A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features

Diane D. Shao; Rachel Straussberg; Hind Ahmed; Amjad Khan; Songhai Tian; R. Sean Hill; Richard S. Smith; Amar J. Majmundar; Najim Ameziane; Jennifer E. Neil; Edward Yang; Amal Al Tenaiji; Saumya S. Jamuar; Thorsten M. Schlaeger; Muna Al-Saffar; Iris Hovel; Aisha Al-Shamsi; Lina Basel-Salmon; Achiya Z. Amir; Lariza M. Rento; Jiin Ying Lim; Indra Ganesan; Shirlee Shril; Gilad Evrony; A. James Barkovich; Peter Bauer; Friedhelm Hildebrandt; Min Dong; Guntram Borck; Christian Beetz; Lihadh Al-Gazali; Wafaa Eyaid; Christopher A. Walsh

doi:10.1038/s41436-021-01097-x

A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features

Diane D. Shao, Rachel Straussberg, Hind Ahmed, Amjad Khan, Songhai Tian, R. Sean Hill, Richard S. Smith, Amar J. Majmundar, Najim Ameziane, Jennifer E. Neil, Edward Yang, Amal Al Tenaiji, Saumya S. Jamuar, Thorsten M. Schlaeger, Muna Al-Saffar, Iris Hovel, Aisha Al-Shamsi, Lina Basel-Salmon, Achiya Z. Amir, Lariza M. RentoJiin Ying Lim, Indra Ganesan, Shirlee Shril, Gilad Evrony, A. James Barkovich, Peter Bauer, Friedhelm Hildebrandt, Min Dong, Guntram Borck, Christian Beetz, Lihadh Al-Gazali, Wafaa Eyaid, Christopher A. Walsh

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

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Abstract

Purpose: The endoplasmic reticulum membrane complex (EMC) is a highly conserved, multifunctional 10-protein complex related to membrane protein biology. In seven families, we identified 13 individuals with highly overlapping phenotypes who harbor a single identical homozygous frameshift variant in EMC10. Methods: Using exome, genome, and Sanger sequencing, a recurrent frameshift EMC10 variant was identified in affected individuals in an international cohort of consanguineous families. Multiple families were independently identified and connected via Matchmaker Exchange and internal databases. We assessed the effect of the frameshift variant on EMC10 RNA and protein expression and evaluated EMC10 expression in normal human brain tissue using immunohistochemistry. Results: A homozygous variant EMC10 c.287delG (Refseq NM_206538.3, p.Gly96Alafs*9) segregated with affected individuals in each family, who exhibited a phenotypic spectrum of intellectual disability (ID) and global developmental delay (GDD), variable seizures and variable dysmorphic features (elongated face, curly hair, cubitus valgus, and arachnodactyly). The variant arose on two founder haplotypes and results in significantly reduced EMC10 RNA expression and an unstable truncated EMC10 protein. Conclusion: We propose that a homozygous loss-of-function variant in EMC10 causes a novel syndromic neurodevelopmental phenotype. Remarkably, the recurrent variant is likely the result of a hypermutable site and arose on distinct founder haplotypes.

Original language	English
Pages (from-to)	1158-1162
Number of pages	5
Journal	Genetics in Medicine
Volume	23
Issue number	6
DOIs	https://doi.org/10.1038/s41436-021-01097-x
Publication status	Published - Jun 2021

ASJC Scopus subject areas

Genetics(clinical)

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10.1038/s41436-021-01097-x

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Shao, D. D., Straussberg, R., Ahmed, H., Khan, A., Tian, S., Hill, R. S., Smith, R. S., Majmundar, A. J., Ameziane, N., Neil, J. E., Yang, E., Al Tenaiji, A., Jamuar, S. S., Schlaeger, T. M., Al-Saffar, M., Hovel, I., Al-Shamsi, A., Basel-Salmon, L., Amir, A. Z., ... Walsh, C. A. (2021). A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features. Genetics in Medicine, 23(6), 1158-1162. https://doi.org/10.1038/s41436-021-01097-x

