TY - JOUR
T1 - Fetoplacental mosaicism
T2 - Potential implications for false-positive and false-negative noninvasive prenatal screening results
AU - Grati, Francesca R.
AU - Malvestiti, Francesca
AU - Ferreira, Jose C.P.B.
AU - Bajaj, Komal
AU - Gaetani, Elisa
AU - Agrati, Cristina
AU - Grimi, Beatrice
AU - Dulcetti, Francesca
AU - Ruggeri, Anna M.
AU - De Toffol, Simona
AU - Maggi, Federico
AU - Wapner, Ronald
AU - Gross, Susan
AU - Simoni, Giuseppe
PY - 2014/8
Y1 - 2014/8
N2 - Purpose:Noninvasive prenatal screening for fetal aneuploidy analyzes cell-free fetal DNA circulating in the maternal plasma. Because cell-free fetal DNA is mainly of placental trophoblast origin, false-positive and false-negative findings may result from placental mosaicism. The aim of this study was to calculate the potential contribution of placental mosaicism in discordant results of noninvasive prenatal screening.Methods:We performed a retrospective audit of 52,673 chorionic villus samples in which cytogenetic analysis of the cytotrophoblast (direct) and villus mesenchyme (culture) was performed, which was followed by confirmatory amniocentesis in chorionic villi mosaic cases. Using cases in which cytogenetic discordance between cytotrophoblast and amniotic fluid samples was identified, we calculated the potential contribution of cell line-specific mosaicism to false-positive and false-negative results of noninvasive prenatal screening.Results:The false-positive rate, secondary to the presence of abnormal cell line with common trisomies in cytotrophoblast and normal amniotic fluid, ranged from 1/1,065 to 1/3,931 at 10% and 100% mosaicism, respectively; the false-negative rate was calculated from cases of true fetal mosaicism, in which a mosaic cell line was absent in cytotrophoblast and present in the fetus; this occurred in 1/107 cases.Conclusion:Despite exciting advances, underlying biologic mechanisms will never allow 100% sensitivity or specificity.
AB - Purpose:Noninvasive prenatal screening for fetal aneuploidy analyzes cell-free fetal DNA circulating in the maternal plasma. Because cell-free fetal DNA is mainly of placental trophoblast origin, false-positive and false-negative findings may result from placental mosaicism. The aim of this study was to calculate the potential contribution of placental mosaicism in discordant results of noninvasive prenatal screening.Methods:We performed a retrospective audit of 52,673 chorionic villus samples in which cytogenetic analysis of the cytotrophoblast (direct) and villus mesenchyme (culture) was performed, which was followed by confirmatory amniocentesis in chorionic villi mosaic cases. Using cases in which cytogenetic discordance between cytotrophoblast and amniotic fluid samples was identified, we calculated the potential contribution of cell line-specific mosaicism to false-positive and false-negative results of noninvasive prenatal screening.Results:The false-positive rate, secondary to the presence of abnormal cell line with common trisomies in cytotrophoblast and normal amniotic fluid, ranged from 1/1,065 to 1/3,931 at 10% and 100% mosaicism, respectively; the false-negative rate was calculated from cases of true fetal mosaicism, in which a mosaic cell line was absent in cytotrophoblast and present in the fetus; this occurred in 1/107 cases.Conclusion:Despite exciting advances, underlying biologic mechanisms will never allow 100% sensitivity or specificity.
KW - cell-free placental DNA
KW - false-negative rate
KW - false-positive rate
KW - fetoplacental mosaicism
KW - noninvasive prenatal screening
UR - http://www.scopus.com/inward/record.url?scp=84905571246&partnerID=8YFLogxK
U2 - 10.1038/gim.2014.3
DO - 10.1038/gim.2014.3
M3 - Article
C2 - 24525917
AN - SCOPUS:84905571246
SN - 1098-3600
VL - 16
SP - 620
EP - 624
JO - Genetics in Medicine
JF - Genetics in Medicine
IS - 8
ER -