De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder

Lot Snijders Blok; Susan M Hiatt; Kevin M Bowling; Jeremy W Prokop; Krysta L Engel; J Nicholas Cochran; E Martina Bebin; Emilia K Bijlsma; Claudia A L Ruivenkamp; Paulien Terhal; Marleen E H Simon; Rosemarie Smith; Jane A Hurst; Heather McLaughlin; Richard Person; Amy Crunk; Michael F Wangler; Haley Streff; Joseph D Symonds; Sameer M Zuberi; Katherine S Elliott; Victoria R Sanders; Abigail Masunga; Robert J Hopkin; Holly A Dubbs; Xilma R Ortiz-Gonzalez; Rolph Pfundt; Han G Brunner; Simon E Fisher; Tjitske Kleefstra; Gregory M Cooper

doi:10.1007/s00439-018-1887-y

De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder

Lot Snijders Blok, Susan M Hiatt, Kevin M Bowling, Jeremy W Prokop, Krysta L Engel, J Nicholas Cochran, E Martina Bebin, Emilia K Bijlsma, Claudia A L Ruivenkamp, Paulien Terhal, Marleen E H Simon, Rosemarie Smith, Jane A Hurst, Heather McLaughlin, Richard Person, Amy Crunk, Michael F Wangler, Haley Streff, Joseph D Symonds, Sameer M ZuberiKatherine S Elliott, Victoria R Sanders, Abigail Masunga, Robert J Hopkin, Holly A Dubbs, Xilma R Ortiz-Gonzalez, Rolph Pfundt, Han G Brunner, Simon E Fisher, Tjitske Kleefstra, Gregory M Cooper^*,

^*Corresponding author for this work

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

Abstract

Many genetic causes of developmental delay and/or intellectual disability (DD/ID) are extremely rare, and robust discovery of these requires both large-scale DNA sequencing and data sharing. Here we describe a GeneMatcher collaboration which led to a cohort of 13 affected individuals harboring protein-altering variants, 11 of which are de novo, in MED13; the only inherited variant was transmitted to an affected child from an affected mother. All patients had intellectual disability and/or developmental delays, including speech delays or disorders. Other features that were reported in two or more patients include autism spectrum disorder, attention deficit hyperactivity disorder, optic nerve abnormalities, Duane anomaly, hypotonia, mild congenital heart abnormalities, and dysmorphisms. Six affected individuals had mutations that are predicted to truncate the MED13 protein, six had missense mutations, and one had an in-frame-deletion of one amino acid. Out of the seven non-truncating mutations, six clustered in two specific locations of the MED13 protein: an N-terminal and C-terminal region. The four N-terminal clustering mutations affect two adjacent amino acids that are known to be involved in MED13 ubiquitination and degradation, p.Thr326 and p.Pro327. MED13 is a component of the CDK8-kinase module that can reversibly bind Mediator, a multi-protein complex that is required for Polymerase II transcription initiation. Mutations in several other genes encoding subunits of Mediator have been previously shown to associate with DD/ID, including MED13L, a paralog of MED13. Thus, our findings add MED13 to the group of CDK8-kinase module-associated disease genes.

Original language	English
Pages (from-to)	375-388
Number of pages	14
Journal	Human Genetics
Volume	137
Issue number	5
Early online date	2018
DOIs	https://doi.org/10.1007/s00439-018-1887-y
Publication status	Published - 1 May 2018

Keywords

Journal Article
Amino Acid Sequence
Sequence Deletion
Humans
Child, Preschool
Male
United Kingdom
Mutation, Missense
Cyclin-Dependent Kinase 8/genetics
Ubiquitination/genetics
Adult
Female
Mediator Complex/genetics
Transcription Initiation, Genetic
Child
Neurodevelopmental Disorders/genetics

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Snijders Blok, L., Hiatt, S. M., Bowling, K. M., Prokop, J. W., Engel, K. L., Cochran, J. N., Bebin, E. M., Bijlsma, E. K., Ruivenkamp, C. A. L., Terhal, P., Simon, M. E. H., Smith, R., Hurst, J. A., McLaughlin, H., Person, R., Crunk, A., Wangler, M. F., Streff, H., Symonds, J. D. (2018). De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder. Human Genetics, 137(5), 375-388. https://doi.org/10.1007/s00439-018-1887-y

