Embryo morphology, developmental rates, and maternal age are correlated with chromosome abnormalities
- PMID: 7615118
Embryo morphology, developmental rates, and maternal age are correlated with chromosome abnormalities
Corrected and republished in
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Reprint of: Embryo morphology, developmental rates, and maternal age are correlated with chromosome abnormalities.Fertil Steril. 2019 Oct;112(4 Suppl1):e71-e80. doi: 10.1016/j.fertnstert.2019.08.076. Fertil Steril. 2019. PMID: 31623745 No abstract available.
Abstract
Objective: To determine some of the unresolved questions related to chromosome anomalies in early human embryos, such are the detection of any advanced maternal age effect; the complete assessment of mosaicism, which requires analysis of all cells; and the relationship with embryonic dysmorphism. Fluorescence in situ hybridization has been used in this study to answer these issues.
Design: Fluorescence in situ hybridization analysis of human embryos using simultaneously probes for three or five chromosomes. Five hundred twenty-four cleavage-stage human embryos obtained by IVF were analyzed by fluorescence in situ hybridization. Embryos were allocated into three groups according to morphological and developmental characteristics (arrested; slow and/or fragmented; morphologically and developmentally normal). The embryos also were analyzed according to maternal age.
Results: Dysmorphic embryos had higher rates of polyploidy and diploid mosaicism. Aneuploidy increased with maternal age in nonarrested embryos. Preimplantation genetic diagnosis successfully detected these abnormalities.
Conclusion: This study demonstrates that, in morphologically and developmentally normal human embryos, cleavage-stage aneuploidy significantly increases with maternal age. The results suggest that implantation failure in older women largely could be due to aneuploidy.
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