Evidence for feasibility of fetal trophoblastic cell-based noninvasive prenatal testing

Amy M. Breman; Jennifer C. Chow; Lance U'Ren; Elizabeth A. Normand; Sadeem Qdaisat; Li Zhao; David M. Henke; Rui Chen; Chad A. Shaw; Laird Jackson; Yaping Yang; Liesbeth Vossaert; Rachel H.V. Needham; Elizabeth J. Chang; Daniel Campton; Jeffrey L. Werbin; Ron C. Seubert; Ignatia B. Van den Veyver; Jackie L. Stilwell; Eric P. Kaldjian; Arthur L. Beaudet

doi:10.1002/pd.4924

Evidence for feasibility of fetal trophoblastic cell-based noninvasive prenatal testing

Amy M. Breman, Jennifer C. Chow, Lance U'Ren, Elizabeth A. Normand, Sadeem Qdaisat, Li Zhao, David M. Henke, Rui Chen, Chad A. Shaw, Laird Jackson, Yaping Yang, Liesbeth Vossaert, Rachel H.V. Needham, Elizabeth J. Chang, Daniel Campton, Jeffrey L. Werbin, Ron C. Seubert, Ignatia B. Van den Veyver, Jackie L. Stilwell, Eric P. KaldjianArthur L. Beaudet

Research output: Contribution to journal › Article › peer-review

66 Scopus citations

Abstract

Objective: The goal was to develop methods for detection of chromosomal and subchromosomal abnormalities in fetal cells in the mother's circulation at 10–16 weeks' gestation using analysis by array comparative genomic hybridization (CGH) and/or next-generation sequencing (NGS). Method: Nucleated cells from 30 mL of blood collected at 10–16 weeks' gestation were separated from red cells by density fractionation and then immunostained to identify cytokeratin positive and CD45 negative trophoblasts. Individual cells were picked and subjected to whole genome amplification, genotyping, and analysis by array CGH and NGS. Results: Fetal cells were recovered from most samples as documented by Y chromosome PCR, short tandem repeat analysis, array CGH, and NGS including over 30 normal male cells, one 47,XXY cell from an affected fetus, one trisomy 18 cell from an affected fetus, nine cells from a trisomy 21 case, three normal cells and one trisomy 13 cell from a case with confined placental mosaicism, and two chromosome 15 deletion cells from a case known by CVS to have a 2.7 Mb de novo deletion. Conclusion: We believe that this is the first report of using array CGH and NGS whole genome sequencing to detect chromosomal abnormalities in fetal trophoblastic cells from maternal blood.

Original language	English (US)
Pages (from-to)	1009-1019
Number of pages	11
Journal	Prenatal diagnosis
Volume	36
Issue number	11
DOIs	https://doi.org/10.1002/pd.4924
State	Published - Nov 1 2016
Externally published	Yes

ASJC Scopus subject areas

Obstetrics and Gynecology
Genetics(clinical)

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Breman, A. M., Chow, J. C., U'Ren, L., Normand, E. A., Qdaisat, S., Zhao, L., Henke, D. M., Chen, R., Shaw, C. A., Jackson, L., Yang, Y., Vossaert, L., Needham, R. H. V., Chang, E. J., Campton, D., Werbin, J. L., Seubert, R. C., Van den Veyver, I. B., Stilwell, J. L., ... Beaudet, A. L. (2016). Evidence for feasibility of fetal trophoblastic cell-based noninvasive prenatal testing. Prenatal diagnosis, 36(11), 1009-1019. https://doi.org/10.1002/pd.4924

Breman, AM, Chow, JC, U'Ren, L, Normand, EA, Qdaisat, S, Zhao, L, Henke, DM, Chen, R, Shaw, CA, Jackson, L, Yang, Y, Vossaert, L, Needham, RHV, Chang, EJ, Campton, D, Werbin, JL, Seubert, RC, Van den Veyver, IB, Stilwell, JL, Kaldjian, EP & Beaudet, AL 2016, 'Evidence for feasibility of fetal trophoblastic cell-based noninvasive prenatal testing', Prenatal diagnosis, vol. 36, no. 11, pp. 1009-1019. https://doi.org/10.1002/pd.4924

