Complete discrepancy between abnormal fetal karyotypes predicted by QF-PCR rapid testing and karyotyped cultured cells in a first-trimester CVS |
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| Authors: | Jonathan J. Waters Sally Walsh Lisa J. Levett Stuart Liddle Yinka Akinfenwa |
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| Affiliation: | 1. Cytogenetics Laboratory, NE Thames Regional Genetics Service, Gt Ormond St Hospital, London WC1N 3BG, UK;2. Cytogenetic DNA Services Ltd, TDL Genetics, Whitfield St, London W1T 4EU, UK;3. Department of Obstetrics and Gynaecology, Homerton University Hospital, Homerton row, London E9 6SR, UK |
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| Abstract: | ![]()
A chorion villus sample (CVS) biopsied at 11 weeks' gestation for raised nuchal translucency, revealed monosomy X (presumptive 45,X karyotype) by QF-PCR for rapid aneuploidy testing for chromosomes 13, 18, 21, X and Y. Long-term culture gave the karyotype: 47,XY,+ 21[66]/49,XYY,+ 21,+ 21 [22]. This discrepancy prompted redigestion of the combined residual villus fragments from the original QF-PCR assay. The repeat QF-PCR assay identified the presence of trisomy 21 and a Y chromosome consistent with a 47,XY,+ 21 karyotype. A double non-disjunction event early in embryogenesis in a 47,XY,+ 21 conceptus with subsequent cell lineage compartmentalisation of the three observed cell lines (45,X; 47,XY,+ 21 and 49,XYY,+ 21,+ 21) would account for these results. This is the first reported case to describe complete discrepancy at diagnosis between abnormal karyotypes detected by QF-PCR rapid aneuploidy testing and a cultured karyotype in the same CVS. Copyright © 2006 John Wiley & Sons, Ltd. |
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| Keywords: | prenatal diagnosis QF-PCR Down syndrome confined placental mosaicism |
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