囊胚非整倍体率在生育人群和不孕人群之间是否存在差异?
Are blastocyst aneuploidy rates different between fertile and infertile populations?
机构信息
Department of Reproductive Endocrinology and Infertility, Stanford University, Stanford, CA, USA.
Department of Genome Sciences, University of Washington, Seattle, WA, USA.
出版信息
J Assist Reprod Genet. 2018 Mar;35(3):403-408. doi: 10.1007/s10815-017-1060-x. Epub 2017 Oct 23.
PURPOSE
This study aimed to determine if patients with infertility or recurrent pregnancy loss have higher rates of embryo aneuploidy than fertile controls.
METHODS
This was a retrospective review of all pre-implantation genetic screening (PGS) cases processed by a single reference lab prior to March 2014 after a blastocyst biopsy. Cases were excluded if no indication for PGS was designated or patients were translocation carriers. The fertile control group consisted of patients undergoing IVF with PGS for sex selection only. The comparison cohorts included those with recurrent pregnancy loss, male factor infertility, unexplained infertility, prior failed IVF, or previous aneuploid conceptions. A quasi-binomial regression model was used to assess the relationship between the dependent variable, aneuploidy rate and the independent variables, maternal age and reason for PGS. A quasi-Poisson regression model was used to evaluate the relationship between similar independent variables and the number of blastocyst biopsies per case.
RESULTS
The initial study population consisted of 3378 IVF-PGS cycles and 18,387 analyzed trophectoderm samples. Controlling for maternal age, we observed an increased rate of aneuploidy among patients with recurrent pregnancy loss (OR 1.330, p < 0.001), prior aneuploid pregnancy (OR 1.439, p < 0.001), or previous failed IVF cycles (OR 1.356, p = 0.0012) compared to fertile controls. Patients with unexplained and male factor infertility did not have a significantly different aneuploidy rate than controls (p > 0.05). The increase in aneuploidy in patients with RPL and prior IVF failure was driven by both an increase in meiotic (OR 1.488 and 1.508, p < 0.05) and mitotic errors (1.269 and 1.393, p < 0.05) relative to fertile controls, while patients with prior aneuploid pregnancies had only an increased risk of meiotic error aneuploidies (OR 1.650, p < 0.05).
CONCLUSIONS
Patients with recurrent pregnancy loss, previous IVF failures, and prior aneuploid pregnancies have a significantly higher, age-independent, aneuploidy rate compared to patients without infertility.
目的
本研究旨在确定不孕或复发性妊娠丢失患者的胚胎非整倍体率是否高于正常生育对照者。
方法
这是对 2014 年 3 月前在单个参考实验室进行的所有胚胎植入前遗传学筛查(PGS)病例的回顾性研究,这些病例均来自囊胚活检。如果未指定 PGS 的指征或患者为易位携带者,则排除该病例。正常生育对照组为仅因性别选择而进行 PGS 的 IVF 患者。比较组包括复发性妊娠丢失、男性因素不孕、不明原因不孕、先前 IVF 失败或先前存在非整倍体概念的患者。使用拟二项式回归模型评估因变量(非整倍体率)与自变量(母体年龄和 PGS 原因)之间的关系。使用拟泊松回归模型评估类似自变量与每个病例的囊胚活检数量之间的关系。
结果
初始研究人群包括 3378 个 IVF-PGS 周期和 18387 个分析的滋养外胚层样本。控制母体年龄后,我们观察到复发性妊娠丢失(OR 1.330,p<0.001)、先前非整倍体妊娠(OR 1.439,p<0.001)或先前 IVF 失败周期(OR 1.356,p=0.0012)的患者胚胎非整倍体率升高,与正常生育对照者相比。不明原因不孕和男性因素不孕患者的非整倍体率与对照组无显著差异(p>0.05)。RPL 和先前 IVF 失败患者的非整倍体增加是由减数分裂(OR 1.488 和 1.508,p<0.05)和有丝分裂错误(1.269 和 1.393,p<0.05)共同导致的,而先前存在非整倍体妊娠的患者仅存在减数分裂错误非整倍体的风险增加(OR 1.650,p<0.05)。
结论
与无不孕的患者相比,复发性妊娠丢失、先前 IVF 失败和先前非整倍体妊娠的患者具有显著更高、与年龄无关的非整倍体率。
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