Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate.

Amelia M Lindgren; Tatiana Hoyos; Michael E Talkowski; Carrie Hanscom; Ian Blumenthal; Colby Chiang; Carl Ernst; Shahrin Pereira; Zehra Ordulu; Carol Clericuzio; Joanne M Drautz; Jill A Rosenfeld; Lisa G Shaffer; Lea Velsher; Tania Pynn; Joris Vermeesch; David J Harris; James F Gusella; Eric C Liao; Cynthia C Morton

doi:10.1007/s00439-013-1263-x

Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate.

Amelia M Lindgren, Tatiana Hoyos, Michael E Talkowski, Carrie Hanscom, Ian Blumenthal, Colby Chiang, Carl Ernst, Shahrin Pereira, Zehra Ordulu, Carol Clericuzio, Joanne M Drautz, Jill A Rosenfeld, Lisa G Shaffer, Lea Velsher, Tania Pynn, Joris Vermeesch, David J Harris, James F Gusella, Eric C Liao, Cynthia C Morton

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

Abstract

We describe a female subject (DGAP100) with a 46,X,t(X;5)(p11.3;q35.3)inv(5)(q35.3q35.1)dn, severe psychomotor retardation with hypotonia, global postnatal growth restriction, microcephaly, globally reduced cerebral volume, seizures, facial dysmorphia and cleft palate. Fluorescence in situ hybridization and whole-genome sequencing demonstrated that the X chromosome breakpoint disrupts KDM6A in the second intron. No genes were directly disrupted on chromosome 5. KDM6A is a histone 3 lysine 27 demethylase and a histone 3 lysine 4 methyltransferase. Expression of KDM6A is significantly reduced in DGAP100 lymphoblastoid cells compared to control samples. We identified nine additional cases with neurodevelopmental delay and various other features consistent with the DGAP100 phenotype with copy number variation encompassing KDM6A from microarray databases. We evaluated haploinsufficiency of kdm6a in a zebrafish model. kdm6a is expressed in the pharyngeal arches and ethmoid plate of the developing zebrafish, while a kdm6a morpholino knockdown exhibited craniofacial defects. We conclude KDM6A dosage regulation is associated with severe and diverse structural defects and developmental abnormalities.

Original language	English
Journal	Human Genetics
Volume	132
Issue number	5
DOIs	https://doi.org/10.1007/s00439-013-1263-x
Publication status	Published - May 2013

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Lindgren, A. M., Hoyos, T., Talkowski, M. E., Hanscom, C., Blumenthal, I., Chiang, C., Ernst, C., Pereira, S., Ordulu, Z., Clericuzio, C., Drautz, J. M., Rosenfeld, J. A., Shaffer, L. G., Velsher, L., Pynn, T., Vermeesch, J., Harris, D. J., Gusella, J. F., Liao, E. C., & Morton, C. C. (2013). Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate. Human Genetics, 132(5). https://doi.org/10.1007/s00439-013-1263-x

@article{3213bab0e0c8478f9b575b49101ec8a3,

title = "Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate.",

abstract = "We describe a female subject (DGAP100) with a 46,X,t(X;5)(p11.3;q35.3)inv(5)(q35.3q35.1)dn, severe psychomotor retardation with hypotonia, global postnatal growth restriction, microcephaly, globally reduced cerebral volume, seizures, facial dysmorphia and cleft palate. Fluorescence in situ hybridization and whole-genome sequencing demonstrated that the X chromosome breakpoint disrupts KDM6A in the second intron. No genes were directly disrupted on chromosome 5. KDM6A is a histone 3 lysine 27 demethylase and a histone 3 lysine 4 methyltransferase. Expression of KDM6A is significantly reduced in DGAP100 lymphoblastoid cells compared to control samples. We identified nine additional cases with neurodevelopmental delay and various other features consistent with the DGAP100 phenotype with copy number variation encompassing KDM6A from microarray databases. We evaluated haploinsufficiency of kdm6a in a zebrafish model. kdm6a is expressed in the pharyngeal arches and ethmoid plate of the developing zebrafish, while a kdm6a morpholino knockdown exhibited craniofacial defects. We conclude KDM6A dosage regulation is associated with severe and diverse structural defects and developmental abnormalities.",

author = "Lindgren, {Amelia M} and Tatiana Hoyos and Talkowski, {Michael E} and Carrie Hanscom and Ian Blumenthal and Colby Chiang and Carl Ernst and Shahrin Pereira and Zehra Ordulu and Carol Clericuzio and Drautz, {Joanne M} and Rosenfeld, {Jill A} and Shaffer, {Lisa G} and Lea Velsher and Tania Pynn and Joris Vermeesch and Harris, {David J} and Gusella, {James F} and Liao, {Eric C} and Morton, {Cynthia C}",

