Recurrent duplications of 17q12 associated with variable phenotypes

Elyse Mitchell; Andrew Douglas; Susanne Kjaegaard; Bert Callewaert; Arnaud Vanlander; Sandra Janssens; Amy Lawson Yuen; Cindy Skinner; Pinella Failla; Antonino Alberti; Emanuela Avola; Marco Fichera; Maria Kibaek; Maria C. Digilio; Mark C. Hannibal; Nicolette S. den Hollander; Veronica Bizzarri; Alessandra Renieri; Maria Antonietta Mencarelli; Tomas Fitzgerald; Serena Piazzolla; Elke van Oudenhove; Corrado Romano; Charles Schwartz; Evan E. Eichler; Anne Slavotinek; Luis Escobar; Diana Rajan; John Crolla; Nigel Carter; Jennelle C. Hodge; Heather C. Mefford

doi:10.1002/ajmg.a.37351

Recurrent duplications of 17q12 associated with variable phenotypes

Elyse Mitchell, Andrew Douglas, Susanne Kjaegaard, Bert Callewaert, Arnaud Vanlander, Sandra Janssens, Amy Lawson Yuen, Cindy Skinner, Pinella Failla, Antonino Alberti, Emanuela Avola, Marco Fichera, Maria Kibaek, Maria C. Digilio, Mark C. Hannibal, Nicolette S. den Hollander, Veronica Bizzarri, Alessandra Renieri, Maria Antonietta Mencarelli, Tomas FitzgeraldSerena Piazzolla, Elke van Oudenhove, Corrado Romano, Charles Schwartz, Evan E. Eichler, Anne Slavotinek, Luis Escobar, Diana Rajan, John Crolla, Nigel Carter, Jennelle C. Hodge, Heather C. Mefford

Laboratory Medicine and Pathology

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

16 Scopus citations

Abstract

The ability to identify the clinical nature of the recurrent duplication of chromosome 17q12 has been limited by its rarity and the diverse range of phenotypes associated with this genomic change. In order to further define the clinical features of affected patients, detailed clinical information was collected in the largest series to date (30 patients and 2 of their siblings) through a multi-institutional collaborative effort. The majority of patients presented with developmental delays varying from mild to severe. Though dysmorphic features were commonly reported, patients do not have consistent and recognizable features. Cardiac, ophthalmologic, growth, behavioral, and other abnormalities were each present in a subset of patients. The newly associated features potentially resulting from 17q12 duplication include height and weight above the 95th percentile, cataracts, microphthalmia, coloboma, astigmatism, tracheomalacia, cutaneous mosaicism, pectus excavatum, scoliosis, hypermobility, hypospadias, diverticulum of Kommerell, pyloric stenosis, and pseudohypoparathryoidism. The majority of duplications were inherited with some carrier parents reporting learning disabilities or microcephaly. We identified additional, potentially contributory copy number changes in a subset of patients, including one patient each with 16p11.2 deletion and 15q13.3 deletion. Our data further define and expand the clinical spectrum associated with duplications of 17q12 and provide support for the role of genomic modifiers contributing to phenotypic variability.

Original language	English (US)
Pages (from-to)	3038-3045
Number of pages	8
Journal	American Journal of Medical Genetics, Part A
Volume	167
Issue number	12
DOIs	https://doi.org/10.1002/ajmg.a.37351
State	Published - Dec 1 2015

Keywords

CNV
Duplication
Genotype phenotype

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1002/ajmg.a.37351

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Mitchell, E., Douglas, A., Kjaegaard, S., Callewaert, B., Vanlander, A., Janssens, S., Yuen, A. L., Skinner, C., Failla, P., Alberti, A., Avola, E., Fichera, M., Kibaek, M., Digilio, M. C., Hannibal, M. C., den Hollander, N. S., Bizzarri, V., Renieri, A., Mencarelli, M. A., ... Mefford, H. C. (2015). Recurrent duplications of 17q12 associated with variable phenotypes. American Journal of Medical Genetics, Part A, 167(12), 3038-3045. https://doi.org/10.1002/ajmg.a.37351

Mitchell, E, Douglas, A, Kjaegaard, S, Callewaert, B, Vanlander, A, Janssens, S, Yuen, AL, Skinner, C, Failla, P, Alberti, A, Avola, E, Fichera, M, Kibaek, M, Digilio, MC, Hannibal, MC, den Hollander, NS, Bizzarri, V, Renieri, A, Mencarelli, MA, Fitzgerald, T, Piazzolla, S, van Oudenhove, E, Romano, C, Schwartz, C, Eichler, EE, Slavotinek, A, Escobar, L, Rajan, D, Crolla, J, Carter, N, Hodge, JC & Mefford, HC 2015, 'Recurrent duplications of 17q12 associated with variable phenotypes', American Journal of Medical Genetics, Part A, vol. 167, no. 12, pp. 3038-3045. https://doi.org/10.1002/ajmg.a.37351