@article{e43e64879ef84833be9641059724eac8,

title = "De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder",

abstract = "Many genetic causes of developmental delay and/or intellectual disability (DD/ID) are extremely rare, and robust discovery of these requires both large-scale DNA sequencing and data sharing. Here we describe a GeneMatcher collaboration which led to a cohort of 13 affected individuals harboring protein-altering variants, 11 of which are de novo, in MED13; the only inherited variant was transmitted to an affected child from an affected mother. All patients had intellectual disability and/or developmental delays, including speech delays or disorders. Other features that were reported in two or more patients include autism spectrum disorder, attention deficit hyperactivity disorder, optic nerve abnormalities, Duane anomaly, hypotonia, mild congenital heart abnormalities, and dysmorphisms. Six affected individuals had mutations that are predicted to truncate the MED13 protein, six had missense mutations, and one had an in-frame-deletion of one amino acid. Out of the seven non-truncating mutations, six clustered in two specific locations of the MED13 protein: an N-terminal and C-terminal region. The four N-terminal clustering mutations affect two adjacent amino acids that are known to be involved in MED13 ubiquitination and degradation, p.Thr326 and p.Pro327. MED13 is a component of the CDK8-kinase module that can reversibly bind Mediator, a multi-protein complex that is required for Polymerase II transcription initiation. Mutations in several other genes encoding subunits of Mediator have been previously shown to associate with DD/ID, including MED13L, a paralog of MED13. Thus, our findings add MED13 to the group of CDK8-kinase module-associated disease genes.",

keywords = "Journal Article, Amino Acid Sequence, Sequence Deletion, Humans, Child, Preschool, Male, United Kingdom, Mutation, Missense, Cyclin-Dependent Kinase 8/genetics, Ubiquitination/genetics, Adult, Female, Mediator Complex/genetics, Transcription Initiation, Genetic, Child, Neurodevelopmental Disorders/genetics",

author = "{Snijders Blok}, Lot and Hiatt, {Susan M} and Bowling, {Kevin M} and Prokop, {Jeremy W} and Engel, {Krysta L} and Cochran, {J Nicholas} and Bebin, {E Martina} and Bijlsma, {Emilia K} and Ruivenkamp, {Claudia A L} and Paulien Terhal and Simon, {Marleen E H} and Rosemarie Smith and Hurst, {Jane A} and Heather McLaughlin and Richard Person and Amy Crunk and Wangler, {Michael F} and Haley Streff and Symonds, {Joseph D} and Zuberi, {Sameer M} and Elliott, {Katherine S} and Sanders, {Victoria R} and Abigail Masunga and Hopkin, {Robert J} and Dubbs, {Holly A} and Ortiz-Gonzalez, {Xilma R} and Rolph Pfundt and Brunner, {Han G} and Fisher, {Simon E} and Tjitske Kleefstra and Cooper, {Gregory M}",

note = "Funding Information: We thank all patients and families for their contributions. This work was supported by the Max Planck Society (S.E.F.), a grant from the US National Human Genome Research Institute (NHGRI; UM1HG007301) (S.M.H., K.M.B., J.N.C., K.L.E., E.M.B., G.M.C.), and the Netherlands Organisation for Scientific Research (NWO) Gravitation Grant 24.001.006 to the Language in Interaction Consortium (L.S.B., H.G.B., S.E.F.). Patient L was part of the DDD study cohort (DECIPHER ID: DDD263479). The DDD study presents independent research commissioned by the Health Innovation Challenge Fund [grant number HICF-1009-003], a parallel funding partnership between the Wellcome Trust and the Department of Health, and the Wellcome Trust Sanger Institute [grant number WT098051]. The views expressed in this publication are those of the author(s) and not necessarily those of the Wellcome Trust or the Department of Health. The study has UK Research Ethics Committee approval (10/H0305/83, granted by the Cambridge South REC, and GEN/284/12 granted by the Republic of Ireland REC). The research team acknowledges the support of the National Institute for Health Research, through the Comprehensive Clinical Research Network. This study makes use of DECIPHER (http://decipher.sanger.ac.uk), which is funded by the Wellcome Trust. H.M., R.P. and A.C. are employees of GeneDx, Inc., a wholly owned subsidiary of OPKO Health, Inc. The other authors declare no conflict of interest. Funding Information: Acknowledgements We thank all patients and families for their contributions. This work was supported by the Max Planck Society (S.E.F.), a grant from the US National Human Genome Research Institute (NHGRI; UM1HG007301) (S.M.H., K.M.B., J.N.C., K.L.E., E.M.B., G.M.C.), and the Netherlands Organisation for Scientific Research (NWO) Gravitation Grant 24.001.006 to the Language in Interaction Consortium (L.S.B., H.G.B., S.E.F.). Patient L was part of the DDD study cohort (DECIPHER ID: DDD263479). The DDD study presents independent research commissioned by the Health Innovation Challenge Fund [grant number HICF-1009-003], a parallel funding partnership between the Wellcome Trust and the Department of Health, and the Wellcome Trust Sanger Institute [grant number WT098051]. The views expressed in this publication are those of the author(s) and not necessarily those of the Wellcome Trust or the Department of Health. The study has UK Research Ethics Committee approval (10/H0305/83, granted by the Cambridge South REC, and GEN/284/12 granted by the Republic of Ireland REC). The research team acknowledges the support of the National Institute for Health Research, through the Comprehensive Clinical Research Network. This study makes use of DECIPHER (http://decipher.sanger.ac.uk), which is funded by the Wellcome Trust. Publisher Copyright: {\textcopyright} 2018, The Author(s).",

