AI Article Synopsis

  • Chromosomal polymorphisms (CPMs) are typically harmless genetic variations, but some studies suggest they might be linked to reproductive issues, particularly in patients with chromosomal translocations (CT).
  • This study analyzed data from 26 patients with CPM and 56 controls with normal chromosomes, assessing fertilization and embryonic development metrics during preimplantation genetic testing between 2013 and 2019.
  • The findings indicated no significant differences in fertilization and cleavage rates between CPM and normal chromosomes; however, the high-quality blastocyst rate was notably lower for those with CTCPM compared to regular CT, suggesting that CPM may adversely affect embryo quality and development, especially in male carriers.

Article Abstract

Traditionally, chromosomal polymorphisms (CPMs) are normal genetic variants in individuals with no phenotypic variations. However, some studies have shown that CPM is related to reproductive diseases. We explored the influence of CPM on embryonic development and molecular karyotype in chromosomal translocation (CT) patients undergoing preimplantation genetic testing (PGT) between February 2013 and May 2019. Twenty-six cases with CPM and 56 controls with normal chromosomes were included. Furthermore, a 1:4 match pair analysis by female age included 39 cases with CTCPM and 185 controls with CT. There was no statistical difference in fertilization rate (78.48% vs. 78.33%), cleavage rate on Day 3 (90.32% vs. 89.16%), blastocyst rate (60.00% vs. 60.80%), and the high-quality blastocyst rate (36.31% vs. 35.22%) between CPM and normal chromosomes. The high-quality blastocyst rate of CTCPM was significantly lower than that for CT (26.78% vs. 38.89%). Moreover, there was no statistical difference in fertilization rate (70.65% vs. 70.37%), cleavage rate on Day 3 (88.67% vs. 89.53%), and blastocyst rate (48.48% vs. 53.17%) between CTCPM and CT. In addition, one CTCPM spouse had a lower high-quality blastocyst rate, especially of males with CTCPM. Abnormal embryo rates of CTCPM were significantly higher than those for CT (78.64% vs. 68.93%). Abnormal embryo rates were higher in both CTCPM and CPM paternal carriers with CT partners, respectively. For CT, CTCPM may have an impact on the high-quality blastocyst rate and embryonic molecular karyotype, especially in male patients. Patients with CTCPM are relatively rare, but this population would benefit from being explored using a larger sample size.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7726188PMC
http://dx.doi.org/10.3389/fphys.2020.543188DOI Listing

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