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对人类胚胎进行多次玻璃化-复温及活检操作:儿童的临床结局及新生儿随访

Multiple vitrification-warming and biopsy procedures on human embryos: clinical outcome and neonatal follow-up of children.

作者信息

De Vos Anick, Van Landuyt Lisbet, De Rycke Martine, Verdyck Pieter, Verheyen Greta, Buysse Andrea, Belva Florence, Keymolen Kathelijn, Tournaye Herman, Verpoest Willem

机构信息

Centre for Reproductive Medicine, Universitair Ziekenhuis Brussel, Brussels 1090, Belgium.

Centre for Medical Genetics, Universitair Ziekenhuis Brussel, Brussels 1090, Belgium.

出版信息

Hum Reprod. 2020 Nov 1;35(11):2488-2496. doi: 10.1093/humrep/deaa236.

Abstract

STUDY QUESTION

Does double vitrification and warming of human blastocysts having undergone biopsy once or twice have an impact on the clinical outcome?

SUMMARY ANSWER

The clinical pregnancy rate obtained with double vitrification single biopsy blastocysts was comparable to that obtained with single vitrification single biopsy blastocysts in our center in the same time period (46%; 2016-2018), whereas that obtained with double-vitrified double-biopsied blastocysts seemed lower and will need further study.

WHAT IS KNOWN ALREADY

Genetic testing on cryopreserved unbiopsied embryos involves two cryopreservation procedures. Retesting of failed/inconclusive-diagnosed blastocysts inevitably involves a second round of biopsy and a second round of vitrification as well. To what extent this practice impacts on the developmental potential of blastocysts has been studied to a limited extent so far and holds controversy. Additionally, the obstetrical/perinatal outcome after the transfer of double-vitrified/single or double-biopsied blastocysts is poorly documented.

STUDY DESIGN, SIZE, DURATION: This retrospective observational study included 97 cycles of trophectoderm biopsy and preimplantation genetic testing (PGT) on vitrified-warmed embryos followed by a second round of vitrification between March 2015 and December 2019.

PARTICIPANTS/MATERIALS, SETTING, METHODS: In 36 warming cycles, no biopsy was performed on the embryos before the first vitrification (single biopsy group). In 61 warming cycles, the embryos had been biopsied on Day 3 (n = 4) or on Day 5/6 (n = 57) before the first vitrification (double biopsy group). A second biopsy was mostly indicated in cycles of failed or inconclusive diagnosis at the first biopsy. Two cycles involved a more specific mutation test for X-linked diseases on male embryos and one cycle involved testing for a second monogenic indication supplementary to a previously tested reciprocal translocation. Post-warming suitability for biopsy, availability of genetically transferable embryos and clinical outcome of subsequent frozen-thawed embryo transfer (FET) cycles were reported. Neonatal follow-up of the children was included.

MAIN RESULTS AND THE ROLE OF CHANCE

In total, 91 cleavage-stage embryos and 154 blastocysts were warmed, of which 34 (37.4%) and 126 (81.8%), respectively, were of sufficient quality to undergo trophectoderm biopsy and were subsequently vitrified for a second time. Out of these, 92 underwent biopsy for the first time (single biopsy), whereas 68 underwent a second biopsy (double biopsy). After diagnosis, 77 blastocysts (48.1%) were revealed to be genetically transferable (44 in the single biopsy group and 33 in the double biopsy group). In 46 warming cycles, 51 blastocysts were warmed and 49 survived this second warming procedure (96.0%). Subsequently, there were 45 FET cycles resulting in 27 biochemical pregnancies and 18 clinical pregnancies with fetal heartbeat (40.0% per FET cycle: 44.0% in the single biopsy group and 35.0% in the double biopsy group, P = 0.54). Thirteen singletons were born (eight in the single biopsy group and five in the double biopsy group), while three pregnancies were ongoing. A total of 26 embryos (13 in each group) remain vitrified and have the potential to increase the final clinical pregnancy rate. The neonatal follow-up of the children born so far is reassuring.

LIMITATIONS, REASONS FOR CAUTION: This is a small retrospective cohort, thus, the implantation potential of double vitrification double biopsy blastocysts, as compared to double vitrification single biopsy blastocysts and standard PGT (single vitrification, single biopsy), certainly needs further investigation. Although one could speculate on birthweight being affected by the number of biopsies performed, the numbers in this study are too small to compare birthweight standard deviation scores in singletons born after single or double biopsy.