year = "2018",

month = may,

day = "1",

doi = "10.1007/s00439-018-1887-y",

language = "English",

volume = "137",

pages = "375--388",

journal = "Human Genetics",

issn = "0340-6717",

publisher = "Springer-Verlag",

number = "5",

}

Snijders Blok, L, Hiatt, SM, Bowling, KM, Prokop, JW, Engel, KL, Cochran, JN, Bebin, EM, Bijlsma, EK, Ruivenkamp, CAL, Terhal, P, Simon, MEH, Smith, R, Hurst, JA, McLaughlin, H, Person, R, Crunk, A, Wangler, MF, Streff, H, Symonds, JD, Zuberi, SM, Elliott, KS, Sanders, VR, Masunga, A, Hopkin, RJ, Dubbs, HA, Ortiz-Gonzalez, XR, Pfundt, R, Brunner, HG, Fisher, SE, Kleefstra, T, Cooper, GM 2018, 'De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder', Human Genetics, vol. 137, no. 5, pp. 375-388. https://doi.org/10.1007/s00439-018-1887-y

TY - JOUR

T1 - De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder

AU - Snijders Blok, Lot

AU - Hiatt, Susan M

AU - Bowling, Kevin M

AU - Prokop, Jeremy W

AU - Engel, Krysta L

AU - Cochran, J Nicholas

AU - Bebin, E Martina

AU - Bijlsma, Emilia K

AU - Ruivenkamp, Claudia A L

AU - Terhal, Paulien

AU - Simon, Marleen E H

AU - Smith, Rosemarie

AU - Hurst, Jane A

AU - McLaughlin, Heather

AU - Person, Richard

AU - Crunk, Amy

AU - Wangler, Michael F

AU - Streff, Haley

AU - Symonds, Joseph D

AU - Zuberi, Sameer M

AU - Elliott, Katherine S

AU - Sanders, Victoria R

AU - Masunga, Abigail

AU - Hopkin, Robert J

AU - Dubbs, Holly A

AU - Ortiz-Gonzalez, Xilma R

AU - Pfundt, Rolph

AU - Brunner, Han G

AU - Fisher, Simon E

AU - Kleefstra, Tjitske

AU - Cooper, Gregory M

N1 - Funding Information: We thank all patients and families for their contributions. This work was supported by the Max Planck Society (S.E.F.), a grant from the US National Human Genome Research Institute (NHGRI; UM1HG007301) (S.M.H., K.M.B., J.N.C., K.L.E., E.M.B., G.M.C.), and the Netherlands Organisation for Scientific Research (NWO) Gravitation Grant 24.001.006 to the Language in Interaction Consortium (L.S.B., H.G.B., S.E.F.). Patient L was part of the DDD study cohort (DECIPHER ID: DDD263479). The DDD study presents independent research commissioned by the Health Innovation Challenge Fund [grant number HICF-1009-003], a parallel funding partnership between the Wellcome Trust and the Department of Health, and the Wellcome Trust Sanger Institute [grant number WT098051]. The views expressed in this publication are those of the author(s) and not necessarily those of the Wellcome Trust or the Department of Health. The study has UK Research Ethics Committee approval (10/H0305/83, granted by the Cambridge South REC, and GEN/284/12 granted by the Republic of Ireland REC). The research team acknowledges the support of the National Institute for Health Research, through the Comprehensive Clinical Research Network. This study makes use of DECIPHER (http://decipher.sanger.ac.uk), which is funded by the Wellcome Trust. H.M., R.P. and A.C. are employees of GeneDx, Inc., a wholly owned subsidiary of OPKO Health, Inc. The other authors declare no conflict of interest. Funding Information: Acknowledgements We thank all patients and families for their contributions. This work was supported by the Max Planck Society (S.E.F.), a grant from the US National Human Genome Research Institute (NHGRI; UM1HG007301) (S.M.H., K.M.B., J.N.C., K.L.E., E.M.B., G.M.C.), and the Netherlands Organisation for Scientific Research (NWO) Gravitation Grant 24.001.006 to the Language in Interaction Consortium (L.S.B., H.G.B., S.E.F.). Patient L was part of the DDD study cohort (DECIPHER ID: DDD263479). The DDD study presents independent research commissioned by the Health Innovation Challenge Fund [grant number HICF-1009-003], a parallel funding partnership between the Wellcome Trust and the Department of Health, and the Wellcome Trust Sanger Institute [grant number WT098051]. The views expressed in this publication are those of the author(s) and not necessarily those of the Wellcome Trust or the Department of Health. The study has UK Research Ethics Committee approval (10/H0305/83, granted by the Cambridge South REC, and GEN/284/12 granted by the Republic of Ireland REC). The research team acknowledges the support of the National Institute for Health Research, through the Comprehensive Clinical Research Network. This study makes use of DECIPHER (http://decipher.sanger.ac.uk), which is funded by the Wellcome Trust. Publisher Copyright: © 2018, The Author(s).

