How to Cite this Article: Jobanputra V, Burke A, Kwame A-Y, Shanmugham A, Shirazi M, Brown S, Warburton PE, Levy B, Warburton D. 2012. Duplication of the ZIC2 gene is not associated with holoprosencephaly. Am J Med Genet Part A 158A:103–108.
Duplication of the ZIC2 gene is not associated with holoprosencephaly†
Version of Record online: 21 NOV 2011
Copyright © 2011 Wiley Periodicals, Inc.
American Journal of Medical Genetics Part A
Volume 158A, Issue 1, pages 103–108, January 2012
How to Cite
Jobanputra, V., Burke, A., Kwame, A.-Y., Shanmugham, A., Shirazi, M., Brown, S., Warburton, P. E., Levy, B. and Warburton, D. (2012), Duplication of the ZIC2 gene is not associated with holoprosencephaly. Am. J. Med. Genet., 158A: 103–108. doi: 10.1002/ajmg.a.34375
- Issue online: 19 DEC 2011
- Version of Record online: 21 NOV 2011
- Manuscript Accepted: 17 OCT 2011
- Manuscript Received: 15 APR 2011
- National Center for Research Resources. Grant Number: KL2 RR024157
- chromosome 13q32;
- prenatal diagnosis
Cytogenetic testing using genomic microarrays presents a clinical challenge when data regarding the phenotypic consequences of the genomic alteration are not available. We describe a chromosome 13q32.3 duplication discovered by microarray testing in a fetus with a prenatally detected apparently balanced de novo translocation 46,XY,t(2;13)(q37;q32). Microarray analysis on the fetal DNA showed duplications of 384 and 564 kb at the breakpoint regions on chromosomes 2q37.3 and 13q32.3, respectively. There were no disease-associated genes in the duplicated region on chromosome 2q37. The duplicated region on chromosome 13q contains the ZIC2 gene. Haploinsufficiency of ZIC2 is known to cause holoprosencephaly and other brain malformations. Studies in the mouse models have suggested that over expression of ZIC2 may also lead to brain malformations. Fetal MRI of the brain was normal and the family elected to continue the pregnancy. An apparently normal baby was born at term. At 3 months of age a physical exam showed no abnormalities and no developmental delay. This report shows that duplication of ZIC2 is not necessarily associated with brain malformations. We also describe the phenotype from four additional patients with duplications of the region of chromosome 13 containing ZIC2 and three previously described patients with supernumerary marker chromosomes derived from distal chromosome 13. None of the eight patients had holoprosencephaly or brain malformations, indicating that duplication of ZIC2 is not associated with brain anomalies. This information will be useful for counseling in other occurrences of this duplication identified by microarray. © 2011 Wiley Periodicals, Inc.