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Combined Preimplantation Genetic Testing for Autosomal Dominant Polycystic Kidney Disease: Consequences for Embryos Available for Transfer

机译:常染色体显性多囊肾疾病的联合植入前遗传学测试:可用于移植的胚胎的后果

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摘要

Autosomal dominant polycystic kidney disease (ADPKD) is the most common hereditary kidney disease and presents with genetic and clinical heterogeneity. ADPKD can also manifest extra-renally, and seminal cysts have been associated with male infertility in some cases. ADPKD-linked male infertility, along with female age, have been proposed as factors that may influence the clinical outcomes of preimplantation genetic testing (PGT) for monogenic disorders (PGT-M). Large PGT for aneuploidy assessment (PGT-A) studies link embryo aneuploidy to increasing female age; other studies suggest that embryo aneuploidy is also linked to severe male-factor infertility. We aimed to assess the number of aneuploid embryos and the number of cycles with transferable embryos in ADPKD patients after combined-PGT. The combined-PGT protocol, involving PGT-M by PCR and PGT-A by next-generation sequencing, was performed in single trophectoderm biopsies from 289 embryos in 83 PGT cycles. Transferable embryos were obtained in 69.9% of cycles. The number of aneuploid embryos and cycles with transferable embryos did not differ when the male or female had the ADPKD mutation. However, a significantly higher proportion of aneuploid embryos was found in the advanced maternal age (AMA) group, but not in the male factor (MF) group, when compared to non-AMA and non-MF groups, respectively. Additionally, no significant differences in the percentage of cycles with transferable embryos were found in any of the groups. Our results indicate that AMA couples among ADPKD patients have an increased risk of aneuploid embryos, but ADPKD-linked male infertility does not promote an increased aneuploidy rate.
机译:常染色体显性遗传性多囊肾病(ADPKD)是最常见的遗传性肾病,具有遗传和临床异质性。 ADPKD也可表现为肾外,在某些情况下精囊肿与男性不育有关。与ADPKD相关的男性不育症以及女性年龄已被提议作为可能影响单基因疾病(PGT-M)植入前基因检测(PGT)临床结果的因素。用于非整倍性评估的大型PGT(PGT-A)研究将胚胎非整倍性与女性年龄增加联系起来。其他研究表明,胚胎非整倍性也与严重的男性因素不育有关。我们的目的是评估联合PGT后ADPKD患者的非整倍体胚胎数和可转移胚胎的周期数。在83个PGT周期中,对来自289个胚胎的单个滋养层活检进行了组合式PGT方案,该方案涉及通过PCR进行的PGT-M和通过下一代测序进行的PGT-A。在69.9%的周期中获得了可移植的胚胎。当雄性或雌性具有ADPKD突变时,非整倍体胚胎的数量和具有可移植胚胎的周期没有差异。但是,与非AMA和非MF组相比,在高龄产妇(AMA)组中发现非整倍体胚胎的比例要高得多,而在男性因子(MF)组中则没有。此外,在任何一组中,均未发现具有可移植胚的周期百分比显着差异。我们的结果表明,ADPKD患者中的AMA夫妇发生非整倍体胚胎的风险增加,但与ADPKD相关的男性不育症并未促进非整倍体率的增加。

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