Shao, DD, Straussberg, R, Ahmed, H, Khan, A, Tian, S, Hill, RS, Smith, RS, Majmundar, AJ, Ameziane, N, Neil, JE, Yang, E, Al Tenaiji, A, Jamuar, SS, Schlaeger, TM, Al-Saffar, M, Hovel, I, Al-Shamsi, A, Basel-Salmon, L, Amir, AZ, Rento, LM, Lim, JY, Ganesan, I, Shril, S, Evrony, G, Barkovich, AJ, Bauer, P, Hildebrandt, F, Dong, M, Borck, G, Beetz, C, Al-Gazali, L, Eyaid, W & Walsh, CA 2021, 'A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features', Genetics in Medicine, vol. 23, no. 6, pp. 1158-1162. https://doi.org/10.1038/s41436-021-01097-x

@article{670802ad3e884ec6a94eae59a1cac15f,

title = "A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features",

abstract = "Purpose: The endoplasmic reticulum membrane complex (EMC) is a highly conserved, multifunctional 10-protein complex related to membrane protein biology. In seven families, we identified 13 individuals with highly overlapping phenotypes who harbor a single identical homozygous frameshift variant in EMC10. Methods: Using exome, genome, and Sanger sequencing, a recurrent frameshift EMC10 variant was identified in affected individuals in an international cohort of consanguineous families. Multiple families were independently identified and connected via Matchmaker Exchange and internal databases. We assessed the effect of the frameshift variant on EMC10 RNA and protein expression and evaluated EMC10 expression in normal human brain tissue using immunohistochemistry. Results: A homozygous variant EMC10 c.287delG (Refseq NM_206538.3, p.Gly96Alafs*9) segregated with affected individuals in each family, who exhibited a phenotypic spectrum of intellectual disability (ID) and global developmental delay (GDD), variable seizures and variable dysmorphic features (elongated face, curly hair, cubitus valgus, and arachnodactyly). The variant arose on two founder haplotypes and results in significantly reduced EMC10 RNA expression and an unstable truncated EMC10 protein. Conclusion: We propose that a homozygous loss-of-function variant in EMC10 causes a novel syndromic neurodevelopmental phenotype. Remarkably, the recurrent variant is likely the result of a hypermutable site and arose on distinct founder haplotypes.",

author = "Shao, {Diane D.} and Rachel Straussberg and Hind Ahmed and Amjad Khan and Songhai Tian and Hill, {R. Sean} and Smith, {Richard S.} and Majmundar, {Amar J.} and Najim Ameziane and Neil, {Jennifer E.} and Edward Yang and {Al Tenaiji}, Amal and Jamuar, {Saumya S.} and Schlaeger, {Thorsten M.} and Muna Al-Saffar and Iris Hovel and Aisha Al-Shamsi and Lina Basel-Salmon and Amir, {Achiya Z.} and Rento, {Lariza M.} and Lim, {Jiin Ying} and Indra Ganesan and Shirlee Shril and Gilad Evrony and Barkovich, {A. James} and Peter Bauer and Friedhelm Hildebrandt and Min Dong and Guntram Borck and Christian Beetz and Lihadh Al-Gazali and Wafaa Eyaid and Walsh, {Christopher A.}",