note = "HD065286, NICHD NIH HHS, United StatesMH095867, NIMH NIH HHS, United StatesP01 GM061354, NIGMS NIH HHS, United StatesP01GM061354, NIGMS NIH HHS, United StatesP30 CA006516, NCI NIH HHS, United StatesP30 CA006516, NCI NIH HHS, United States",

year = "2013",

month = may,

doi = "10.1007/s00439-013-1263-x",

language = "English",

volume = "132",

journal = "Human Genetics",

issn = "1432-1203",

publisher = "Springer Nature",

number = "5",

}

Lindgren, AM, Hoyos, T, Talkowski, ME, Hanscom, C, Blumenthal, I, Chiang, C, Ernst, C, Pereira, S, Ordulu, Z, Clericuzio, C, Drautz, JM, Rosenfeld, JA, Shaffer, LG, Velsher, L, Pynn, T, Vermeesch, J, Harris, DJ, Gusella, JF, Liao, EC & Morton, CC 2013, 'Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate.', Human Genetics, vol. 132, no. 5. https://doi.org/10.1007/s00439-013-1263-x

TY - JOUR

T1 - Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate.

AU - Lindgren, Amelia M

AU - Hoyos, Tatiana

AU - Talkowski, Michael E

AU - Hanscom, Carrie

AU - Blumenthal, Ian

AU - Chiang, Colby

AU - Ernst, Carl

AU - Pereira, Shahrin

AU - Ordulu, Zehra

AU - Clericuzio, Carol

AU - Drautz, Joanne M

AU - Rosenfeld, Jill A

AU - Shaffer, Lisa G

AU - Velsher, Lea

AU - Pynn, Tania

AU - Vermeesch, Joris

AU - Harris, David J

AU - Gusella, James F

AU - Liao, Eric C

AU - Morton, Cynthia C

N1 - HD065286, NICHD NIH HHS, United StatesMH095867, NIMH NIH HHS, United StatesP01 GM061354, NIGMS NIH HHS, United StatesP01GM061354, NIGMS NIH HHS, United StatesP30 CA006516, NCI NIH HHS, United StatesP30 CA006516, NCI NIH HHS, United States

PY - 2013/5

Y1 - 2013/5

N2 - We describe a female subject (DGAP100) with a 46,X,t(X;5)(p11.3;q35.3)inv(5)(q35.3q35.1)dn, severe psychomotor retardation with hypotonia, global postnatal growth restriction, microcephaly, globally reduced cerebral volume, seizures, facial dysmorphia and cleft palate. Fluorescence in situ hybridization and whole-genome sequencing demonstrated that the X chromosome breakpoint disrupts KDM6A in the second intron. No genes were directly disrupted on chromosome 5. KDM6A is a histone 3 lysine 27 demethylase and a histone 3 lysine 4 methyltransferase. Expression of KDM6A is significantly reduced in DGAP100 lymphoblastoid cells compared to control samples. We identified nine additional cases with neurodevelopmental delay and various other features consistent with the DGAP100 phenotype with copy number variation encompassing KDM6A from microarray databases. We evaluated haploinsufficiency of kdm6a in a zebrafish model. kdm6a is expressed in the pharyngeal arches and ethmoid plate of the developing zebrafish, while a kdm6a morpholino knockdown exhibited craniofacial defects. We conclude KDM6A dosage regulation is associated with severe and diverse structural defects and developmental abnormalities.

AB - We describe a female subject (DGAP100) with a 46,X,t(X;5)(p11.3;q35.3)inv(5)(q35.3q35.1)dn, severe psychomotor retardation with hypotonia, global postnatal growth restriction, microcephaly, globally reduced cerebral volume, seizures, facial dysmorphia and cleft palate. Fluorescence in situ hybridization and whole-genome sequencing demonstrated that the X chromosome breakpoint disrupts KDM6A in the second intron. No genes were directly disrupted on chromosome 5. KDM6A is a histone 3 lysine 27 demethylase and a histone 3 lysine 4 methyltransferase. Expression of KDM6A is significantly reduced in DGAP100 lymphoblastoid cells compared to control samples. We identified nine additional cases with neurodevelopmental delay and various other features consistent with the DGAP100 phenotype with copy number variation encompassing KDM6A from microarray databases. We evaluated haploinsufficiency of kdm6a in a zebrafish model. kdm6a is expressed in the pharyngeal arches and ethmoid plate of the developing zebrafish, while a kdm6a morpholino knockdown exhibited craniofacial defects. We conclude KDM6A dosage regulation is associated with severe and diverse structural defects and developmental abnormalities.

U2 - 10.1007/s00439-013-1263-x

DO - 10.1007/s00439-013-1263-x

M3 - Article

C2 - 23354975

SN - 1432-1203

VL - 132

JO - Human Genetics

JF - Human Genetics

IS - 5

ER -

Haploinsufficiency of KDM6A is associated with severe psychomotor retardation, global growth restriction, seizures and cleft palate.

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