Cell-based non-invasive prenatal diagnosis in a pregnancy at risk of cystic fibrosis

产科 妊娠期 胎龄
作者
Line Dahl Jeppesen,Lotte Hatt,Ripudaman Singh,Katarina Ravn,Mathias Kølvraa,Palle Schelde,Niels Uldbjerg,Ida Vogel,Dorte L Lildballe
出处
期刊:Prenatal Diagnosis [Wiley]
卷期号:41 (2): 234-240 被引量:5
标识
DOI:10.1002/pd.5861
摘要

Objective We aimed to develop cell-based NIPT for cystic fibrosis (CF) and test a pregnancy at risk of two common pathogenic variants. Method A pregnant woman carrying monozygotic twins opted for prenatal testing as she and her partner were heterozygote carriers of F508del (c.1521:1523del). The partner was also positive for the CFTR-related variant R117H (c.350G>A). Fetal trophoblasts from maternal blood were enriched and isolated using antibodies and a capillary-based cell-picking instrument. Multiplex PCR-based fragment length analysis was performed on the extracted fetal DNA for STR-genotyping, fetal gender and F508del variant status. The R117H variant status was tested using SNaPshot analysis. Results The fetal origin of the isolated cells was verified by detection of two paternally inherited STR alleles and an Y chromosome marker, while no maternal DNA contamination was detected. The direct variant analysis detected F508del heterozygosity and the SNaPshot analysis for R117H detected only the normal allele. Thus, the results showed that the fetuses were healthy carriers of F508del, concordant with the findings of conventional prenatal testing. Conclusion Cell-based NIPT could accurately state the fetal variant status and distinguish fetal trophoblasts from maternal cells. In the future, cell-based NIPT may provide an accurate less invasive alternative to chorionic villous sampling.
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