De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females

E. E. Palmer; T. Stuhlmann; S. Weinert; E. Haan; H. Van Esch; M. Holvoet; J. Boyle; M. Leffler; M. Raynaud; C. Moraine; H. Van Bokhoven; T. Kleefstra; K. Kahrizi; H. Najmabadi; H. H. Ropers; M. R. Delgado; D. Sirsi; S. Golla; A. Sommer; M. P. Pietryga; W. K. Chung; J. Wynn; L. Rohena; E. Bernardo; D. Hamlin; B. M. Faux; D. K. Grange; L. Manwaring; J. Tolmie; S. Joss; D. D.D. Study; J. M. Cobben; F. A.M. Duijkers; J. M. Goehringer; T. D. Challman; F. Hennig; U. Fischer; A. Grimme; V. Suckow; L. Musante; J. Nicholl; M. Shaw; S. P. Lodh; Z. Niu; J. A. Rosenfeld; P. Stankiewicz; T. J. Jentsch; J. Gecz; M. Field; V. M. Kalscheuer

doi:10.1038/mp.2016.135

De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females

E. E. Palmer, T. Stuhlmann, S. Weinert, E. Haan, H. Van Esch, M. Holvoet, J. Boyle, M. Leffler, M. Raynaud, C. Moraine, H. Van Bokhoven, T. Kleefstra, K. Kahrizi, H. Najmabadi, H. H. Ropers, M. R. Delgado, D. Sirsi, S. Golla, A. Sommer, M. P. PietrygaW. K. Chung, J. Wynn, L. Rohena, E. Bernardo, D. Hamlin, B. M. Faux, D. K. Grange, L. Manwaring, J. Tolmie, S. Joss, D. D.D. Study, J. M. Cobben, F. A.M. Duijkers, J. M. Goehringer, T. D. Challman, F. Hennig, U. Fischer, A. Grimme, V. Suckow, L. Musante, J. Nicholl, M. Shaw, S. P. Lodh, Z. Niu, J. A. Rosenfeld, P. Stankiewicz, T. J. Jentsch, J. Gecz, M. Field, V. M. Kalscheuer

Laboratory Medicine and Pathology

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

19 Scopus citations

Abstract

Variants in CLCN4, which encodes the chloride/hydrogen ion exchanger CIC-4 prominently expressed in brain, were recently described to cause X-linked intellectual disability and epilepsy. We present detailed phenotypic information on 52 individuals from 16 families with CLCN4-related disorder: 5 affected females and 2 affected males with a de novo variant in CLCN4 (6 individuals previously unreported) and 27 affected males, 3 affected females and 15 asymptomatic female carriers from 9 families with inherited CLCN4 variants (4 families previously unreported). Intellectual disability ranged from borderline to profound. Behavioral and psychiatric disorders were common in both child-and adulthood, and included autistic features, mood disorders, obsessive-compulsive behaviors and hetero-and autoaggression. Epilepsy was common, with severity ranging from epileptic encephalopathy to well-controlled seizures. Several affected individuals showed white matter changes on cerebral neuroimaging and progressive neurological symptoms, including movement disorders and spasticity. Heterozygous females can be as severely affected as males. The variability of symptoms in females is not correlated with the X inactivation pattern studied in their blood. The mutation spectrum includes frameshift, missense and splice site variants and one single-exon deletion. All missense variants were predicted to affect CLCN4's function based on in silico tools and either segregated with the phenotype in the family or were de novo. Pathogenicity of all previously unreported missense variants was further supported by electrophysiological studies in Xenopus laevis oocytes. We compare CLCN4-related disorder with conditions related to dysfunction of other members of the CLC family.

