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稳定的形态动力学进展是活产的独立预测指标:整倍体胚胎的描述性参考。

Steady morphokinetic progression is an independent predictor of live birth: a descriptive reference for euploid embryos.

作者信息

Bayram Aşina, Elkhatib Ibrahim, Kalafat Erkan, Abdala Andrea, Ferracuti Virginia, Melado Laura, Lawrenz Barbara, Fatemi Human, Nogueira Daniela

机构信息

IVF Department, ART Fertility Clinics, Abu Dhabi, UAE.

Department of Reproductive Medicine, UZ Ghent, Ghent, Belgium.

出版信息

Hum Reprod Open. 2024 Oct 10;2024(4):hoae059. doi: 10.1093/hropen/hoae059. eCollection 2024.

Abstract

STUDY QUESTION

Can modelling the longitudinal morphokinetic pattern of euploid embryos during time-lapse monitoring (TLM) be helpful for selecting embryos with the highest live birth potential?

SUMMARY ANSWER

Longitudinal reference ranges of morphokinetic development of euploid embryos have been identified, and embryos with steadier progression during TLM are associated with higher chances of live birth.

WHAT IS KNOWN ALREADY

TLM imaging is increasingly adopted by fertility clinics as an attempt to improve the ability of selecting embryos with the highest potential for implantation. Many markers of embryonic morphokinetics have been incorporated into decision algorithms for embryo (de)selection. However, longitudinal changes during this temporal process, and the impact of such changes on embryonic competence remain unknown. Aiming to model the reference ranges of morphokinetic development of euploid embryos and using it as a single longitudinal trajectory might provide an additive value to the blastocyst morphological grade in identifying highly competent embryos.

STUDY DESIGN SIZE DURATION

This observational, retrospective cohort study was performed in a single IVF clinic between October 2017 and June 2021 and included only autologous single euploid frozen embryo transfers (seFET).

PARTICIPANTS/MATERIALS SETTING METHODS: Reference ranges were developed from [hours post-insemination (hpi)] of the standard morphokinetic parameters of euploid embryos assessed as tPB2, tPNa, tPNf, t2-t9, tSC, tM, tSB, and tB. Variance in morphokinetic patterns was measured and reported as morphokinetic variance score (MVS). Nuclear errors (micronucleation, binucleation, and multinucleation) were annotated when present in at least one blastomere at the two- or four-cell stages. The blastocyst grade of expansion, trophectoderm (TE), and inner cell mass (ICM) were assessed immediately before biopsy using Gardner's criteria. Pre-implantation genetic diagnosis for aneuploidy (PGT-A) was performed by next-generation sequencing. All euploid embryos were singly transferred in a frozen transferred cycle and outcomes were assessed as live birth, pregnancy loss, or not pregnant. Association of MVS with live birth was investigated with regression analyses.

MAIN RESULTS AND THE ROLE OF CHANCE

TLM data from 340 seFET blastocysts were included in the study, of which 189 (55.6%) resulted in a live birth. The median time for euploid embryos to reach blastulation was 109.9 hpi (95% CI: 98.8-121.0 hpi). The MVS was calculated from the variance in time taken for the embryo to reach all morphokinetic points and reflects the total morphokinetic variability it exhibits during its development. Embryos with more erratic kinetics, i.e. higher morphokinetic variance, had higher rates of pregnancy loss ( = 0.004) and no pregnancy ( < 0.001) compared to embryos with steadier morphokinetic patterns. In the multivariable analysis adjusting for ICM, TE grade, presence of nuclear errors, and time of blastulation, MVS was independently associated with live birth (odds ratio [OR]: 0.62, 95% CI: 0.46-0.84,  = 0.002) along with ICM quality. Live birth rate of embryos with the same ICM grading but different morphokinetic variance patterns differed significantly. Live birth rates of embryos exhibiting low MVS with ICM grades A, B, and C were 85%, 76%, and 67%, respectively. However, ICM grades A, B, and C embryos with high MVS had live birth rates of 65%, 48%, and 21% ( < 0.001). The addition of the MVS to embryo morphology score (ICM and TE grading) significantly improved the model's AUC value (0.67 vs 0.62,  = 0.015) and this finding persisted through repeat cross-validation (0.64 ± 0.08 vs 0.60 ± 0.07,  < 0.001).

LIMITATIONS REASONS FOR CAUTION

The exclusion of IVF cases limits, for now, the utility of the model to only ICSI-derived embryos. The utility of these reference ranges and the association of MVS with various clinical outcomes should be further investigated.

