Single-cell DNA sequencing reveals a high incidence of chromosomal abnormalities in human blastocysts
Effrosyni A. Chavli, … , Geert J.P.L. Kops, Esther B. Baart
Effrosyni A. Chavli, … , Geert J.P.L. Kops, Esther B. Baart
Published January 4, 2024
Citation Information: J Clin Invest. 2024;134(6):e174483. https://doi.org/10.1172/JCI174483.
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Research Article Genetics Reproductive biology

Single-cell DNA sequencing reveals a high incidence of chromosomal abnormalities in human blastocysts

Abstract

Aneuploidy, a deviation from the normal chromosome copy number, is common in human embryos and is considered a primary cause of implantation failure and early pregnancy loss. Meiotic errors lead to uniformly abnormal karyotypes, while mitotic errors lead to chromosomal mosaicism: the presence of cells with at least 2 different karyotypes within an embryo. Knowledge about mosaicism in blastocysts mainly derives from bulk DNA sequencing (DNA-Seq) of multicellular trophectoderm (TE) and/or inner cell mass (ICM) samples. However, this can only detect an average net gain or loss of DNA above a detection threshold of 20%–30%. To accurately assess mosaicism, we separated the TE and ICM of 55 good-quality surplus blastocysts and successfully applied single-cell whole-genome sequencing (scKaryo-Seq) on 1,057 cells. Mosaicism involving numerical and structural chromosome abnormalities was detected in 82% of the embryos, in which most abnormalities affected less than 20% of the cells. Structural abnormalities, potentially caused by replication stress and DNA damage, were observed in 69% of the embryos. In conclusion, our findings indicated that mosaicism was prevalent in good-quality blastocysts, whereas these blastocysts would likely be identified as normal with current bulk DNA-Seq techniques used for preimplantation genetic testing for aneuploidy.

Authors

Effrosyni A. Chavli, Sjoerd J. Klaasen, Diane Van Opstal, Joop S.E. Laven, Geert J.P.L. Kops, Esther B. Baart

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Figure 2

Chromosomal abnormalities in the TE versus the ICM.

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Chromosomal abnormalities in the TE versus the ICM. (A) Proportion of ab...
(A) Proportion of abnormal cells in the TE versus the ICM per embryo (n = 52). Data indicate the mean ± SEM. P = 0.26, by Fisher’s exact test. Embryos in which the TE and ICM were not separated are excluded. (B) Percentage of complex abnormal cells in the TE (n = 58 of 812) versus the ICM (n = 4 of 160). P = 0.03, by Fisher’s exact test. Complex cells have more than 4 chromosomal abnormalities. (C) Percentage of embryos that shared a mitotic abnormality in the embryonic lineages and percentage of embryos that had only abnormalities restricted to either the ICM or the TE. (D) Percentage of mitotic events that led to shared or restricted mitotic abnormalities in the embryonic lineages.