrum encompasses a broader range of severities than initially reported. This study guides the diagnosis and molecular understanding of this rare neurodevelopmental disorder and highlights a key role for SYT1 function in emotional regulation, motor control, and emergent cognitive function.

AB - PURPOSE: Synaptotagmin-1 (SYT1) is a critical mediator of neurotransmitter release in the central nervous system. Previously reported missense SYT1 variants in the C2B domain are associated with severe intellectual disability, movement disorders, behavioral disturbances, and electroencephalogram abnormalities. In this study, we expand the genotypes and phenotypes and identify discriminating features of this disorder.METHODS: We describe 22 individuals with 15 de novo missense SYT1 variants. The evidence for pathogenicity is discussed, including the American College of Medical Genetics and Genomics/Association for Molecular Pathology criteria, known structure-function relationships, and molecular dynamics simulations. Quantitative behavioral data for 14 cases were compared with other monogenic neurodevelopmental disorders.RESULTS: Four variants were located in the C2A domain with the remainder in the C2B domain. We classified 6 variants as pathogenic, 4 as likely pathogenic, and 5 as variants of uncertain significance. Prevalent clinical phenotypes included delayed developmental milestones, abnormal eye physiology, movement disorders, and sleep disturbances. Discriminating behavioral characteristics were severity of motor and communication impairment, presence of motor stereotypies, and mood instability.CONCLUSION: Neurodevelopmental disorder-associated SYT1 variants extend beyond previously reported regions, and the phenotypic spectrum encompasses a broader range of severities than initially reported. This study guides the diagnosis and molecular understanding of this rare neurodevelopmental disorder and highlights a key role for SYT1 function in emotional regulation, motor control, and emergent cognitive function.

KW - Intellectual disability

KW - Neurotransmission

KW - Synapse

KW - Synaptic vesicle

KW - Synaptotagmin

KW - Movement Disorders/genetics

KW - Humans

KW - Genotype

KW - Calcium/metabolism

KW - Intellectual Disability/genetics

KW - Phenotype

KW - Neurodevelopmental Disorders/genetics

KW - Synaptotagmin I/genetics

U2 - 10.1016/j.gim.2021.12.002

DO - 10.1016/j.gim.2021.12.002

M3 - Journal article

C2 - 35101335

SN - 1098-3600

VL - 24

SP - 880

EP - 893

JO - Genetics in Medicine

JF - Genetics in Medicine

IS - 4

ER -

Expanding the genotype and phenotype spectrum of SYT1-associated neurodevelopmental disorder

Abstract

Bibliografisk note

Dokumenter og links

SDU link

Fingeraftryk

Citationsformater