Original language	English (US)
Pages (from-to)	222-230
Number of pages	9
Journal	Molecular Psychiatry
Volume	23
Issue number	2
DOIs	https://doi.org/10.1038/mp.2016.135
State	Published - Feb 1 2018

ASJC Scopus subject areas

Molecular Biology
Cellular and Molecular Neuroscience
Psychiatry and Mental health

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Palmer, E. E., Stuhlmann, T., Weinert, S., Haan, E., Van Esch, H., Holvoet, M., Boyle, J., Leffler, M., Raynaud, M., Moraine, C., Van Bokhoven, H., Kleefstra, T., Kahrizi, K., Najmabadi, H., Ropers, H. H., Delgado, M. R., Sirsi, D., Golla, S., Sommer, A., ... Kalscheuer, V. M. (2018). De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females. Molecular Psychiatry, 23(2), 222-230. https://doi.org/10.1038/mp.2016.135

Palmer, EE, Stuhlmann, T, Weinert, S, Haan, E, Van Esch, H, Holvoet, M, Boyle, J, Leffler, M, Raynaud, M, Moraine, C, Van Bokhoven, H, Kleefstra, T, Kahrizi, K, Najmabadi, H, Ropers, HH, Delgado, MR, Sirsi, D, Golla, S, Sommer, A, Pietryga, MP, Chung, WK, Wynn, J, Rohena, L, Bernardo, E, Hamlin, D, Faux, BM, Grange, DK, Manwaring, L, Tolmie, J, Joss, S, Study, DDD, Cobben, JM, Duijkers, FAM, Goehringer, JM, Challman, TD, Hennig, F, Fischer, U, Grimme, A, Suckow, V, Musante, L, Nicholl, J, Shaw, M, Lodh, SP, Niu, Z, Rosenfeld, JA, Stankiewicz, P, Jentsch, TJ, Gecz, J, Field, M & Kalscheuer, VM 2018, 'De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females', Molecular Psychiatry, vol. 23, no. 2, pp. 222-230. https://doi.org/10.1038/mp.2016.135

@article{24751f17c9c24e51909ec8a751e40a9c,

title = "De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females",

abstract = "Variants in CLCN4, which encodes the chloride/hydrogen ion exchanger CIC-4 prominently expressed in brain, were recently described to cause X-linked intellectual disability and epilepsy. We present detailed phenotypic information on 52 individuals from 16 families with CLCN4-related disorder: 5 affected females and 2 affected males with a de novo variant in CLCN4 (6 individuals previously unreported) and 27 affected males, 3 affected females and 15 asymptomatic female carriers from 9 families with inherited CLCN4 variants (4 families previously unreported). Intellectual disability ranged from borderline to profound. Behavioral and psychiatric disorders were common in both child-and adulthood, and included autistic features, mood disorders, obsessive-compulsive behaviors and hetero-and autoaggression. Epilepsy was common, with severity ranging from epileptic encephalopathy to well-controlled seizures. Several affected individuals showed white matter changes on cerebral neuroimaging and progressive neurological symptoms, including movement disorders and spasticity. Heterozygous females can be as severely affected as males. The variability of symptoms in females is not correlated with the X inactivation pattern studied in their blood. The mutation spectrum includes frameshift, missense and splice site variants and one single-exon deletion. All missense variants were predicted to affect CLCN4's function based on in silico tools and either segregated with the phenotype in the family or were de novo. Pathogenicity of all previously unreported missense variants was further supported by electrophysiological studies in Xenopus laevis oocytes. We compare CLCN4-related disorder with conditions related to dysfunction of other members of the CLC family.",

author = "Palmer, {E. E.} and T. Stuhlmann and S. Weinert and E. Haan and {Van Esch}, H. and M. Holvoet and J. Boyle and M. Leffler and M. Raynaud and C. Moraine and {Van Bokhoven}, H. and T. Kleefstra and K. Kahrizi and H. Najmabadi and Ropers, {H. H.} and Delgado, {M. R.} and D. Sirsi and S. Golla and A. Sommer and Pietryga, {M. P.} and Chung, {W. K.} and J. Wynn and L. Rohena and E. Bernardo and D. Hamlin and Faux, {B. M.} and Grange, {D. K.} and L. Manwaring and J. Tolmie and S. Joss and Study, {D. D.D.} and Cobben, {J. M.} and Duijkers, {F. A.M.} and Goehringer, {J. M.} and Challman, {T. D.} and F. Hennig and U. Fischer and A. Grimme and V. Suckow and L. Musante and J. Nicholl and M. Shaw and Lodh, {S. P.} and Z. Niu and Rosenfeld, {J. A.} and P. Stankiewicz and Jentsch, {T. J.} and J. Gecz and M. Field and Kalscheuer, {V. M.}",