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title = "Recurrent duplications of 17q12 associated with variable phenotypes",

abstract = "The ability to identify the clinical nature of the recurrent duplication of chromosome 17q12 has been limited by its rarity and the diverse range of phenotypes associated with this genomic change. In order to further define the clinical features of affected patients, detailed clinical information was collected in the largest series to date (30 patients and 2 of their siblings) through a multi-institutional collaborative effort. The majority of patients presented with developmental delays varying from mild to severe. Though dysmorphic features were commonly reported, patients do not have consistent and recognizable features. Cardiac, ophthalmologic, growth, behavioral, and other abnormalities were each present in a subset of patients. The newly associated features potentially resulting from 17q12 duplication include height and weight above the 95th percentile, cataracts, microphthalmia, coloboma, astigmatism, tracheomalacia, cutaneous mosaicism, pectus excavatum, scoliosis, hypermobility, hypospadias, diverticulum of Kommerell, pyloric stenosis, and pseudohypoparathryoidism. The majority of duplications were inherited with some carrier parents reporting learning disabilities or microcephaly. We identified additional, potentially contributory copy number changes in a subset of patients, including one patient each with 16p11.2 deletion and 15q13.3 deletion. Our data further define and expand the clinical spectrum associated with duplications of 17q12 and provide support for the role of genomic modifiers contributing to phenotypic variability.",

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author = "Elyse Mitchell and Andrew Douglas and Susanne Kjaegaard and Bert Callewaert and Arnaud Vanlander and Sandra Janssens and Yuen, {Amy Lawson} and Cindy Skinner and Pinella Failla and Antonino Alberti and Emanuela Avola and Marco Fichera and Maria Kibaek and Digilio, {Maria C.} and Hannibal, {Mark C.} and {den Hollander}, {Nicolette S.} and Veronica Bizzarri and Alessandra Renieri and Mencarelli, {Maria Antonietta} and Tomas Fitzgerald and Serena Piazzolla and {van Oudenhove}, Elke and Corrado Romano and Charles Schwartz and Eichler, {Evan E.} and Anne Slavotinek and Luis Escobar and Diana Rajan and John Crolla and Nigel Carter and Hodge, {Jennelle C.} and Mefford, {Heather C.}",

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T1 - Recurrent duplications of 17q12 associated with variable phenotypes

AU - Mitchell, Elyse

AU - Douglas, Andrew

AU - Kjaegaard, Susanne

AU - Callewaert, Bert

AU - Vanlander, Arnaud

AU - Janssens, Sandra

AU - Yuen, Amy Lawson

AU - Skinner, Cindy

AU - Failla, Pinella

AU - Alberti, Antonino

AU - Avola, Emanuela

AU - Fichera, Marco

AU - Kibaek, Maria

AU - Digilio, Maria C.

AU - Hannibal, Mark C.

AU - den Hollander, Nicolette S.

AU - Bizzarri, Veronica

AU - Renieri, Alessandra

AU - Mencarelli, Maria Antonietta

AU - Fitzgerald, Tomas

AU - Piazzolla, Serena

AU - van Oudenhove, Elke

AU - Romano, Corrado

AU - Schwartz, Charles

AU - Eichler, Evan E.

AU - Slavotinek, Anne

AU - Escobar, Luis

AU - Rajan, Diana

AU - Crolla, John

AU - Carter, Nigel

AU - Hodge, Jennelle C.

AU - Mefford, Heather C.

PY - 2015/12/1

Y1 - 2015/12/1

N2 - The ability to identify the clinical nature of the recurrent duplication of chromosome 17q12 has been limited by its rarity and the diverse range of phenotypes associated with this genomic change. In order to further define the clinical features of affected patients, detailed clinical information was collected in the largest series to date (30 patients and 2 of their siblings) through a multi-institutional collaborative effort. The majority of patients presented with developmental delays varying from mild to severe. Though dysmorphic features were commonly reported, patients do not have consistent and recognizable features. Cardiac, ophthalmologic, growth, behavioral, and other abnormalities were each present in a subset of patients. The newly associated features potentially resulting from 17q12 duplication include height and weight above the 95th percentile, cataracts, microphthalmia, coloboma, astigmatism, tracheomalacia, cutaneous mosaicism, pectus excavatum, scoliosis, hypermobility, hypospadias, diverticulum of Kommerell, pyloric stenosis, and pseudohypoparathryoidism. The majority of duplications were inherited with some carrier parents reporting learning disabilities or microcephaly. We identified additional, potentially contributory copy number changes in a subset of patients, including one patient each with 16p11.2 deletion and 15q13.3 deletion. Our data further define and expand the clinical spectrum associated with duplications of 17q12 and provide support for the role of genomic modifiers contributing to phenotypic variability.

AB - The ability to identify the clinical nature of the recurrent duplication of chromosome 17q12 has been limited by its rarity and the diverse range of phenotypes associated with this genomic change. In order to further define the clinical features of affected patients, detailed clinical information was collected in the largest series to date (30 patients and 2 of their siblings) through a multi-institutional collaborative effort. The majority of patients presented with developmental delays varying from mild to severe. Though dysmorphic features were commonly reported, patients do not have consistent and recognizable features. Cardiac, ophthalmologic, growth, behavioral, and other abnormalities were each present in a subset of patients. The newly associated features potentially resulting from 17q12 duplication include height and weight above the 95th percentile, cataracts, microphthalmia, coloboma, astigmatism, tracheomalacia, cutaneous mosaicism, pectus excavatum, scoliosis, hypermobility, hypospadias, diverticulum of Kommerell, pyloric stenosis, and pseudohypoparathryoidism. The majority of duplications were inherited with some carrier parents reporting learning disabilities or microcephaly. We identified additional, potentially contributory copy number changes in a subset of patients, including one patient each with 16p11.2 deletion and 15q13.3 deletion. Our data further define and expand the clinical spectrum associated with duplications of 17q12 and provide support for the role of genomic modifiers contributing to phenotypic variability.

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KW - Duplication

KW - Genotype phenotype

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Recurrent duplications of 17q12 associated with variable phenotypes

Abstract

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