Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes

Ying Qiao; Kajari Mondal; Valentina Trapani; Jiadi Wen; Gillian Carpenter; Robert Wildin; E. Magda Price; Richard J. Gibbons; Jennifer Eichmeyer; Ruby Jiang; Barbara Dupont; Sally Martell; Suzanne M.E. Lewis; Wendy P. Robinson; Mark O'Driscoll; Federica I. Wolf; Michael E. Zwick; Evica Rajcan-Separovic

doi:10.1002/humu.22465

Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes

Ying Qiao, Kajari Mondal, Valentina Trapani, Jiadi Wen, Gillian Carpenter, Robert Wildin, E. Magda Price, Richard J. Gibbons, Jennifer Eichmeyer, Ruby Jiang, Barbara Dupont, Sally Martell, Suzanne M.E. Lewis, Wendy P. Robinson, Mark O'Driscoll, Federica I. Wolf, Michael E. Zwick, Evica Rajcan-Separovic

School of Allied Health Science

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

10 Scopus citations

Abstract

A 0.8kb intronic duplication in MAGT1 and a single base pair deletion in the last exon of ATRX were identified using a chromosome X-specific microarray and exome sequencing in a family with five males demonstrating intellectual disability (ID) and unusual skin findings (e.g., generalized pruritus). MAGT1 is an Mg²⁺ transporter previously associated with primary immunodeficiency and ID, whereas mutations in ATRX cause ATRX-ID syndrome. In patient cells, the function of ATRX was demonstrated to be abnormal based on altered RNA/protein expression, hypomethylation of rDNA, and abnormal cytokinesis. Dysfunction of MAGT1 was reflected in reduced RNA/protein expression and Mg²⁺ influx. The mutation in ATRX most likely explains the ID, whereas MAGT1 disruption could be linked to abnormal skin findings, as normal magnesium homeostasis is necessary for skin health. This work supports observations that multiple mutations collectively contribute to the phenotypic variability of syndromic ID, and emphasizes the importance of correlating clinical phenotype with genomic and cell function analyses.

Original language	English
Pages (from-to)	58-62
Number of pages	5
Journal	Human Mutation
Volume	35
Issue number	1
DOIs	https://doi.org/10.1002/humu.22465
State	Published - Jan 2014

Keywords

ATRX
Chromosome X
CNV
Exome
Intellectual disability
MAGT1

EGS Disciplines

Genetics and Genomics

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10.1002/humu.22465

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Qiao, Y., Mondal, K., Trapani, V., Wen, J., Carpenter, G., Wildin, R., Price, E. M., Gibbons, R. J., Eichmeyer, J., Jiang, R., Dupont, B., Martell, S., Lewis, S. M. E., Robinson, W. P., O'Driscoll, M., Wolf, F. I., Zwick, M. E., & Rajcan-Separovic, E. (2014). Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes. Human Mutation, 35(1), 58-62. https://doi.org/10.1002/humu.22465

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title = "Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes",

abstract = "A 0.8kb intronic duplication in MAGT1 and a single base pair deletion in the last exon of ATRX were identified using a chromosome X-specific microarray and exome sequencing in a family with five males demonstrating intellectual disability (ID) and unusual skin findings (e.g., generalized pruritus). MAGT1 is an Mg2+ transporter previously associated with primary immunodeficiency and ID, whereas mutations in ATRX cause ATRX-ID syndrome. In patient cells, the function of ATRX was demonstrated to be abnormal based on altered RNA/protein expression, hypomethylation of rDNA, and abnormal cytokinesis. Dysfunction of MAGT1 was reflected in reduced RNA/protein expression and Mg2+ influx. The mutation in ATRX most likely explains the ID, whereas MAGT1 disruption could be linked to abnormal skin findings, as normal magnesium homeostasis is necessary for skin health. This work supports observations that multiple mutations collectively contribute to the phenotypic variability of syndromic ID, and emphasizes the importance of correlating clinical phenotype with genomic and cell function analyses.",

keywords = "ATRX, Chromosome X, CNV, Exome, Intellectual disability, MAGT1",

author = "Ying Qiao and Kajari Mondal and Valentina Trapani and Jiadi Wen and Gillian Carpenter and Robert Wildin and Price, {E. Magda} and Gibbons, {Richard J.} and Jennifer Eichmeyer and Ruby Jiang and Barbara Dupont and Sally Martell and Lewis, {Suzanne M.E.} and Robinson, {Wendy P.} and Mark O'Driscoll and Wolf, {Federica I.} and Zwick, {Michael E.} and Evica Rajcan-Separovic",

