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2000 to >30 000 (tiling-path) interrogating BAC/PAC probes have detected chromosome abnormalities in up to 17% of cases. Surprisingly, some of the pathogenic changes are mosaic and not detectable in conventional karyotyping. Commercially available genome-wide microarrays with >300 000 synthesized oligonucleotide probes enable higher resolution and sensitivity and will probably replace the BAC/PAC arrays in clinical laboratories.
doi:10.1016/j.ejmg.2007.01.004 
Copyright © 2007 Elsevier Masson SAS All rights reserved.
Chromosomal imbalance letter
Duplication 16q12.1–q22.1 characterized by array CGH in a girl with spina bifida
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Peter Gustavssona, 
, 
, Jacqueline Schoumansa, Johan Staafb, Åke Borgb, Magnus Nordenskjölda and Göran Annerénc
Received 19 January 2007;
Abstract
We report a 7-year-old girl with spina bifida carrying a complex chromosome abnormality resulting in duplication 16q12.1–q22.1. An abnormal karyotype was identified involving the long arm of chromosome 11 and fluorescent in situ hybridization (FISH) to metaphase chromosomes revealed an insertion of part of chromosome 16 on chromosome 11.
A detailed mapping of the chromosome abnormality using whole genome array based comparative genomic hybridization (CGH) of the patient DNA revealed a duplication 16q12.1–q22.1 corresponding to gain of 19.8 Mb of DNA without any detectable loss of genetic material on chromosome 11. The karyotype is defined as 46,XX,der(11)ins(11;16)(q13;q12.1q22.1).
We present here the clinical findings and a fine mapping of the associated structural chromosome abnormalities. We suggest that a gene dosage imbalance of 16q12.1–q22.1 is associated with spina bifida in the patient.
Keywords: Array CGH; Duplication 16q12.1–q22.1; Spina bifida
