De novo variants in SNAP25 cause an early-onset developmental and epileptic encephalopathy

Care4Rare Canada Consortium

doi:https://doi.org/10.1038/s41436-020-01020-w

De novo variants in SNAP25 cause an early-onset developmental and epileptic encephalopathy

Care4Rare Canada Consortium

Research output: Contribution to journal › Article › Academic › peer-review

18 Citations (Scopus)

Abstract

Purpose: This study aims to provide a comprehensive description of the phenotypic and genotypic spectrum of SNAP25 developmental and epileptic encephalopathy (SNAP25-DEE) by reviewing newly identified and previously reported individuals. Methods: Individuals harboring heterozygous missense or loss-of-function variants in SNAP25 were assembled through collaboration with international colleagues, matchmaking platforms, and literature review. For each individual, detailed phenotyping, classification, and structural modeling of the identified variant were performed. Results: The cohort comprises 23 individuals with pathogenic or likely pathogenic de novo variants in SNAP25. Intellectual disability and early-onset epilepsy were identified as the core symptoms of SNAP25-DEE, with recurrent findings of movement disorders, cerebral visual impairment, and brain atrophy. Structural modeling for all variants predicted possible functional defects concerning SNAP25 or impaired interaction with other components of the SNARE complex. Conclusion: We provide a comprehensive description of SNAP25-DEE with intellectual disability and early-onset epilepsy mostly occurring before the age of two years. These core symptoms and additional recurrent phenotypes show an overlap to genes encoding other components or associated proteins of the SNARE complex such as STX1B, STXBP1, or VAMP2. Thus, these findings advance the concept of a group of neurodevelopmental disorders that may be termed “SNAREopathies.”

Original language	English
Pages (from-to)	653-660
Number of pages	8
Journal	Genetics in medicine
Volume	23
Issue number	4
Early online date	2020
DOIs	https://doi.org/10.1038/s41436-020-01020-w
Publication status	Published - Apr 2021

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https://doi.org/10.1038/s41436-020-01020-w

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@article{7dac605bf2d54173aa153cfb63712990,

title = "De novo variants in SNAP25 cause an early-onset developmental and epileptic encephalopathy",

abstract = "Purpose: This study aims to provide a comprehensive description of the phenotypic and genotypic spectrum of SNAP25 developmental and epileptic encephalopathy (SNAP25-DEE) by reviewing newly identified and previously reported individuals. Methods: Individuals harboring heterozygous missense or loss-of-function variants in SNAP25 were assembled through collaboration with international colleagues, matchmaking platforms, and literature review. For each individual, detailed phenotyping, classification, and structural modeling of the identified variant were performed. Results: The cohort comprises 23 individuals with pathogenic or likely pathogenic de novo variants in SNAP25. Intellectual disability and early-onset epilepsy were identified as the core symptoms of SNAP25-DEE, with recurrent findings of movement disorders, cerebral visual impairment, and brain atrophy. Structural modeling for all variants predicted possible functional defects concerning SNAP25 or impaired interaction with other components of the SNARE complex. Conclusion: We provide a comprehensive description of SNAP25-DEE with intellectual disability and early-onset epilepsy mostly occurring before the age of two years. These core symptoms and additional recurrent phenotypes show an overlap to genes encoding other components or associated proteins of the SNARE complex such as STX1B, STXBP1, or VAMP2. Thus, these findings advance the concept of a group of neurodevelopmental disorders that may be termed “SNAREopathies.”",

author = "{Care4Rare Canada Consortium} and Chiara Kl{\"o}ckner and Heinrich Sticht and Pia Zacher and Bernt Popp and Babcock, {Holly E.} and Bakker, {Dewi P.} and Katy Barwick and Bonfert, {Michaela V.} and B{\"o}nnemann, {Carsten G.} and Brilstra, {Eva H.} and Chung, {Wendy K.} and Clarke, {Angus J.} and Patrick Devine and Sandra Donkervoort and Fraser, {Jamie L.} and Jennifer Friedman and Alyssa Gates and Jamal Ghoumid and Emma Hobson and Gabriella Horvath and Jennifer Keller-Ramey and Boris Keren and Kurian, {Manju A.} and Virgina Lee and Leppig, {Kathleen A.} and Johan Lundgren and McDonald, {Marie T.} and McLaughlin, {Heather M.} and Amy McTague and Mefford, {Heather C.} and Cyril Mignot and Mikati, {Mohamad A.} and Caroline Nava and Raymond, {F. Lucy} and Sampson, {Julian R.} and Alba Sanchis-Juan and Vandana Shashi and Shieh, {Joseph T.C.} and Marwan Shinawi and Anne Slavotinek and Tommy St{\"o}dberg and Nicholas Stong and Sullivan, {Jennifer A.} and Taylor, {Ashley C.} and Toler, {Tomi L.} and {van den Boogaard}, {Marie Jos{\'e}} and {van der Crabben}, {Saskia N.} and {van Gassen}, {Koen L.I.} and {van Jaarsveld}, {Richard H.} and {Van Ziffle}, Jessica and Wadley, {Alexandrea F.}",

