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不孕诊断对胚胎-子宫内膜对话的影响。

The impact of infertility diagnosis on embryo-endometrial dialogue.

机构信息

Colorado Center for Reproductive MedicineLone Tree, Colorado, USA

University of KentCanterbury, UK.

出版信息

Reproduction. 2018 Jun;155(6):543-552. doi: 10.1530/REP-17-0566. Epub 2018 Apr 10.

DOI:10.1530/REP-17-0566
PMID:29636406
Abstract

Initial stages of implantation involve bi-directional molecular crosstalk between the blastocyst and endometrium. This study investigated an association between infertility etiologies, specifically advanced maternal age (AMA) and endometriosis, on the embryo-endometrial molecular dialogue prior to implantation. Co-culture experiments were performed with endometrial epithelial cells (EEC) and cryopreserved day 5 blastocysts ( = 41 ≥ Grade 3BB) donated from patients presenting with AMA or endometriosis, compared to fertile donor oocyte controls. Extracellular vesicles isolated from co-culture supernatant were analyzed for miRNA expression and revealed significant alterations correlating to AMA or endometriosis. Specifically, AMA resulted in 16 miRNAs with increased expression ( ≤ 0.05) and strong evidence for negative regulation toward 206 target genes. , a known activator of cell adhesion, displayed decreased expression ( ≤ 0.05), validating negative regulation by 4 of these increased miRNAs: miR-126; 150; 29a; 29b ( ≤ 0.05). In endometriosis patients, a total of 10 significantly altered miRNAs displayed increased expression compared to controls (miR-7b; 9; 24; 34b; 106a; 191; 200b; 200c; 342-3p; 484) ( ≤ 0.05), targeting 1014 strong evidence-based genes. Three target genes of miR-106a (, and ) were independently validated. Functional annotation analysis of miRNA-target genes revealed enriched pathways for both infertility etiologies, including disrupted cell cycle regulation and proliferation ( ≤ 0.05). These extracellular vesicle-bound secreted miRNAs are key transcriptional regulators in embryo-endometrial dialogue and may be prospective biomarkers of implantation success. One of the limitations of this study is that it was a stimulated, model and therefore may not accurately reflect the environment.

摘要

胚胎着床的初始阶段涉及胚泡和子宫内膜之间的双向分子串扰。本研究探讨了不孕病因,特别是高龄产妇(AMA)和子宫内膜异位症,对着床前胚胎-子宫内膜分子对话的影响。将来自 AMA 或子宫内膜异位症患者的冷冻第 5 天的囊胚(≥Grade 3BB)与来自生育力正常的供卵者的囊胚进行共培养实验,并与对照组进行比较。对共培养上清液中分离的细胞外囊泡进行 miRNA 表达分析,结果显示与 AMA 或子宫内膜异位症相关的表达谱发生显著改变。具体而言,与 AMA 相关的有 16 个 miRNA 表达上调(≤0.05),并且对 206 个靶基因有强烈的负调控证据。作为细胞黏附的已知激活剂,其表达下调(≤0.05),验证了这 4 个上调 miRNA 对其的负调控作用:miR-126;150;29a;29b(≤0.05)。在子宫内膜异位症患者中,与对照组相比,共有 10 个 miRNA 表达上调(miR-7b;9;24;34b;106a;191;200b;200c;342-3p;484)(≤0.05),靶向 1014 个具有强证据的基因。miR-106a 的 3 个靶基因(、和)也得到了独立验证。miRNA 靶基因的功能注释分析显示,两种不孕病因均存在丰富的通路,包括细胞周期调控和增殖失调(≤0.05)。这些细胞外囊泡结合分泌的 miRNA 是胚胎-子宫内膜对话中的关键转录调节剂,可能是植入成功的潜在生物标志物。本研究的局限性之一是这是一个体外刺激模型,因此可能无法准确反映体内环境。

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