note = "Funding Information: C.A.W. is supported by National Institute of Neurologic Disorders and Stroke (NINDS) (RO1 35129) and is an Investigator of the Howard Hughes Medical Institute. This research was supported by the Allen Discovery Center program, a Paul G. Allen Frontiers Group advised program of the Paul G. Allen family Foundation. D.D.S. is supported by NINDS Neurology Resident Research Education Program (R25 NS070682). R.S.S. is supported by National Institute of Health (NIH) K99NS112604. A.J.M. acknowledges support from NIH Training Grant (T32DK-007726), the 2017 Postdoctoral Fellowship Grant from the Harvard Stem Cell Institute, and the American Society of Nephrology Lipps Research Program 2018 Polycystic Kidney Disease Foundation Jared J. Grantham Research Fellowship. M.D. acknowledges support from NIH (R01NS080833 and R21NS106159), the NIH-funded Harvard Digestive Disease Center (P30DK034854) and BCH Intellectual and Developmental Disabilities Research Center (P30HD18655). M. D. holds the Investigator in the Pathogenesis of Infectious Disease Award from the Burroughs Wellcome Fund. F.H. is the William E. Harmon Professor of Pediatrics and this work was supported by grants from the NIH DK-068306. Funding Information: We are sincerely indebted to the generosity of the families and patients who participated in this study. We acknowledge clinicians (names withheld) whose contributions enhanced our understanding of the patient phenotype, but who could not formally participate in this work due to geopolitical conflicts. We acknowledge Connor Kenny, who performed Sanger validation. Human postmortem brain tissue was obtained from the National Institutes of Health (NIH) Neurobiobank at the University of Maryland in Baltimore. We thank the Thomas Sudhof Laboratory at Stanford University for gifting lentiviral vectors for NGN2 transduction to the Human Neuron Core at Boston Children{\textquoteright}s Hospital (BCH). The Human Neuron Core is supported by BCH IDDRC U54HD090255 and played the key role in generation of neurons derived from induced pluripotent stem cells (iPSCs). The Yale Center for Mendelian Genomics (UM1HG006504), funded by the National Human Genome Research Institute, and the GSP Coordinating Center (U24 HG008956) provided sequencing, and logistical and general study coordination, respectively. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = jun,

doi = "10.1038/s41436-021-01097-x",

language = "English",

volume = "23",

pages = "1158--1162",

journal = "Genetics in Medicine",

issn = "1098-3600",

publisher = "Lippincott Williams and Wilkins",

number = "6",

}

TY - JOUR

T1 - A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features

AU - Shao, Diane D.

AU - Straussberg, Rachel

AU - Ahmed, Hind

AU - Khan, Amjad

AU - Tian, Songhai

AU - Hill, R. Sean

AU - Smith, Richard S.

AU - Majmundar, Amar J.

AU - Ameziane, Najim

AU - Neil, Jennifer E.

AU - Yang, Edward

AU - Al Tenaiji, Amal

AU - Jamuar, Saumya S.

AU - Schlaeger, Thorsten M.

AU - Al-Saffar, Muna

AU - Hovel, Iris

AU - Al-Shamsi, Aisha

AU - Basel-Salmon, Lina

AU - Amir, Achiya Z.

AU - Rento, Lariza M.

AU - Lim, Jiin Ying

AU - Ganesan, Indra

AU - Shril, Shirlee

AU - Evrony, Gilad

AU - Barkovich, A. James

AU - Bauer, Peter

AU - Hildebrandt, Friedhelm

AU - Dong, Min

AU - Borck, Guntram

AU - Beetz, Christian

AU - Al-Gazali, Lihadh

AU - Eyaid, Wafaa

AU - Walsh, Christopher A.

N1 - Funding Information: C.A.W. is supported by National Institute of Neurologic Disorders and Stroke (NINDS) (RO1 35129) and is an Investigator of the Howard Hughes Medical Institute. This research was supported by the Allen Discovery Center program, a Paul G. Allen Frontiers Group advised program of the Paul G. Allen family Foundation. D.D.S. is supported by NINDS Neurology Resident Research Education Program (R25 NS070682). R.S.S. is supported by National Institute of Health (NIH) K99NS112604. A.J.M. acknowledges support from NIH Training Grant (T32DK-007726), the 2017 Postdoctoral Fellowship Grant from the Harvard Stem Cell Institute, and the American Society of Nephrology Lipps Research Program 2018 Polycystic Kidney Disease Foundation Jared J. Grantham Research Fellowship. M.D. acknowledges support from NIH (R01NS080833 and R21NS106159), the NIH-funded Harvard Digestive Disease Center (P30DK034854) and BCH Intellectual and Developmental Disabilities Research Center (P30HD18655). M. D. holds the Investigator in the Pathogenesis of Infectious Disease Award from the Burroughs Wellcome Fund. F.H. is the William E. Harmon Professor of Pediatrics and this work was supported by grants from the NIH DK-068306. Funding Information: We are sincerely indebted to the generosity of the families and patients who participated in this study. We acknowledge clinicians (names withheld) whose contributions enhanced our understanding of the patient phenotype, but who could not formally participate in this work due to geopolitical conflicts. We acknowledge Connor Kenny, who performed Sanger validation. Human postmortem brain tissue was obtained from the National Institutes of Health (NIH) Neurobiobank at the University of Maryland in Baltimore. We thank the Thomas Sudhof Laboratory at Stanford University for gifting lentiviral vectors for NGN2 transduction to the Human Neuron Core at Boston Children’s Hospital (BCH). The Human Neuron Core is supported by BCH IDDRC U54HD090255 and played the key role in generation of neurons derived from induced pluripotent stem cells (iPSCs). The Yale Center for Mendelian Genomics (UM1HG006504), funded by the National Human Genome Research Institute, and the GSP Coordinating Center (U24 HG008956) provided sequencing, and logistical and general study coordination, respectively. Publisher Copyright: © 2021, The Author(s).