note = "Department of Pathology, University of British Columbia (UBC), Vancouver, BC, Canada Department of Medical Genetics, UBC, Vancouver, BC, Canada These authors are considered as first coauthors. Search for more papers by this author Kajari Mondal , Valentina Trapani , E. Magda Price , Wendy P. Robinson , Federica I. Qiao, Ying; Mondal, Kajari; Trapani, Valentina; Wen, Jiadi; Carpenter, Gillian; WIldin, Robert; . . . and Rajcan-Separovic, Evica. (2014). {"}Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes{"}. Human Mutation: Variation, Informatics, and Disease, 35(1), 58-62. https://doi.org/10.1002/humu.22465",

year = "2014",

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doi = "10.1002/humu.22465",

language = "English",

volume = "35",

pages = "58--62",

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TY - JOUR

T1 - Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes

AU - Qiao, Ying

AU - Mondal, Kajari

AU - Trapani, Valentina

AU - Wen, Jiadi

AU - Carpenter, Gillian

AU - Wildin, Robert

AU - Price, E. Magda

AU - Gibbons, Richard J.

AU - Eichmeyer, Jennifer

AU - Jiang, Ruby

AU - Dupont, Barbara

AU - Martell, Sally

AU - Lewis, Suzanne M.E.

AU - Robinson, Wendy P.

AU - O'Driscoll, Mark

AU - Wolf, Federica I.

AU - Zwick, Michael E.

AU - Rajcan-Separovic, Evica

N1 - Department of Pathology, University of British Columbia (UBC), Vancouver, BC, Canada Department of Medical Genetics, UBC, Vancouver, BC, Canada These authors are considered as first coauthors. Search for more papers by this author Kajari Mondal , Valentina Trapani , E. Magda Price , Wendy P. Robinson , Federica I. Qiao, Ying; Mondal, Kajari; Trapani, Valentina; Wen, Jiadi; Carpenter, Gillian; WIldin, Robert; . . . and Rajcan-Separovic, Evica. (2014). "Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes". Human Mutation: Variation, Informatics, and Disease, 35(1), 58-62. https://doi.org/10.1002/humu.22465

PY - 2014/1

Y1 - 2014/1

N2 - A 0.8kb intronic duplication in MAGT1 and a single base pair deletion in the last exon of ATRX were identified using a chromosome X-specific microarray and exome sequencing in a family with five males demonstrating intellectual disability (ID) and unusual skin findings (e.g., generalized pruritus). MAGT1 is an Mg2+ transporter previously associated with primary immunodeficiency and ID, whereas mutations in ATRX cause ATRX-ID syndrome. In patient cells, the function of ATRX was demonstrated to be abnormal based on altered RNA/protein expression, hypomethylation of rDNA, and abnormal cytokinesis. Dysfunction of MAGT1 was reflected in reduced RNA/protein expression and Mg2+ influx. The mutation in ATRX most likely explains the ID, whereas MAGT1 disruption could be linked to abnormal skin findings, as normal magnesium homeostasis is necessary for skin health. This work supports observations that multiple mutations collectively contribute to the phenotypic variability of syndromic ID, and emphasizes the importance of correlating clinical phenotype with genomic and cell function analyses.

AB - A 0.8kb intronic duplication in MAGT1 and a single base pair deletion in the last exon of ATRX were identified using a chromosome X-specific microarray and exome sequencing in a family with five males demonstrating intellectual disability (ID) and unusual skin findings (e.g., generalized pruritus). MAGT1 is an Mg2+ transporter previously associated with primary immunodeficiency and ID, whereas mutations in ATRX cause ATRX-ID syndrome. In patient cells, the function of ATRX was demonstrated to be abnormal based on altered RNA/protein expression, hypomethylation of rDNA, and abnormal cytokinesis. Dysfunction of MAGT1 was reflected in reduced RNA/protein expression and Mg2+ influx. The mutation in ATRX most likely explains the ID, whereas MAGT1 disruption could be linked to abnormal skin findings, as normal magnesium homeostasis is necessary for skin health. This work supports observations that multiple mutations collectively contribute to the phenotypic variability of syndromic ID, and emphasizes the importance of correlating clinical phenotype with genomic and cell function analyses.

KW - ATRX

KW - Chromosome X

KW - CNV

KW - Exome

KW - Intellectual disability

KW - MAGT1

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UR - https://doi.org/10.1002/humu.22465

U2 - 10.1002/humu.22465

DO - 10.1002/humu.22465

M3 - Article

C2 - 24130152

AN - SCOPUS:84890796071

SN - 1059-7794

VL - 35

SP - 58

EP - 62

JO - Human Mutation

JF - Human Mutation

IS - 1

ER -

Variant ATRX Syndrome with Dysfunction of ATRX and MAGT1 Genes

Abstract

Keywords

EGS Disciplines

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