Do fetal extravillous trophoblasts circulate in maternal blood postpartum?

Looij, Anne Van De; Singh, Ripudaman; Hatt, Lotte; Ravn, Katarina; Jeppesen, Line Dahl; Nicolaisen, Bolette Hestbek; Kølvraa, Mathias; Vogel, Ida; Schelde, Palle; Uldbjerg, Niels

doi:10.1111/aogs.13880

Cited by 12 publications

(6 citation statements)

References 23 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This persistence makes fetal circulating lymphocytes and stem/progenitor cells unsuitable for non‐invasive prenatal testing, as their presence in subsequent pregnancies could confound test results. In contrast, fnRBC and trophoblasts are rapidly cleared from the maternal circulation after delivery, with none detectable ≥8 weeks post‐partum 13 . Primitive erythroblasts from the yolk sac are the first fnRBC to appear at 7‐12 weeks gestation, but disappear after 12w, 14 when definitive erythroblasts, derived from the fetal liver, appear.…”

Section: Fetal and Placental Cells In The Maternal Circulationmentioning

confidence: 99%

“…In contrast, fnRBC and trophoblasts are rapidly cleared from the maternal circulation after delivery, with none detectable ≥8 weeks post-partum. 13 Primitive erythroblasts from the yolk sac are the first fnRBC to appear at 7-12 weeks gestation, but disappear after 12w, 14 when definitive erythroblasts, derived from the fetal liver, appear. The trophoblasts that enter the maternal circulation can originate from different trophoblast cell types.…”

mentioning

confidence: 99%

See 1 more Smart Citation

Overview and recent developments in cell‐based noninvasive prenatal testing

et al. 2021

View full text Add to dashboard Cite

Investigators have long been interested in the natural phenomenon of fetal and placental cell trafficking into the maternal circulation. The scarcity of these circulating cells makes their detection and isolation technically challenging. However, as a DNA source of fetal origin not mixed with maternal DNA, they have the potential of considerable benefit over circulating cell‐free DNA‐based noninvasive prenatal genetic testing (NIPT). Endocervical trophoblasts, which are less rare but more challenging to recover are also being investigated as an approach for cell‐based NIPT. We review published studies from around the world describing both forms of cell‐based NIPT and highlight the different approaches’ advantages and drawbacks. We also offer guidance for developing a sound cell‐based NIPT protocol.

show abstract

Section: Fetal and Placental Cells In The Maternal Circulationmentioning

confidence: 99%

mentioning

confidence: 99%

Overview and recent developments in cell‐based noninvasive prenatal testing

et al. 2021

View full text Add to dashboard Cite

show abstract

“…However, other technical issues may explain these findings as the authors used REPLI‐g Single Cell Kit for WGA, which, following manufacturer's protocol, cannot be used for fixed cells 13 . Recent results published by Weymaere et al (and supplemented by experiences from our laboratory) demonstrate that whole genome amplified DNA from a single fetal extravillous trophoblast using PicoPLEX Single Cell WGA kit (Takara Bio Inc.) is sufficient for STR or SNP genotyping to identify fetal origin of isolated candidate cells 14,15 . Overall, the feasibility of cell‐based NIPT relies not only on an efficient technology for enrichment and isolation of the fetal extravillous trophoblasts, but also on the ability to obtain fetal DNA of a quality sufficient for the genetic analysis.…”

Section: Discussionmentioning

confidence: 96%

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

Jeppesen

Hatt²,

Singh³

et al. 2020

Prenatal Diagnosis

Self Cite

View full text Add to dashboard Cite

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.

show abstract

“…is persistence makes circulating fetal lymphocytes and granulocytes unsuitable for NIPD, as their presence in subsequent pregnancies may influence test results. In contrast, FNRBC and trophoblast cells were cleared from the maternal circulation rapidly after delivery and were not detected after ≥8 weeks [16]. erefore, at present, trophoblast cells and fetal nucleated red cells are mainly studied as fetal cells in prenatal diagnosis.…”

Section: Classification Of Fetal Cells In Maternal Peripheral Bloodmentioning

confidence: 97%

Research Progress in Isolation and Enrichment of Fetal Cells from Maternal Blood

Tang

Luo

et al. 2022

Journal of Chemistry

View full text Add to dashboard Cite

Prenatal diagnosis is an important means of early diagnosis of genetic diseases, which can effectively reduce the risk of birth defects. Free fetal cells, as a carrier of intact fetal genetic material, provide hope for the development of high-sensitivity and high-accuracy prenatal diagnosis technology. However, the number of fetal cells is small and it is difficult to apply clinically. In recent years, noninvasive prenatal diagnosis (NIPD) technology for fetal genetic material in maternal peripheral blood has developed rapidly, which makes it possible to diagnose genetic diseases by fetal cells in maternal peripheral blood. This article reviewed the current status of fetal cell separation and enrichment technology and its application in noninvasive prenatal diagnosis technology.

show abstract

Do fetal extravillous trophoblasts circulate in maternal blood postpartum?

Cited by 12 publications

References 23 publications

Overview and recent developments in cell‐based noninvasive prenatal testing

Overview and recent developments in cell‐based noninvasive prenatal testing

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

Research Progress in Isolation and Enrichment of Fetal Cells from Maternal Blood

Contact Info

Product

Resources

About