note = "Funding Information: We thank the patients and their families for their participation and support of this study. We especially thank Elizabeth Dellureficio for her continuous efforts to bring affected families together. Work on individual 5 was supported in part by grants from SFARI and the JPB Foundation. We thank the clinicians involved with the care of these patients including Stephen Nirmal, Alasdair Parker, and Manali Chitre, UK. A.M., K.B., and M.A.K. are funded by the National Institute for Health Research (NIHR) GOSH BRC. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health. Individual 7 was enrolled in the NIHR BioResource research study, supported by the Cambridge Biomedical Research Centre and the NIHR for the NIHR BioResource (grant number RG65966). Individual 17 was ascertained in the Duke Genome Sequencing Clinic. Funding for the Duke Genome Sequencing Clinic which is supported by the Duke University Health System. Individual V6 was enrolled in Care4Rare Canada Consortium, funded by Genome Canada, Ontario Genomics Institute (OGI-147), Canadian Institutes of Health Research, Ontario Research Fund, Genome Alberta, Genome British Columbia, BC Children{\textquoteright}s Hospital Foundation, BC Children{\textquoteright}s Hospital Research Institute, BC Provincial Health Services Authority, Genome Quebec, and Children{\textquoteright}s Hospital of Eastern Ontario Foundation. This study makes use of data generated by the DECIPHER Consortium. A full list of centers who contributed to the generation of the data is available from https://decipher.sanger.ac.uk/ and via email from decipher@sanger.ac.uk. Funding for the project was provided by the Wellcome Trust. R.S.M. was supported by a grant from the Lundbeck Foundation (R277-2018-802). Funding for the Duke Genome Sequencing Clinic was provided by Duke University Health System. Research reported in this publication was supported by the National Human Genome Research Institute of the National Institutes of Health under award number U01HG009599. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. We thank Katherine R. Chao for her help with the exome data analysis. The work in C.G. B{\"o}nnemann{\textquoteright}s laboratory is supported by intramural funds from the NIH National Institute of Neurological Disorders and Stroke. Sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute grant UM1 HG008900 to Daniel MacArthur and Heidi Rehm. Publisher Copyright: {\textcopyright} 2020, American College of Medical Genetics and Genomics.",

year = "2021",

month = apr,

doi = "https://doi.org/10.1038/s41436-020-01020-w",

language = "English",

volume = "23",

pages = "653--660",

journal = "Genetics in medicine",

issn = "1098-3600",

publisher = "Lippincott Williams and Wilkins",

number = "4",

}

TY - JOUR

T1 - De novo variants in SNAP25 cause an early-onset developmental and epileptic encephalopathy

AU - Care4Rare Canada Consortium

AU - Klöckner, Chiara

AU - Sticht, Heinrich

AU - Zacher, Pia

AU - Popp, Bernt

AU - Babcock, Holly E.

AU - Bakker, Dewi P.

AU - Barwick, Katy

AU - Bonfert, Michaela V.

AU - Bönnemann, Carsten G.

AU - Brilstra, Eva H.

AU - Chung, Wendy K.

AU - Clarke, Angus J.

AU - Devine, Patrick

AU - Donkervoort, Sandra

AU - Fraser, Jamie L.

AU - Friedman, Jennifer

AU - Gates, Alyssa

AU - Ghoumid, Jamal

AU - Hobson, Emma

AU - Horvath, Gabriella

AU - Keller-Ramey, Jennifer

AU - Keren, Boris

AU - Kurian, Manju A.

AU - Lee, Virgina

AU - Leppig, Kathleen A.

AU - Lundgren, Johan

AU - McDonald, Marie T.

AU - McLaughlin, Heather M.

AU - McTague, Amy

AU - Mefford, Heather C.

AU - Mignot, Cyril

AU - Mikati, Mohamad A.

AU - Nava, Caroline

AU - Raymond, F. Lucy

AU - Sampson, Julian R.

AU - Sanchis-Juan, Alba

AU - Shashi, Vandana

AU - Shieh, Joseph T.C.

AU - Shinawi, Marwan

AU - Slavotinek, Anne

AU - Stödberg, Tommy

AU - Stong, Nicholas

AU - Sullivan, Jennifer A.

AU - Taylor, Ashley C.

AU - Toler, Tomi L.

AU - van den Boogaard, Marie José

AU - van der Crabben, Saskia N.

AU - van Gassen, Koen L.I.

AU - van Jaarsveld, Richard H.

AU - Van Ziffle, Jessica

AU - Wadley, Alexandrea F.

