Phenotypic manifestations of copy number variation in chromosome 16p13.11

Sandesh C.Sreenath Nagamani; Ayelet Erez; Patricia Bader; Seema R. Lalani; Daryl A. Scott; Fernando Scaglia; Sharon E. Plon; Chun Hui Tsai; Tyler Reimschisel; Elizabeth Roeder; Amy D. Malphrus; Patricia A. Eng; Patricia M. Hixson; Sung Hae L. Kang; Pawel Stankiewicz; Ankita Patel; Sau Wai Cheung

doi:10.1038/ejhg.2010.184

Phenotypic manifestations of copy number variation in chromosome 16p13.11

Sandesh C.Sreenath Nagamani, Ayelet Erez, Patricia Bader, Seema R. Lalani, Daryl A. Scott, Fernando Scaglia, Sharon E. Plon, Chun Hui Tsai, Tyler Reimschisel, Elizabeth Roeder, Amy D. Malphrus, Patricia A. Eng, Patricia M. Hixson, Sung Hae L. Kang, Pawel Stankiewicz, Ankita Patel, Sau Wai Cheung

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

88 Scopus citations

Abstract

The widespread clinical utilization of array comparative genome hybridization, has led to the unraveling of many new copy number variations (CNVs). Although some of these CNVs are clearly pathogenic, the phenotypic consequences of others, such as those in 16p13.11 remain unclear. Whereas deletions of 16p13.11 have been associated with multiple congenital anomalies, the relevance of duplications of the region is still being debated. We report detailed clinical and molecular characterization of 10 patients with duplication and 4 patients with deletion of 16p13.11. We found that patients with duplication of the region have varied clinical features including behavioral abnormalities, cognitive impairment, congenital heart defects and skeletal manifestations, such as hypermobility, craniosynostosis and polydactyly. These features were incompletely penetrant. Patients with deletion of the region presented with microcephaly, developmental delay and behavioral abnormalities as previously described. The CNVs were of varying sizes and were likely mediated by non-allelic homologous recombination between low copy repeats. Our findings expand the repertoire of clinical features observed in patients with CNV in 16p13.11 and strengthen the hypothesis that this is a dosage sensitive region with clinical relevance.

Original language	English (US)
Pages (from-to)	280-286
Number of pages	7
Journal	European Journal of Human Genetics
Volume	19
Issue number	3
DOIs	https://doi.org/10.1038/ejhg.2010.184
State	Published - Mar 2011
Externally published	Yes

Keywords

16p13.11
CNV
behavioral abnormality
cognitive impairment

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1038/ejhg.2010.184

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Nagamani, S. C. S., Erez, A., Bader, P., Lalani, S. R., Scott, D. A., Scaglia, F., Plon, S. E., Tsai, C. H., Reimschisel, T., Roeder, E., Malphrus, A. D., Eng, P. A., Hixson, P. M., Kang, S. H. L., Stankiewicz, P., Patel, A., & Cheung, S. W. (2011). Phenotypic manifestations of copy number variation in chromosome 16p13.11. European Journal of Human Genetics, 19(3), 280-286. https://doi.org/10.1038/ejhg.2010.184

Nagamani, SCS, Erez, A, Bader, P, Lalani, SR, Scott, DA, Scaglia, F, Plon, SE, Tsai, CH, Reimschisel, T, Roeder, E, Malphrus, AD, Eng, PA, Hixson, PM, Kang, SHL, Stankiewicz, P, Patel, A & Cheung, SW 2011, 'Phenotypic manifestations of copy number variation in chromosome 16p13.11', European Journal of Human Genetics, vol. 19, no. 3, pp. 280-286. https://doi.org/10.1038/ejhg.2010.184