WIDER IMPLICATIONS OF THE FINDINGS

PGT on vitrified-warmed embryos, including a second vitrification-warming step, results in healthy live birth deliveries, for both single- and double-biopsied embryos. The neonatal follow-up of the 13 children born so far did not indicate any adverse effect. The present study is important in order to provide proper counseling to couples on their chance of a live birth per initial warming cycle planned and concerning the safety issue of rebiopsy and double vitrification.

STUDY FUNDING/COMPETING INTEREST(S): None.

TRIAL REGISTRATION NUMBER

N/A.

摘要

研究问题

对已进行过一次或两次活检的人类囊胚进行双重玻璃化冷冻及解冻,是否会对临床结局产生影响?

总结答案

在我们中心,同一时期双重玻璃化冷冻单次活检囊胚的临床妊娠率与单次玻璃化冷冻单次活检囊胚的临床妊娠率相当(46%;2016 - 2018年),而双重玻璃化冷冻两次活检囊胚的临床妊娠率似乎较低,仍需进一步研究。

已知信息

对冷冻保存的未活检胚胎进行基因检测涉及两次冷冻保存程序。对诊断失败/不确定的囊胚进行重新检测不可避免地也涉及第二轮活检和第二轮玻璃化冷冻。到目前为止,这种做法对囊胚发育潜能的影响在一定程度上已有研究,但仍存在争议。此外,双重玻璃化冷冻/单次或两次活检囊胚移植后的产科/围产期结局记录较少。

研究设计、规模、持续时间:这项回顾性观察研究纳入了2015年3月至2019年12月期间97个对玻璃化冷冻解冻胚胎进行滋养外胚层活检和植入前基因检测(PGT)并随后进行第二轮玻璃化冷冻的周期。

参与者/材料、设置、方法:在36个解冻周期中,第一次玻璃化冷冻前未对胚胎进行活检(单次活检组)。在61个解冻周期中,胚胎在第一次玻璃化冷冻前的第3天(n = 4)或第5/6天(n = 57)已进行过活检(两次活检组)。第二次活检主要用于第一次活检诊断失败或不确定的周期。两个周期涉及对男性胚胎进行更特异的X连锁疾病突变检测,一个周期涉及针对先前检测的相互易位补充进行的第二个单基因指征检测。报告了解冻后活检的适宜性、可用于基因检测的胚胎情况以及随后冻融胚胎移植(FET)周期的临床结局。纳入了对所生孩子的新生儿随访。

主要结果及机遇的作用

总共91个卵裂期胚胎和154个囊胚被解冻,其中分别有34个(37.4%)和126个(81.8%)质量足够进行滋养外胚层活检,随后进行了第二次玻璃化冷冻。其中,92个首次进行活检(单次活检),而68个进行了第二次活检(两次活检)。诊断后,77个囊胚(48.1%)被发现可用于基因检测(单次活检组44个,两次活检组33个)。在46个解冻周期中,51个囊胚被解冻,49个在第二次解冻过程中存活(96.0%)。随后,有45个FET周期,导致27例生化妊娠和18例有胎心的临床妊娠(每个FET周期40.0%:单次活检组44.0%,两次活检组35.0%,P = 0.54)。13例单胎出生(单次活检组8例,两次活检组5例),3例妊娠仍在继续。共有26个胚胎(每组13个)仍处于玻璃化冷冻状态,有可能提高最终临床妊娠率。到目前为止对所生孩子的新生儿随访情况令人安心。

局限性、谨慎原因:这是一个小的回顾性队列研究,因此,与双重玻璃化冷冻单次活检囊胚和标准PGT(单次玻璃化冷冻、单次活检)相比,双重玻璃化冷冻两次活检囊胚的着床潜能肯定需要进一步研究。虽然有人推测出生体重可能受活检次数影响,但本研究中的样本量太小,无法比较单次或两次活检后出生的单胎的出生体重标准差评分。

研究结果的更广泛影响

对玻璃化冷冻解冻胚胎进行PGT,包括第二步玻璃化冷冻解冻步骤,对于单次和两次活检的胚胎均能实现健康活产。到目前为止对13例出生儿童的新生儿随访未显示任何不良影响。本研究对于为夫妇提供关于每个计划的初始解冻周期活产几率以及再次活检和双重玻璃化冷冻安全性问题的适当咨询很重要。

研究资金/利益冲突:无。

试验注册号

无。

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