note = "Funding Information: We thank the individuals and their families who participated in this study, and the bioinformaticians and molecular geneticists analyzing NGS data. We thank Patrick Seidler for help with oocyte measurements. We thank Professor David Sillence for his valuable assistance in the preparation of the manuscript. Part of this study was financed by a grant of the German Ministry of Education and Research through the MRNET and the EU FP7 project GENCODYS, grant number 241995; TJJ was supported by the Deutsche Forschungsgemeinschaft (SFB740); JG received NHMRC Grants 628952 and 1041920, and WKC received grant support from the Simons Foundation and National Institute of Health grant (HD057036) and was supported in part by Columbia University's Clinical and Translational Science Award (CTSA), grant (UL1 RR024156). 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 authors 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. Funding Information: We thank the individuals and their families who participated in this study, and the bioinformaticians and molecular geneticists analyzing NGS data. We thank Patrick Seidler for help with oocyte measurements. We thank Professor David Sillence for his valuable assistance in the preparation of the manuscript. Part of this study was financed by a grant of the German Ministry of Education and Research through the MRNET and the EU FP7 project GENCODYS, grant number 241995; TJJ was supported by the Deutsche Forschungsgemeinschaft (SFB740); JG received NHMRC Grants 628952 and 1041920, and WKC received grant support from the Simons Foundation and National Institute of Health grant (HD057036) and was supported in part by Columbia University{\textquoteright}s Clinical and Translational Science Award (CTSA), grant (UL1 RR024156). 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 authors 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. Publisher Copyright: {\textcopyright} 2018 Macmillan Publishers Limited, part of Springer Nature. All rights reserved.",

year = "2018",

month = feb,

day = "1",

doi = "10.1038/mp.2016.135",

language = "English (US)",

volume = "23",

pages = "222--230",

journal = "Molecular Psychiatry",

issn = "1359-4184",

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TY - JOUR

T1 - De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females

AU - Palmer, E. E.

AU - Stuhlmann, T.

AU - Weinert, S.

AU - Haan, E.

AU - Van Esch, H.

AU - Holvoet, M.

AU - Boyle, J.

AU - Leffler, M.

AU - Raynaud, M.

AU - Moraine, C.

AU - Van Bokhoven, H.

AU - Kleefstra, T.

AU - Kahrizi, K.

AU - Najmabadi, H.

AU - Ropers, H. H.

AU - Delgado, M. R.

AU - Sirsi, D.

AU - Golla, S.

AU - Sommer, A.

AU - Pietryga, M. P.

AU - Chung, W. K.

AU - Wynn, J.

AU - Rohena, L.

AU - Bernardo, E.

AU - Hamlin, D.

AU - Faux, B. M.

AU - Grange, D. K.

AU - Manwaring, L.

AU - Tolmie, J.

AU - Joss, S.

AU - Study, D. D.D.

AU - Cobben, J. M.

AU - Duijkers, F. A.M.

AU - Goehringer, J. M.

AU - Challman, T. D.

AU - Hennig, F.

AU - Fischer, U.

AU - Grimme, A.

AU - Suckow, V.

AU - Musante, L.

AU - Nicholl, J.

AU - Shaw, M.

AU - Lodh, S. P.

AU - Niu, Z.

AU - Rosenfeld, J. A.

AU - Stankiewicz, P.

AU - Jentsch, T. J.

AU - Gecz, J.

AU - Field, M.

AU - Kalscheuer, V. M.