PY - 2021/6

Y1 - 2021/6

N2 - Purpose: The endoplasmic reticulum membrane complex (EMC) is a highly conserved, multifunctional 10-protein complex related to membrane protein biology. In seven families, we identified 13 individuals with highly overlapping phenotypes who harbor a single identical homozygous frameshift variant in EMC10. Methods: Using exome, genome, and Sanger sequencing, a recurrent frameshift EMC10 variant was identified in affected individuals in an international cohort of consanguineous families. Multiple families were independently identified and connected via Matchmaker Exchange and internal databases. We assessed the effect of the frameshift variant on EMC10 RNA and protein expression and evaluated EMC10 expression in normal human brain tissue using immunohistochemistry. Results: A homozygous variant EMC10 c.287delG (Refseq NM_206538.3, p.Gly96Alafs*9) segregated with affected individuals in each family, who exhibited a phenotypic spectrum of intellectual disability (ID) and global developmental delay (GDD), variable seizures and variable dysmorphic features (elongated face, curly hair, cubitus valgus, and arachnodactyly). The variant arose on two founder haplotypes and results in significantly reduced EMC10 RNA expression and an unstable truncated EMC10 protein. Conclusion: We propose that a homozygous loss-of-function variant in EMC10 causes a novel syndromic neurodevelopmental phenotype. Remarkably, the recurrent variant is likely the result of a hypermutable site and arose on distinct founder haplotypes.

AB - Purpose: The endoplasmic reticulum membrane complex (EMC) is a highly conserved, multifunctional 10-protein complex related to membrane protein biology. In seven families, we identified 13 individuals with highly overlapping phenotypes who harbor a single identical homozygous frameshift variant in EMC10. Methods: Using exome, genome, and Sanger sequencing, a recurrent frameshift EMC10 variant was identified in affected individuals in an international cohort of consanguineous families. Multiple families were independently identified and connected via Matchmaker Exchange and internal databases. We assessed the effect of the frameshift variant on EMC10 RNA and protein expression and evaluated EMC10 expression in normal human brain tissue using immunohistochemistry. Results: A homozygous variant EMC10 c.287delG (Refseq NM_206538.3, p.Gly96Alafs*9) segregated with affected individuals in each family, who exhibited a phenotypic spectrum of intellectual disability (ID) and global developmental delay (GDD), variable seizures and variable dysmorphic features (elongated face, curly hair, cubitus valgus, and arachnodactyly). The variant arose on two founder haplotypes and results in significantly reduced EMC10 RNA expression and an unstable truncated EMC10 protein. Conclusion: We propose that a homozygous loss-of-function variant in EMC10 causes a novel syndromic neurodevelopmental phenotype. Remarkably, the recurrent variant is likely the result of a hypermutable site and arose on distinct founder haplotypes.

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JO - Genetics in Medicine

JF - Genetics in Medicine

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ER -

A recurrent, homozygous EMC10 frameshift variant is associated with a syndrome of developmental delay with variable seizures and dysmorphic features

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