Publication details

Concordance of various chromosomal errors among different parts of the embryo and the value of re-biopsy in embryos with segmental aneuploidies

Authors	NAVRÁTIL Rostislav HORAK Jakub HORNAK Miroslav KUBICEK David BALCOVA Maria TAUWINKLOVA Gabriela TRAVNIK Pavel VESELA Katerina
Year of publication	2020
Type	Article in Periodical
Magazine / Source	Molecular Human Reproduction
MU Faculty or unit	Faculty of Science
Citation
Web	https://doi.org/10.1093/molehr/gaaa012
Doi	http://dx.doi.org/10.1093/molehr/gaaa012
Keywords	preimplantation genetic testing for aneuploidy; segmental aneuploidy; mosaicism; embryo re-biopsy; massive parallel sequencing; concordance of chromosomal errors; infertility; ART
Description	Chromosomal mosaicism detected during preimplantation genetic testing for aneuploidy (PGT-A) and its impact on embryo implantation have been widely discussed, and healthy live births from mosaic embryos were reported by many groups. On the other hand, only very few studies have focused on segmental chromosome aneuploidies and their clinical impact. Eighty-nine embryos with various PGT-A results (trophectoderm 1: TE1) were re-analysed using a second trophectoderm biopsy (TE2) and the rest of the embryo (RE) for testing. Of 19 euploid TE1 biopsies, 18 were concordant across TE2 and RE. Similarly, whole chromosomal aneuploidies were concordant in 59 of 62 TE1-TE2 and 58 TE1-RE. In contrast, from 31 segmental aneuploidies detected in TE1, only 15 were observed again in TE2 and 14 in RE. If a TE1 segmental abnormality appeared again in TE2, it was almost always present in RE (17/18) as well. Moreover, when a TE1 segmental abnormality was not detected in TE2, in 12 out of 13 cases RE was also unaffected. Similarly, only 1 of 26 TE1 whole chromosome mosaics were repeated in TE2 and 7 in RE. Our study confirms that euploid and whole chromosomal aneuploidy results are highly predictive of the embryo. In contrast, mosaicism has a very low concordance rate. Most importantly, re-biopsy of embryos with segmental aneuploidies demonstrated that they are mostly not uniform across the embryo. Finally, in the case of segmental aneuploidy, the second biopsy enables an accurate prediction of the real status of the embryo and could be offered to patients undergoing PGT-A.