N1 - Funding Information: We thank the individuals and their families who participated in this study, and the bioinformaticians and molecular geneticists analyzing NGS data. We thank Patrick Seidler for help with oocyte measurements. We thank Professor David Sillence for his valuable assistance in the preparation of the manuscript. Part of this study was financed by a grant of the German Ministry of Education and Research through the MRNET and the EU FP7 project GENCODYS, grant number 241995; TJJ was supported by the Deutsche Forschungsgemeinschaft (SFB740); JG received NHMRC Grants 628952 and 1041920, and WKC received grant support from the Simons Foundation and National Institute of Health grant (HD057036) and was supported in part by Columbia University's Clinical and Translational Science Award (CTSA), grant (UL1 RR024156). 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 authors 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. Funding Information: We thank the individuals and their families who participated in this study, and the bioinformaticians and molecular geneticists analyzing NGS data. We thank Patrick Seidler for help with oocyte measurements. We thank Professor David Sillence for his valuable assistance in the preparation of the manuscript. Part of this study was financed by a grant of the German Ministry of Education and Research through the MRNET and the EU FP7 project GENCODYS, grant number 241995; TJJ was supported by the Deutsche Forschungsgemeinschaft (SFB740); JG received NHMRC Grants 628952 and 1041920, and WKC received grant support from the Simons Foundation and National Institute of Health grant (HD057036) and was supported in part by Columbia University’s Clinical and Translational Science Award (CTSA), grant (UL1 RR024156). 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 authors 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. Publisher Copyright: © 2018 Macmillan Publishers Limited, part of Springer Nature. All rights reserved.

PY - 2018/2/1

Y1 - 2018/2/1

N2 - Variants in CLCN4, which encodes the chloride/hydrogen ion exchanger CIC-4 prominently expressed in brain, were recently described to cause X-linked intellectual disability and epilepsy. We present detailed phenotypic information on 52 individuals from 16 families with CLCN4-related disorder: 5 affected females and 2 affected males with a de novo variant in CLCN4 (6 individuals previously unreported) and 27 affected males, 3 affected females and 15 asymptomatic female carriers from 9 families with inherited CLCN4 variants (4 families previously unreported). Intellectual disability ranged from borderline to profound. Behavioral and psychiatric disorders were common in both child-and adulthood, and included autistic features, mood disorders, obsessive-compulsive behaviors and hetero-and autoaggression. Epilepsy was common, with severity ranging from epileptic encephalopathy to well-controlled seizures. Several affected individuals showed white matter changes on cerebral neuroimaging and progressive neurological symptoms, including movement disorders and spasticity. Heterozygous females can be as severely affected as males. The variability of symptoms in females is not correlated with the X inactivation pattern studied in their blood. The mutation spectrum includes frameshift, missense and splice site variants and one single-exon deletion. All missense variants were predicted to affect CLCN4's function based on in silico tools and either segregated with the phenotype in the family or were de novo. Pathogenicity of all previously unreported missense variants was further supported by electrophysiological studies in Xenopus laevis oocytes. We compare CLCN4-related disorder with conditions related to dysfunction of other members of the CLC family.

AB - Variants in CLCN4, which encodes the chloride/hydrogen ion exchanger CIC-4 prominently expressed in brain, were recently described to cause X-linked intellectual disability and epilepsy. We present detailed phenotypic information on 52 individuals from 16 families with CLCN4-related disorder: 5 affected females and 2 affected males with a de novo variant in CLCN4 (6 individuals previously unreported) and 27 affected males, 3 affected females and 15 asymptomatic female carriers from 9 families with inherited CLCN4 variants (4 families previously unreported). Intellectual disability ranged from borderline to profound. Behavioral and psychiatric disorders were common in both child-and adulthood, and included autistic features, mood disorders, obsessive-compulsive behaviors and hetero-and autoaggression. Epilepsy was common, with severity ranging from epileptic encephalopathy to well-controlled seizures. Several affected individuals showed white matter changes on cerebral neuroimaging and progressive neurological symptoms, including movement disorders and spasticity. Heterozygous females can be as severely affected as males. The variability of symptoms in females is not correlated with the X inactivation pattern studied in their blood. The mutation spectrum includes frameshift, missense and splice site variants and one single-exon deletion. All missense variants were predicted to affect CLCN4's function based on in silico tools and either segregated with the phenotype in the family or were de novo. Pathogenicity of all previously unreported missense variants was further supported by electrophysiological studies in Xenopus laevis oocytes. We compare CLCN4-related disorder with conditions related to dysfunction of other members of the CLC family.

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De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females

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