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Cell-free fetal DNA and intact fetal cells in maternal blood circulation: implications for first and second trimester non-invasive prenatal diagnosis
Authors:Bischoff Farideh Z  Sinacori Mina K  Dang Dianne D  Marquez-Do Deborah  Horne Cassandra  Lewis Dorothy E  Simpson Joe Leigh
Institution:Department of Obstetrics and Gynecology, Baylor College of Medicine, Houston, Texas 77030, USA. bischoff@bcm.tmc.edu
Abstract:Both intact fetal cells as well as cell-free fetal DNA are present in the maternal circulation and can be recovered for non-invasive prenatal genetic diagnosis. Although methods for enrichment and isolation of rare intact fetal cells have been challenging, diagnosis of fetal chromosomal aneuploidy including trisomy 21 in first- and second-trimester pregnancies has been achieved with a 50-75% detection rate. Similarly, cell-free fetal DNA can be reliably recovered from maternal plasma and assessed by quantitative PCR to detect fetal trisomy 21 and paternally derived single gene mutations. Real-time PCR assays are robust in detecting low-level fetal DNA concentrations, with sensitivity of approximately 95-100% and specificity near 100%. Comparing intact fetal cell versus cell-free fetal DNA methods for non-invasive prenatal screening for fetal chromosomal aneuploidy reveals that the latter is at least four times more sensitive. These preliminary results do not support a relationship between frequency of intact fetal cells and concentration of cell-free fetal DNA. The above results imply that the concentration of fetal DNA in maternal plasma may not be dependent on circulating intact fetal cells but rather be a product of growth and cellular turnover during embryonic or fetal development.
Keywords:cell-free fetal DNA in maternal plasma /  fetal cells in maternal blood /  fetal chromosomal aneuploidy /  non-invasive prenatal diagnosis /  real-time quantitative PCR
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