PY - 2018/5/1

Y1 - 2018/5/1

N2 - Many genetic causes of developmental delay and/or intellectual disability (DD/ID) are extremely rare, and robust discovery of these requires both large-scale DNA sequencing and data sharing. Here we describe a GeneMatcher collaboration which led to a cohort of 13 affected individuals harboring protein-altering variants, 11 of which are de novo, in MED13; the only inherited variant was transmitted to an affected child from an affected mother. All patients had intellectual disability and/or developmental delays, including speech delays or disorders. Other features that were reported in two or more patients include autism spectrum disorder, attention deficit hyperactivity disorder, optic nerve abnormalities, Duane anomaly, hypotonia, mild congenital heart abnormalities, and dysmorphisms. Six affected individuals had mutations that are predicted to truncate the MED13 protein, six had missense mutations, and one had an in-frame-deletion of one amino acid. Out of the seven non-truncating mutations, six clustered in two specific locations of the MED13 protein: an N-terminal and C-terminal region. The four N-terminal clustering mutations affect two adjacent amino acids that are known to be involved in MED13 ubiquitination and degradation, p.Thr326 and p.Pro327. MED13 is a component of the CDK8-kinase module that can reversibly bind Mediator, a multi-protein complex that is required for Polymerase II transcription initiation. Mutations in several other genes encoding subunits of Mediator have been previously shown to associate with DD/ID, including MED13L, a paralog of MED13. Thus, our findings add MED13 to the group of CDK8-kinase module-associated disease genes.

AB - Many genetic causes of developmental delay and/or intellectual disability (DD/ID) are extremely rare, and robust discovery of these requires both large-scale DNA sequencing and data sharing. Here we describe a GeneMatcher collaboration which led to a cohort of 13 affected individuals harboring protein-altering variants, 11 of which are de novo, in MED13; the only inherited variant was transmitted to an affected child from an affected mother. All patients had intellectual disability and/or developmental delays, including speech delays or disorders. Other features that were reported in two or more patients include autism spectrum disorder, attention deficit hyperactivity disorder, optic nerve abnormalities, Duane anomaly, hypotonia, mild congenital heart abnormalities, and dysmorphisms. Six affected individuals had mutations that are predicted to truncate the MED13 protein, six had missense mutations, and one had an in-frame-deletion of one amino acid. Out of the seven non-truncating mutations, six clustered in two specific locations of the MED13 protein: an N-terminal and C-terminal region. The four N-terminal clustering mutations affect two adjacent amino acids that are known to be involved in MED13 ubiquitination and degradation, p.Thr326 and p.Pro327. MED13 is a component of the CDK8-kinase module that can reversibly bind Mediator, a multi-protein complex that is required for Polymerase II transcription initiation. Mutations in several other genes encoding subunits of Mediator have been previously shown to associate with DD/ID, including MED13L, a paralog of MED13. Thus, our findings add MED13 to the group of CDK8-kinase module-associated disease genes.

KW - Journal Article

KW - Amino Acid Sequence

KW - Sequence Deletion

KW - Humans

KW - Child, Preschool

KW - Male

KW - United Kingdom

KW - Mutation, Missense

KW - Cyclin-Dependent Kinase 8/genetics

KW - Ubiquitination/genetics

KW - Adult

KW - Female

KW - Mediator Complex/genetics

KW - Transcription Initiation, Genetic

KW - Child

KW - Neurodevelopmental Disorders/genetics

UR - http://www.scopus.com/inward/record.url?scp=85046628315&partnerID=8YFLogxK

U2 - 10.1007/s00439-018-1887-y

DO - 10.1007/s00439-018-1887-y

M3 - Article

C2 - 29740699

SN - 0340-6717

VL - 137

SP - 375

EP - 388

JO - Human Genetics

JF - Human Genetics

IS - 5

ER -

De novo mutations in MED13, a component of the Mediator complex, are associated with a novel neurodevelopmental disorder

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