人类囊胚中的细胞质串:关于其作用的假设及其对胚胎选择的影响。

IF 6 1区 医学 Q1 OBSTETRICS & GYNECOLOGY
Anabella Marconetto, Federica Innocenti, Gaia Saturno, Marilena Taggi, Viviana Chiappetta, Samuele Trio, Felicia De Falco, Laura Albricci, Giovanni Coticchio, Aisling Ahlström, Giulia Fiorentino, Roberta Maggiulli, Alberto Vaiarelli, Maurizio Zuccotti, Laura Rienzi, Danilo Cimadomo
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引用次数: 0

摘要

研究问题:细胞质串(Cyt-S)的存在及其数量和动态对人类囊胚植入前的发育有何影响?Cyt-S 在人类胚胎中很常见,与囊胚发育速度更快、体积更大和形态质量更好有关:Cyt-S是连接内细胞团和滋养层细胞(TE)的动态细胞突起,可在囊胚扩张过程中观察到。据估计,它们在人类胚胎中的发生率在 44% 到 93% 之间。有关它们的临床意义和在发育中的作用的数据还很缺乏、有限或存在争议:研究设计、规模、持续时间:2013 年 5 月至 2014 年 11 月期间在一家试管婴儿中心进行的回顾性研究,涉及 124 个植入前非整倍体基因检测周期,在延时培养箱中对≥1 个囊胚进行了活检和玻璃化处理(N = 370 个胚胎评估)。这些周期共进行了 87 次玻璃化加热单倍囊胚移植:ICSI、连续囊胚培养(第 5-7 天)、第 3 天未钻透明带的完全膨大囊胚 TE 活检、qPCR 评估均匀全染色体非整倍体和玻璃化。只进行了玻璃化温育的单胚胎移植。囊胚形态质量根据加德纳标准进行定义。基于人工智能的软件 CHLOE™ (Fairtility) 自动将从开始囊胚形成(tSB)到活检(t-活检,即囊胚完全膨大)的时间记录为授精后小时数(hpi)、胚胎面积(包括透明带,单位 µm2)和自发性囊胚塌陷。一位资深胚胎学家手动标注 Cyt-S 的存在、数量、时间和类型(细胞间粗连接和/或线状)。通过回归分析确认了所有重要关联。还检测了所有夫妇、周期和胚胎的主要特征与 Cyt-S 存在、数量和动态的关联性:约 94.3% 的患者(N = 117/124)有≥1 个胚胎带有 Cyt-S。在总共 370 个囊胚中,有 55 个在囊胚形成和完全扩展之间退化(N = 55/370,14.9%)。≥1个Cyt-S的胚胎退化率为10.8%(N = 33/304),明显低于无Cyt-S的胚胎(33.3%,N = 22/66,P 局限性,需谨慎的原因:Cyt-S的存在和动态是通过每15分钟记录一次的视频帧在七个焦点平面上手动评估的。纳入的患者多为高龄产妇。只能报告相关性,而不能报告因果关系。最后,需要更大的数据集来更好地评估 Cyt-S 与临床结果的关联:Cyt-S在人类囊胚扩张过程中很常见,这表明它们在这一过程中具有生理意义。它们的存在、数量和动态反映了胚胎的存活率和形态质量,但它们的作用仍然未知。鼓励未来的基础科学研究最终描述 Cyt-S 的分子性质和生物物理特性,人工智能工具应通过纳入 Cyt-S 评估来帮助这些研究:无。试验登记号:不适用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cytoplasmic strings in human blastocysts: hypotheses of their role and implications for embryo selection.

Study question: What are the implications of the presence cytoplasmic strings (Cyt-S) and their quantity and dynamics for the pre-implantation development of human blastocysts?

Summary answer: Cyt-S are common in human embryos and are associated with faster blastocyst development, larger expansion, and better morphological quality.

What is known already: Cyt-S are dynamic cellular projections connecting inner cell mass and trophectoderm (TE) cells, that can be observed during blastocyst expansion. Their prevalence in human embryos has been estimated to be between 44% and 93%. Data relevant to their clinical implications and role in development are lacking, limited, or controversial.

