Two clinical case reports of embryonic mosaicism identified with PGT-A persisting during pregnancy as true fetal mosaicism

羊膜穿刺术 绒毛取样 非整倍体 胎儿 怀孕 胚胎 生物 胎盘 产前诊断 概念产品 绒毛 三体 产科 胚胎干细胞 基因检测 男科 遗传学 妊娠期 医学 染色体 基因
作者
Ermanno Greco,Pavel Yakovlev,N. N. Kornilov,Svetlana Vyatkina,Daria Bogdanova,Marina Ermakova,Yulia Tarasova,Andrei V. Tikhonov,Anna A. Pendina,Anıl Biricik,Maria Teresa Sessa,Ilaria Listorti,Carlo Ronsini,Pierfrancesco Greco,Andrea R. Victor,Frank L. Barnes,Christo Zouves,Francesca Spinella,Manuel Viotti
出处
期刊:Human Reproduction [Oxford University Press]
卷期号:38 (2): 315-323 被引量:23
标识
DOI:10.1093/humrep/deac263
摘要

The health risks associated with transferring embryos classified as mosaic by preimplantation genetic testing for aneuploidies (PGT-A) are currently unknown. Such embryos produce PGT-A results indicating the presence of both euploid and aneuploid cells and have historically been deselected from transfer and grouped with uniformly aneuploid embryos as 'abnormal'. In recent years, numerous groups have reported the intentional transfer of mosaic embryos in the absence of uniformly euploid embryos, largely observing births of seemingly healthy babies. However, it remains to be understood whether the embryonic mosaicism invariably becomes resolved during the ensuing pregnancy, or whether the placenta and/or fetal tissues retain aneuploid cells, and if so to what potential clinical effect. Here, we report two cases of mosaicism persisting from the embryonic stage to the established pregnancy. Case 1 involved an embryonic low-level segmental mosaic loss in Chromosome (Chr) 1, which was confirmed in amniocentesis as well as in brain tissue of the products of conception. This pregnancy was terminated due to the chromosomal pathologies associated with 1p36 deletion syndrome, such as severe intellectual disability. Case 2 involved a low-level mosaic Chr 21 trisomy, which was confirmed with chorionic villus sampling and amniocentesis. The ensuing pregnancy was terminated after ultrasound identification of severe abnormalities in the placenta and fetus. Together, these two cases should be taken into account for risk-benefit assessments of prospective mosaic embryo transfers.
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