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title = "Phenotypic manifestations of copy number variation in chromosome 16p13.11",

abstract = "The widespread clinical utilization of array comparative genome hybridization, has led to the unraveling of many new copy number variations (CNVs). Although some of these CNVs are clearly pathogenic, the phenotypic consequences of others, such as those in 16p13.11 remain unclear. Whereas deletions of 16p13.11 have been associated with multiple congenital anomalies, the relevance of duplications of the region is still being debated. We report detailed clinical and molecular characterization of 10 patients with duplication and 4 patients with deletion of 16p13.11. We found that patients with duplication of the region have varied clinical features including behavioral abnormalities, cognitive impairment, congenital heart defects and skeletal manifestations, such as hypermobility, craniosynostosis and polydactyly. These features were incompletely penetrant. Patients with deletion of the region presented with microcephaly, developmental delay and behavioral abnormalities as previously described. The CNVs were of varying sizes and were likely mediated by non-allelic homologous recombination between low copy repeats. Our findings expand the repertoire of clinical features observed in patients with CNV in 16p13.11 and strengthen the hypothesis that this is a dosage sensitive region with clinical relevance.",

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author = "Nagamani, {Sandesh C.Sreenath} and Ayelet Erez and Patricia Bader and Lalani, {Seema R.} and Scott, {Daryl A.} and Fernando Scaglia and Plon, {Sharon E.} and Tsai, {Chun Hui} and Tyler Reimschisel and Elizabeth Roeder and Malphrus, {Amy D.} and Eng, {Patricia A.} and Hixson, {Patricia M.} and Kang, {Sung Hae L.} and Pawel Stankiewicz and Ankita Patel and Cheung, {Sau Wai}",

note = "Funding Information: We thank the participating families for their kind cooperation. This work was supported in part by fellowship grants by the LCRC from Osteogenesis Imperfecta Foundation (SNSC), DK081735-01A1, NIH/NIGMS T32 contract grant number GM07526 (AE). We thank Pengfei Lui for his input on the mechanism of rearrangement.",

year = "2011",

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doi = "10.1038/ejhg.2010.184",

language = "English (US)",

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AU - Nagamani, Sandesh C.Sreenath

AU - Erez, Ayelet

AU - Bader, Patricia

AU - Lalani, Seema R.

AU - Scott, Daryl A.

AU - Scaglia, Fernando

AU - Plon, Sharon E.

AU - Tsai, Chun Hui

AU - Reimschisel, Tyler

AU - Roeder, Elizabeth

AU - Malphrus, Amy D.

AU - Eng, Patricia A.

AU - Hixson, Patricia M.

AU - Kang, Sung Hae L.

AU - Stankiewicz, Pawel

AU - Patel, Ankita

AU - Cheung, Sau Wai

N1 - Funding Information: We thank the participating families for their kind cooperation. This work was supported in part by fellowship grants by the LCRC from Osteogenesis Imperfecta Foundation (SNSC), DK081735-01A1, NIH/NIGMS T32 contract grant number GM07526 (AE). We thank Pengfei Lui for his input on the mechanism of rearrangement.

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N2 - The widespread clinical utilization of array comparative genome hybridization, has led to the unraveling of many new copy number variations (CNVs). Although some of these CNVs are clearly pathogenic, the phenotypic consequences of others, such as those in 16p13.11 remain unclear. Whereas deletions of 16p13.11 have been associated with multiple congenital anomalies, the relevance of duplications of the region is still being debated. We report detailed clinical and molecular characterization of 10 patients with duplication and 4 patients with deletion of 16p13.11. We found that patients with duplication of the region have varied clinical features including behavioral abnormalities, cognitive impairment, congenital heart defects and skeletal manifestations, such as hypermobility, craniosynostosis and polydactyly. These features were incompletely penetrant. Patients with deletion of the region presented with microcephaly, developmental delay and behavioral abnormalities as previously described. The CNVs were of varying sizes and were likely mediated by non-allelic homologous recombination between low copy repeats. Our findings expand the repertoire of clinical features observed in patients with CNV in 16p13.11 and strengthen the hypothesis that this is a dosage sensitive region with clinical relevance.

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Phenotypic manifestations of copy number variation in chromosome 16p13.11

Abstract

Keywords

ASJC Scopus subject areas

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