Study design, size, duration: Retrospective study conducted at a single IVF center between May 2013 and November 2014 and involving 124 pre-implantation genetic testing for aneuploidy cycles in a time-lapse incubator with ≥1 blastocyst biopsied and vitrified (N = 370 embryos assessed). These cycles resulted in 87 vitrified-warmed single-euploid blastocyst transfers.

Participants/materials, setting, methods: ICSI, continuous blastocyst culture (Days 5-7), TE biopsy of fully expanded blastocysts without Day 3 zona pellucida drilling, qPCR to assess uniform full-chromosome aneuploidies, and vitrification were all performed. Only vitrified-warmed euploid single-embryo-transfers were conducted. Blastocyst morphological quality was defined according to Gardner's criteria. The AI-based software CHLOE™ (Fairtility) automatically registered timings from time of starting blastulation (tSB) to biopsy (t-biopsy, i.e. blastocyst full-expansion) as hours-post-insemination (hpi), embryo area (including zona pellucida in µm2), and spontaneous blastocyst collapses. One senior embryologist manually annotated Cyt-S presence, quantity, timings, and type (thick cell-to-cell connections and/or threads). All significant associations were confirmed through regression analyses. All couples', cycles', and embryos' main features were also tested for associations with Cyt-S presence, quantity, and dynamics.

Main results and the role of chance: About 94.3% of the patients (N = 117/124) had ≥1 embryo with Cyt-S. Out of a total of 370 blastocysts, 55 degenerated between blastulation and full-expansion (N = 55/370, 14.9%). The degeneration rate among embryos with ≥1 Cyt-S was 10.8% (N = 33/304), significantly lower than that of embryos without Cyt-S (33.3%, N = 22/66, P < 0.01). Of the remaining 315 viable blastocysts analyzed, 86% (N = 271/315; P < 0.01) had ≥1 Cyt-S, on average 3.5 ± 2.1 per embryo ranging 1-13. The first Cyt-S per viable embryo appeared at 115.3 ± 12.5 hpi (85.7-157.7), corresponding to 10.5 ± 5.8 h (0.5-31) after tSB. Overall, we analyzed 937 Cyt-S showing a mean duration of 3.8 ± 2.7 h (0.3-20.9). Cyt-S were mostly threads (N = 508/937, 54.2%) or thick cell-to-cell connections becoming threads (N = 382/937, 40.8%) than thick bridges (N = 47/937, 5.0%). The presence and quantity of Cyt-S were significantly associated with developmentally faster (on average 6-12 h faster) and more expanded (on average 2700 µm2-larger blastocyst's area at t-biopsy) embryos. Also, the presence and duration of Cyt-S were associated with better morphology. Lastly, while euploidy rates were comparable between blastocysts with and without Cyt-S, all euploid blastocysts transferred from the latter group failed to implant (N = 10).

Limitations, reasons for caution: Cyt-S presence and dynamics were assessed manually on seven focal planes from video frames recorded every 15 min. The patients included were mostly of advanced maternal age. Only associations could be reported, but no causations/consequences. Lastly, larger datasets are required to better assess Cyt-S associations with clinical outcomes.

Wider implications of the findings: Cyt-S are common during human blastocyst expansion, suggesting their physiological implication in this process. Their presence, quantity and dynamics mirror embryo viability, and morphological quality, yet their role is still unknown. Future basic science studies are encouraged to finally describe Cyt-S molecular nature and biophysical properties, and Artificial Intelligence tools should aid these studies by incorporating Cyt-S assessment.

Study funding/competing interest(s): None.

Trial registration number: N/A.

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来源期刊
Human reproduction
Human reproduction 医学-妇产科学
CiteScore
10.90
自引率
6.60%
发文量
1369
审稿时长
1 months
期刊介绍: Human Reproduction features full-length, peer-reviewed papers reporting original research, concise clinical case reports, as well as opinions and debates on topical issues. Papers published cover the clinical science and medical aspects of reproductive physiology, pathology and endocrinology; including andrology, gonad function, gametogenesis, fertilization, embryo development, implantation, early pregnancy, genetics, genetic diagnosis, oncology, infectious disease, surgery, contraception, infertility treatment, psychology, ethics and social issues.
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