Exome analysis of Smith–Magenis-like syndrome cohort identifies de novo likely pathogenic variants

NISC Comparative Sequencing Program

doi:10.1007/s00439-017-1767-x

Exome analysis of Smith–Magenis-like syndrome cohort identifies de novo likely pathogenic variants

NISC Comparative Sequencing Program

Pediatrics - Genetics and Metabolism

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

22 Scopus citations

Abstract

Smith–Magenis syndrome (SMS), a neurodevelopmental disorder characterized by dysmorphic features, intellectual disability (ID), and sleep disturbances, results from a 17p11.2 microdeletion or a mutation in the RAI1 gene. We performed exome sequencing on 6 patients with SMS-like phenotypes but without chromosomal abnormalities or RAI1 variants. We identified pathogenic de novo variants in two cases, a nonsense variant in IQSEC2 and a missense variant in the SAND domain of DEAF1, and candidate de novo missense variants in an additional two cases. One candidate variant was located in an alpha helix of Necdin (NDN), phased to the paternally inherited allele. NDN is maternally imprinted within the 15q11.2 Prader–Willi Syndrome (PWS) region. This can help clarify NDN’s role in the PWS phenotype. No definitive pathogenic gene variants were detected in the remaining SMS-like cases, but we report our findings for future comparison. This study provides information about the inheritance pattern and recurrence risk for patients with identified variants and demonstrates clinical and genetic overlap of neurodevelopmental disorders. Identification and characterization of ID-related genes that assist in development of common developmental pathways and/or gene-networks, may inform disease mechanism and treatment strategies.

Original language	English (US)
Pages (from-to)	409-420
Number of pages	12
Journal	Human Genetics
Volume	136
Issue number	4
DOIs	https://doi.org/10.1007/s00439-017-1767-x
State	Published - Apr 1 2017

Bibliographical note

Funding Information:
We thank the SMS-like patients and their families for participating in this study. The authors appreciate the support of Settara C Chandrasekharappa, Ph.D., and the Genomics Core of the National Human Genome Research Institute, NIH. This study was partially supported by an NIH Bench to Bedside award (to ACM Smith) and by the Intramural Research Program of the National Human Genome Research Institute, NIH, Bethesda, Maryland, USA.

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© 2017, Springer-Verlag Berlin Heidelberg (outside the USA).

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title = "Exome analysis of Smith–Magenis-like syndrome cohort identifies de novo likely pathogenic variants",

abstract = "Smith–Magenis syndrome (SMS), a neurodevelopmental disorder characterized by dysmorphic features, intellectual disability (ID), and sleep disturbances, results from a 17p11.2 microdeletion or a mutation in the RAI1 gene. We performed exome sequencing on 6 patients with SMS-like phenotypes but without chromosomal abnormalities or RAI1 variants. We identified pathogenic de novo variants in two cases, a nonsense variant in IQSEC2 and a missense variant in the SAND domain of DEAF1, and candidate de novo missense variants in an additional two cases. One candidate variant was located in an alpha helix of Necdin (NDN), phased to the paternally inherited allele. NDN is maternally imprinted within the 15q11.2 Prader–Willi Syndrome (PWS) region. This can help clarify NDN{\textquoteright}s role in the PWS phenotype. No definitive pathogenic gene variants were detected in the remaining SMS-like cases, but we report our findings for future comparison. This study provides information about the inheritance pattern and recurrence risk for patients with identified variants and demonstrates clinical and genetic overlap of neurodevelopmental disorders. Identification and characterization of ID-related genes that assist in development of common developmental pathways and/or gene-networks, may inform disease mechanism and treatment strategies.",

author = "{NISC Comparative Sequencing Program} and Berger, {Seth I.} and Carla Ciccone and Simon, {Karen L.} and Malicdan, {May Christine} and Thierry Vilboux and Charles Billington and Roxanne Fischer and Introne, {Wendy J.} and Andrea Gropman and Blancato, {Jan K.} and Mullikin, {James C.} and Gahl, {William A.} and Marjan Huizing and Smith, {Ann C.M.}",

note = "Funding Information: We thank the SMS-like patients and their families for participating in this study. The authors appreciate the support of Settara C Chandrasekharappa, Ph.D., and the Genomics Core of the National Human Genome Research Institute, NIH. This study was partially supported by an NIH Bench to Bedside award (to ACM Smith) and by the Intramural Research Program of the National Human Genome Research Institute, NIH, Bethesda, Maryland, USA. Publisher Copyright: {\textcopyright} 2017, Springer-Verlag Berlin Heidelberg (outside the USA).",

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doi = "10.1007/s00439-017-1767-x",

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AU - NISC Comparative Sequencing Program

AU - Berger, Seth I.

AU - Ciccone, Carla

AU - Simon, Karen L.

AU - Malicdan, May Christine

AU - Vilboux, Thierry

AU - Billington, Charles

AU - Fischer, Roxanne

AU - Introne, Wendy J.

AU - Gropman, Andrea

AU - Blancato, Jan K.

AU - Mullikin, James C.

AU - Gahl, William A.

AU - Huizing, Marjan

AU - Smith, Ann C.M.

N1 - Funding Information: We thank the SMS-like patients and their families for participating in this study. The authors appreciate the support of Settara C Chandrasekharappa, Ph.D., and the Genomics Core of the National Human Genome Research Institute, NIH. This study was partially supported by an NIH Bench to Bedside award (to ACM Smith) and by the Intramural Research Program of the National Human Genome Research Institute, NIH, Bethesda, Maryland, USA. Publisher Copyright: © 2017, Springer-Verlag Berlin Heidelberg (outside the USA).

PY - 2017/4/1

Y1 - 2017/4/1

N2 - Smith–Magenis syndrome (SMS), a neurodevelopmental disorder characterized by dysmorphic features, intellectual disability (ID), and sleep disturbances, results from a 17p11.2 microdeletion or a mutation in the RAI1 gene. We performed exome sequencing on 6 patients with SMS-like phenotypes but without chromosomal abnormalities or RAI1 variants. We identified pathogenic de novo variants in two cases, a nonsense variant in IQSEC2 and a missense variant in the SAND domain of DEAF1, and candidate de novo missense variants in an additional two cases. One candidate variant was located in an alpha helix of Necdin (NDN), phased to the paternally inherited allele. NDN is maternally imprinted within the 15q11.2 Prader–Willi Syndrome (PWS) region. This can help clarify NDN’s role in the PWS phenotype. No definitive pathogenic gene variants were detected in the remaining SMS-like cases, but we report our findings for future comparison. This study provides information about the inheritance pattern and recurrence risk for patients with identified variants and demonstrates clinical and genetic overlap of neurodevelopmental disorders. Identification and characterization of ID-related genes that assist in development of common developmental pathways and/or gene-networks, may inform disease mechanism and treatment strategies.

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JO - Human Genetics

JF - Human Genetics

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ER -

Exome analysis of Smith–Magenis-like syndrome cohort identifies de novo likely pathogenic variants

Abstract

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