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Stem Cell-Based Trophoblast Models to Unravel the Genetic Causes of Human Miscarriages

Journal

CELLS
Volume 11, Issue 12, Pages -

Publisher

MDPI
DOI: 10.3390/cells11121923

Keywords

miscarriage; recurrent pregnancy loss; trophoblast; trophoblast stem cells; trophoblast organoid; extended blastocyst culture; aneuploidy; mosaicism

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Funding

  1. Russian Science Foundation [21-65-00017]
  2. Russian Science Foundation [21-65-00017] Funding Source: Russian Science Foundation

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Miscarriage is a common issue, affecting around 15% of clinically recognized pregnancies, with 1-3% of couples experiencing recurrent pregnancy loss. Chromosomal abnormalities account for approximately 50-60% of miscarriages, while variants in candidate genes play a role in up to 60% of recurrent abortions with euploid fetuses. This review discusses the use of state-of-the-art human in vitro trophoblast models to study specific abnormalities/variants implicated in pregnancy loss. These models provide valuable insights into the impact of genetic variants on placental development and pregnancy outcomes.
Miscarriage affects approximately 15% of clinically recognized pregnancies, and 1-3% of couples experience pregnancy loss recurrently. Approximately 50-60% of miscarriages result from chromosomal abnormalities, whereas up to 60% of euploid recurrent abortions harbor variants in candidate genes. The growing number of detected genetic variants requires an investigation into their role in adverse pregnancy outcomes. Since placental defects are the main cause of first-trimester miscarriages, the purpose of this review is to provide a survey of state-of-the-art human in vitro trophoblast models that can be used for the functional assessment of specific abnormalities/variants implicated in pregnancy loss. Since 2018, when primary human trophoblast stem cells were first derived, there has been rapid growth in models of trophoblast lineage. It has been found that a proper balance between self-renewal and differentiation in trophoblast progenitors is crucial for the maintenance of pregnancy. Different responses to aneuploidy have been shown in human embryonic and extra-embryonic lineages. Stem cell-based models provide a powerful tool to explore the effect of a specific aneuploidy/variant on the fetus through placental development, which is important, from a clinical point of view, for deciding on the suitability of embryos for transfer after preimplantation genetic testing for aneuploidy.

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