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title = "Evidence for feasibility of fetal trophoblastic cell-based noninvasive prenatal testing",

abstract = "Objective: The goal was to develop methods for detection of chromosomal and subchromosomal abnormalities in fetal cells in the mother's circulation at 10–16 weeks' gestation using analysis by array comparative genomic hybridization (CGH) and/or next-generation sequencing (NGS). Method: Nucleated cells from 30 mL of blood collected at 10–16 weeks' gestation were separated from red cells by density fractionation and then immunostained to identify cytokeratin positive and CD45 negative trophoblasts. Individual cells were picked and subjected to whole genome amplification, genotyping, and analysis by array CGH and NGS. Results: Fetal cells were recovered from most samples as documented by Y chromosome PCR, short tandem repeat analysis, array CGH, and NGS including over 30 normal male cells, one 47,XXY cell from an affected fetus, one trisomy 18 cell from an affected fetus, nine cells from a trisomy 21 case, three normal cells and one trisomy 13 cell from a case with confined placental mosaicism, and two chromosome 15 deletion cells from a case known by CVS to have a 2.7 Mb de novo deletion. Conclusion: We believe that this is the first report of using array CGH and NGS whole genome sequencing to detect chromosomal abnormalities in fetal trophoblastic cells from maternal blood.",

author = "Breman, {Amy M.} and Chow, {Jennifer C.} and Lance U'Ren and Normand, {Elizabeth A.} and Sadeem Qdaisat and Li Zhao and Henke, {David M.} and Rui Chen and Shaw, {Chad A.} and Laird Jackson and Yaping Yang and Liesbeth Vossaert and Needham, {Rachel H.V.} and Chang, {Elizabeth J.} and Daniel Campton and Werbin, {Jeffrey L.} and Seubert, {Ron C.} and {Van den Veyver}, {Ignatia B.} and Stilwell, {Jackie L.} and Kaldjian, {Eric P.} and Beaudet, {Arthur L.}",

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year = "2016",

month = nov,

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doi = "10.1002/pd.4924",

language = "English (US)",

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AU - Breman, Amy M.

AU - Chow, Jennifer C.

AU - U'Ren, Lance

AU - Normand, Elizabeth A.

AU - Qdaisat, Sadeem

AU - Zhao, Li

AU - Henke, David M.

AU - Chen, Rui

AU - Shaw, Chad A.

AU - Jackson, Laird

AU - Yang, Yaping

AU - Vossaert, Liesbeth

AU - Needham, Rachel H.V.

AU - Chang, Elizabeth J.

AU - Campton, Daniel

AU - Werbin, Jeffrey L.

AU - Seubert, Ron C.

AU - Van den Veyver, Ignatia B.

AU - Stilwell, Jackie L.

AU - Kaldjian, Eric P.

AU - Beaudet, Arthur L.

PY - 2016/11/1

Y1 - 2016/11/1

N2 - Objective: The goal was to develop methods for detection of chromosomal and subchromosomal abnormalities in fetal cells in the mother's circulation at 10–16 weeks' gestation using analysis by array comparative genomic hybridization (CGH) and/or next-generation sequencing (NGS). Method: Nucleated cells from 30 mL of blood collected at 10–16 weeks' gestation were separated from red cells by density fractionation and then immunostained to identify cytokeratin positive and CD45 negative trophoblasts. Individual cells were picked and subjected to whole genome amplification, genotyping, and analysis by array CGH and NGS. Results: Fetal cells were recovered from most samples as documented by Y chromosome PCR, short tandem repeat analysis, array CGH, and NGS including over 30 normal male cells, one 47,XXY cell from an affected fetus, one trisomy 18 cell from an affected fetus, nine cells from a trisomy 21 case, three normal cells and one trisomy 13 cell from a case with confined placental mosaicism, and two chromosome 15 deletion cells from a case known by CVS to have a 2.7 Mb de novo deletion. Conclusion: We believe that this is the first report of using array CGH and NGS whole genome sequencing to detect chromosomal abnormalities in fetal trophoblastic cells from maternal blood.

AB - Objective: The goal was to develop methods for detection of chromosomal and subchromosomal abnormalities in fetal cells in the mother's circulation at 10–16 weeks' gestation using analysis by array comparative genomic hybridization (CGH) and/or next-generation sequencing (NGS). Method: Nucleated cells from 30 mL of blood collected at 10–16 weeks' gestation were separated from red cells by density fractionation and then immunostained to identify cytokeratin positive and CD45 negative trophoblasts. Individual cells were picked and subjected to whole genome amplification, genotyping, and analysis by array CGH and NGS. Results: Fetal cells were recovered from most samples as documented by Y chromosome PCR, short tandem repeat analysis, array CGH, and NGS including over 30 normal male cells, one 47,XXY cell from an affected fetus, one trisomy 18 cell from an affected fetus, nine cells from a trisomy 21 case, three normal cells and one trisomy 13 cell from a case with confined placental mosaicism, and two chromosome 15 deletion cells from a case known by CVS to have a 2.7 Mb de novo deletion. Conclusion: We believe that this is the first report of using array CGH and NGS whole genome sequencing to detect chromosomal abnormalities in fetal trophoblastic cells from maternal blood.

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Evidence for feasibility of fetal trophoblastic cell-based noninvasive prenatal testing

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