N1 - Funding Information: We thank the patients and their families for their participation and support of this study. We especially thank Elizabeth Dellureficio for her continuous efforts to bring affected families together. Work on individual 5 was supported in part by grants from SFARI and the JPB Foundation. We thank the clinicians involved with the care of these patients including Stephen Nirmal, Alasdair Parker, and Manali Chitre, UK. A.M., K.B., and M.A.K. are funded by the National Institute for Health Research (NIHR) GOSH BRC. The views expressed are those of the author(s) and not necessarily those of the NHS, the NIHR or the Department of Health. Individual 7 was enrolled in the NIHR BioResource research study, supported by the Cambridge Biomedical Research Centre and the NIHR for the NIHR BioResource (grant number RG65966). Individual 17 was ascertained in the Duke Genome Sequencing Clinic. Funding for the Duke Genome Sequencing Clinic which is supported by the Duke University Health System. Individual V6 was enrolled in Care4Rare Canada Consortium, funded by Genome Canada, Ontario Genomics Institute (OGI-147), Canadian Institutes of Health Research, Ontario Research Fund, Genome Alberta, Genome British Columbia, BC Children’s Hospital Foundation, BC Children’s Hospital Research Institute, BC Provincial Health Services Authority, Genome Quebec, and Children’s Hospital of Eastern Ontario Foundation. This study makes use of data generated by the DECIPHER Consortium. A full list of centers who contributed to the generation of the data is available from https://decipher.sanger.ac.uk/ and via email from decipher@sanger.ac.uk. Funding for the project was provided by the Wellcome Trust. R.S.M. was supported by a grant from the Lundbeck Foundation (R277-2018-802). Funding for the Duke Genome Sequencing Clinic was provided by Duke University Health System. Research reported in this publication was supported by the National Human Genome Research Institute of the National Institutes of Health under award number U01HG009599. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. We thank Katherine R. Chao for her help with the exome data analysis. The work in C.G. Bönnemann’s laboratory is supported by intramural funds from the NIH National Institute of Neurological Disorders and Stroke. Sequencing and analysis were provided by the Broad Institute of MIT and Harvard Center for Mendelian Genomics (Broad CMG) and was funded by the National Human Genome Research Institute, the National Eye Institute, and the National Heart, Lung and Blood Institute grant UM1 HG008900 to Daniel MacArthur and Heidi Rehm. Publisher Copyright: © 2020, American College of Medical Genetics and Genomics.

PY - 2021/4

Y1 - 2021/4

N2 - Purpose: This study aims to provide a comprehensive description of the phenotypic and genotypic spectrum of SNAP25 developmental and epileptic encephalopathy (SNAP25-DEE) by reviewing newly identified and previously reported individuals. Methods: Individuals harboring heterozygous missense or loss-of-function variants in SNAP25 were assembled through collaboration with international colleagues, matchmaking platforms, and literature review. For each individual, detailed phenotyping, classification, and structural modeling of the identified variant were performed. Results: The cohort comprises 23 individuals with pathogenic or likely pathogenic de novo variants in SNAP25. Intellectual disability and early-onset epilepsy were identified as the core symptoms of SNAP25-DEE, with recurrent findings of movement disorders, cerebral visual impairment, and brain atrophy. Structural modeling for all variants predicted possible functional defects concerning SNAP25 or impaired interaction with other components of the SNARE complex. Conclusion: We provide a comprehensive description of SNAP25-DEE with intellectual disability and early-onset epilepsy mostly occurring before the age of two years. These core symptoms and additional recurrent phenotypes show an overlap to genes encoding other components or associated proteins of the SNARE complex such as STX1B, STXBP1, or VAMP2. Thus, these findings advance the concept of a group of neurodevelopmental disorders that may be termed “SNAREopathies.”

AB - Purpose: This study aims to provide a comprehensive description of the phenotypic and genotypic spectrum of SNAP25 developmental and epileptic encephalopathy (SNAP25-DEE) by reviewing newly identified and previously reported individuals. Methods: Individuals harboring heterozygous missense or loss-of-function variants in SNAP25 were assembled through collaboration with international colleagues, matchmaking platforms, and literature review. For each individual, detailed phenotyping, classification, and structural modeling of the identified variant were performed. Results: The cohort comprises 23 individuals with pathogenic or likely pathogenic de novo variants in SNAP25. Intellectual disability and early-onset epilepsy were identified as the core symptoms of SNAP25-DEE, with recurrent findings of movement disorders, cerebral visual impairment, and brain atrophy. Structural modeling for all variants predicted possible functional defects concerning SNAP25 or impaired interaction with other components of the SNARE complex. Conclusion: We provide a comprehensive description of SNAP25-DEE with intellectual disability and early-onset epilepsy mostly occurring before the age of two years. These core symptoms and additional recurrent phenotypes show an overlap to genes encoding other components or associated proteins of the SNARE complex such as STX1B, STXBP1, or VAMP2. Thus, these findings advance the concept of a group of neurodevelopmental disorders that may be termed “SNAREopathies.”

UR - http://www.scopus.com/inward/record.url?scp=85097436058&partnerID=8YFLogxK

U2 - https://doi.org/10.1038/s41436-020-01020-w

DO - https://doi.org/10.1038/s41436-020-01020-w

M3 - Article

C2 - 33299146

SN - 1098-3600

VL - 23

SP - 653

EP - 660

JO - Genetics in medicine

JF - Genetics in medicine

IS - 4

ER -

De novo variants in SNAP25 cause an early-onset developmental and epileptic encephalopathy

Abstract

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