O-302 Triploid conceptions are predominantly caused by female meiosis II errors and their risk increases with advancing maternal age

Picchetta, L; Figliuzzi, Matteo; Poli, Maurizio; Zhan, Yiping; Caroselli, Silvia; Tao, Xin; Jalas, C; Capalbo, Antonio

doi:10.1093/humrep/dead093.366

Human Reproduction

2023

DOI: 10.1093/humrep/dead093.366

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O-302 Triploid conceptions are predominantly caused by female meiosis II errors and their risk increases with advancing maternal age

L Picchetta¹,

Matteo Figliuzzi²,

Maurizio Poli³

et al.

Abstract: Study question What are the incidence and origin of ploidy abnormalities in embryos derived from 2 pronuclei (2PN) zygotes, and is their risk linked to maternal age? Summary answer While embryo haploidy is usually due to male meiosis errors, triploidy is mainly caused by female meiosis II errors, whose incidence increases with maternal age. What is known already … Show more

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2024

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Incidence of haploidy and triploidy in trophectoderm biopsies of blastocysts derived from normally and abnormally fertilized oocytes

Girardi,

Patassini,

Miravet Valenciano

et al. 2024

J Assist Reprod Genet

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Incidence of haploidy and triploidy in trophectoderm biopsies of blastocysts derived from normally and abnormally fertilized oocytes

Girardi,

Patassini,

Miravet Valenciano

et al. 2024

J Assist Reprod Genet

View full text Add to dashboard Cite

An expert opinion on rescuing atypically pronucleated human zygotes by molecular genetic fertilization checks in IVF

Capalbo,

Cimadomo,

Coticchio

et al. 2024

Human Reproduction

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IVF laboratories routinely adopt morphological pronuclear assessment at the zygote stage to identify abnormally fertilized embryos deemed unsuitable for clinical use. In essence, this is a pseudo-genetic test for ploidy motivated by the notion that biparental diploidy is required for normal human life and abnormal ploidy will lead to either failed implantation, miscarriage, or significant pregnancy complications, including molar pregnancy and chorionic carcinoma. Here, we review the literature associated with ploidy assessment of human embryos derived from zygotes displaying a pronuclear configuration other than the canonical two, and the related pregnancy outcome following transfer. We highlight that pronuclear assessment, although associated with aberrant ploidy outcomes, has a low specificity in the prediction of abnormal ploidy status in the developing embryo, while embryos deemed abnormally fertilized can yield healthy pregnancies. Therefore, this universal strategy of pronuclear assessment invariably leads to incorrect classification of over 50% of blastocysts derived from atypically pronucleated zygotes, and the systematic disposal of potentially viable embryos in IVF. To overcome this limitation of current practice, we discuss the new preimplantation genetic testing technologies that enable accurate identification of the ploidy status of preimplantation embryos and suggest a progress from morphology-based checks to molecular fertilization check as the new gold standard. This alternative molecular fertilization checking represents a possible non-incremental and controversy-free improvement to live birth rates in IVF as it adds to the pool of viable embryos available for transfer. This is especially important for the purposes of ‘family building’ or for poor-prognosis IVF patients where embryo numbers are often limited.

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O-302 Triploid conceptions are predominantly caused by female meiosis II errors and their risk increases with advancing maternal age

Cited by 2 publications

References 0 publications

Incidence of haploidy and triploidy in trophectoderm biopsies of blastocysts derived from normally and abnormally fertilized oocytes

Incidence of haploidy and triploidy in trophectoderm biopsies of blastocysts derived from normally and abnormally fertilized oocytes

An expert opinion on rescuing atypically pronucleated human zygotes by molecular genetic fertilization checks in IVF

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