WIDER IMPLICATIONS OF THE FINDINGS

We have developed reference ranges for morphokinetic development of euploid embryos and a marker for measuring total morphokinetic variability exhibited by developed blastocysts. Longitudinal assessment of embryonic morphokinetics rather than static time points may provide more insight about which embryos have higher live birth potential. The developed reference ranges and MVS show an association with live birth that is independent of known morphological factors and could emerge as a valuable tool in prioritizing embryos for transfer.

STUDY FUNDING/COMPETING INTERESTS: This study received no external funding. The authors declare no conflicting interests.

TRIAL REGISTRATION NUMBER

N/A.

摘要

研究问题

在延时监测(TLM)过程中对整倍体胚胎的纵向形态动力学模式进行建模,是否有助于选择具有最高活产潜能的胚胎?

总结答案

已确定整倍体胚胎形态动力学发育的纵向参考范围,并且在TLM期间进展更稳定的胚胎活产几率更高。

已知信息

生育诊所越来越多地采用TLM成像,试图提高选择具有最高着床潜能胚胎的能力。许多胚胎形态动力学标记已被纳入胚胎(去)选择的决策算法中。然而,在此时间过程中的纵向变化以及这些变化对胚胎能力的影响仍然未知。旨在对整倍体胚胎形态动力学发育的参考范围进行建模,并将其用作单一纵向轨迹,可能会在识别高能力胚胎方面为囊胚形态学等级提供附加价值。

研究设计、规模、持续时间:这项观察性、回顾性队列研究于2017年10月至2021年6月在一家单一的体外受精诊所进行,仅纳入自体单整倍体冷冻胚胎移植(seFET)。

参与者/材料、设置、方法:参考范围是根据作为tPB2、tPNa、tPNf、t2 - t9、tSC、tM、tSB和tB评估的整倍体胚胎标准形态动力学参数的[授精后小时数(hpi)]制定的。测量形态动力学模式的方差并报告为形态动力学方差评分(MVS)。当在二细胞或四细胞阶段至少一个卵裂球中出现时,对核错误(微核化、双核化和多核化)进行注释。在活检前立即使用加德纳标准评估囊胚的扩张等级、滋养外胚层(TE)和内细胞团(ICM)。通过下一代测序进行非整倍体植入前基因诊断(PGT - A)。所有整倍体胚胎在冷冻移植周期中单独移植,结局评估为活产、妊娠丢失或未妊娠。通过回归分析研究MVS与活产的关联。

主要结果及机遇的作用

340个seFET囊胚的TLM数据被纳入研究,其中189个(55.6%)活产。整倍体胚胎达到囊胚形成的中位时间为109.9 hpi(95% CI:98.8 - 121.0 hpi)。MVS是根据胚胎到达所有形态动力学点所需时间的方差计算得出的,反映了其在发育过程中表现出的总形态动力学变异性。与形态动力学模式更稳定的胚胎相比,动力学更不稳定(即形态动力学方差更高)的胚胎妊娠丢失率更高(P = 0.004)且未妊娠率更高(P < 0.001)。在多变量分析中,调整ICM、TE等级、核错误的存在以及囊胚形成时间后,MVS与活产独立相关(优势比[OR]:0.62,95% CI:0.46 - 0.84,P = 0.002),同时与ICM质量相关。具有相同ICM分级但不同形态动力学方差模式的胚胎活产率差异显著。ICM分级为A、B和C且MVS低的胚胎活产率分别为85%、76%和67%。然而,ICM分级为A、B和C且MVS高的胚胎活产率分别为65%、48%和21%(P < 0.001)。将MVS添加到胚胎形态学评分(ICM和TE分级)中显著提高了模型的AUC值(0.67对0.62,P = 0.015),并且这一发现通过重复交叉验证得以持续(0.64 ± 0.08对0.60 ± 0.07,P < 0.001)。

局限性、谨慎原因:目前,排除体外受精病例限制了该模型仅对卵胞浆内单精子注射(ICSI)衍生胚胎的效用。这些参考范围的效用以及MVS与各种临床结局的关联应进一步研究。

研究结果的更广泛影响

我们已经为整倍体胚胎的形态动力学发育制定了参考范围,并开发了一种用于测量发育囊胚表现出的总形态动力学变异性的标记。对胚胎形态动力学进行纵向评估而非静态时间点评估,可能会提供更多关于哪些胚胎具有更高活产潜能的见解。所开发的参考范围和MVS显示出与活产的关联,且独立于已知的形态学因素,可能会成为在优先选择移植胚胎方面的一个有价值工具。

研究资金/利益冲突:本研究未获得外部资金。作者声明无利益冲突。

试验注册号

无。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/95c9/11540439/dd2960b482ed/hoae059f1.jpg

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