Clinical outcome and follow‐up of the first reported case of Russell‐Silver syndrome with the unique combination of maternal uniparental heterodisomy 7 and mosaic trisomy 7
- 8 July 2005
- journal article
- case report
- Published by Wiley in Birth Defects Research Part A: Clinical and Molecular Teratology
- Vol. 73 (8) , 577-582
- https://doi.org/10.1002/bdra.20174
Abstract
BACKGROUND Russell‐Silver syndrome (RSS) has been associated with maternal uniparental disomy (UPD) for chromosome 7 although the etiology of the syndrome is still unknown. Cases of RSS associated with maternal UPD7 have involved isodisomies, heterodisomies, and mixed isodisomy with heterodisomy simultaneously. This publication is a follow‐up report of the postnatal clinical outcome of the first prenatally suspected case of combined mosaic trisomy 7 with maternal uniparental disomy of chromosome 7 (UPD7). CASE The diagnosis of RSS in the proband was suspected prenatally because trisomy 7 mosaicism (47,XX,+7[13]/46,XX[19]) and maternal uniparental heterodisomy 7 were both found in amniotic fluid cells. Cord blood karyotype analysis showed only disomic cells (46,XX[50]), whereas postpartum chorionic villus analysis was completely trisomic for chromosome 7 (47,XX,+7[19]). Postnatally, the diagnosis of RSS was confirmed by physical findings, her trisomy 7 mosaicism was confirmed by cytogenetic analysis of her skin biopsy (47,XX,+7[9]/46,XX[20]) and her UPD7 was confirmed on both peripheral blood and skin biopsy using microsatellite markers. During infancy, the proband experienced growth deficiency, persistent hypoglycemia, and psychomotor developmental delay. CONCLUSIONS Trisomic rescue as a life‐saving mechanism, with subsequent chromosomal mosaicism in combination with UPD may occur more frequently in RSS than has been reported. Systematic testing of cases suspected prenatally or postnatally would be informative regarding the individual contribution of each factor. Imprinting, loss of heterozygosity for recessive genes, and mosaicism may explain the short stature, asymmetry, and the variable expression of the phenotype. The contribution of these mechanisms to the syndrome should be evaluated in these cases. Birth Defects Research (Part A), 2005.Keywords
This publication has 36 references indexed in Scilit:
- Prenatal diagnosis of a trisomy 7/maternal uniparental heterodisomy 7 mosaic fetusAmerican Journal of Medical Genetics Part A, 2002
- Low incidence of UPD in spontaneous abortions beyond the 5th gestational weekEuropean Journal of Human Genetics, 2001
- Do patients with maternal uniparental disomy for chromosome 7 have a distinct mild Silver-Russell phenotype?Journal of Medical Genetics, 2001
- The contribution of uniparental disomy to congenital development defects in children born to mothers at advanced childbearing ageAmerican Journal of Medical Genetics, 2000
- Human GRB10 is imprinted and expressed from the paternal and maternal allele in a highly tissue- and isoform-specific fashionHuman Molecular Genetics, 2000
- Genomic Imprinting and Uniparental DisomyPublished by Springer Nature ,1999
- RARE TRISOMY MOSAICISM DIAGNOSED IN AMNIOCYTES, INVOLVING AN AUTOSOME OTHER THAN CHROMOSOMES 13, 18, 20, AND 21: KARYOTYPE/PHENOTYPE CORRELATIONSPrenatal Diagnosis, 1997
- Mosaicism in Human SkinArchives of Dermatology, 1993
- Hypomelanosis of Ito associated with mosaicism for trisomy 7 and apparent 'pseudomosaicism' at amniocentesis.Journal of Medical Genetics, 1993
- A new genetic concept: Uniparental disomy and its potential effect, isodisomyAmerican Journal of Medical Genetics, 1980