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人类子宫内膜细胞外囊泡可促进人类滋养层模型着床:双向母胎通讯的理解。

Human Endometrial Extracellular Vesicles Functionally Prepare Human Trophectoderm Model for Implantation: Understanding Bidirectional Maternal-Embryo Communication.

机构信息

Endometrial Remodelling Laboratory, Centre for Reproductive Health, Hudson Institute of Medical Research, Clayton, VIC, 3800, Australia.

Department of Molecular and Translational Science, Monash University, Clayton, VIC, 3800, Australia.

出版信息

Proteomics. 2019 Dec;19(23):e1800423. doi: 10.1002/pmic.201800423. Epub 2019 Oct 30.

Abstract

Embryo implantation into maternal endometrium is critical for initiation and establishment of pregnancy, requiring developmental synchrony between endometrium and blastocyst. However, factors regulating human endometrial-embryo cross talk and facilitate implantation remain largely unknown. Extracellular vesicles (EVs) are emerging as important mediators of this process. Here, a trophectoderm spheroid-based in vitro model mimicking the pre-implantation human embryo is used to recapitulate important functional aspects of blastocyst implantation. Functionally, human endometrial EVs, derived from hormonally treated cells synchronous with implantation, are readily internalized by trophectoderm cells, regulating adhesive and invasive capacity of human trophectoderm spheroids. To gain molecular insights into mechanisms underpinning endometrial EV-mediated enhancement of implantation, quantitative proteomics reveal critical alterations in trophectoderm cellular adhesion networks (cell adhesion molecule binding, cell-cell adhesion mediator activity, and cell adherens junctions) and metabolic and gene expression networks, and the soluble secretome from human trophectodermal spheroids. Importantly, transfer of endometrial EV cargo proteins to trophectoderm to mediate changes in trophectoderm function is demonstrated. This is highlighted by correlation among endometrial EVs, the trophectodermal proteome following EV uptake, and EV-mediated trophectodermal cellular proteome, important for implantation. This work provides an understanding into molecular mechanisms of endometrial EV-mediated regulation of human trophectoderm functions-fundamental in understanding human endometrium-embryo signaling during implantation.

摘要

胚胎植入母体子宫内膜对于妊娠的启动和建立至关重要,这需要子宫内膜和囊胚之间的发育同步。然而,调节人类子宫内膜-胚胎相互作用并促进着床的因素在很大程度上仍不清楚。细胞外囊泡 (EVs) 正成为这一过程的重要介质。在这里,使用滋养外胚层球体为基础的体外模型模拟人类着床前胚胎,以重现囊胚着床的重要功能方面。从与着床同步的激素处理细胞中衍生的功能性人类子宫内膜 EV 可被滋养外胚层细胞轻易内化,调节人类滋养外胚层球体的黏附和侵袭能力。为了深入了解子宫内膜 EV 介导的着床增强的机制,定量蛋白质组学揭示了滋养外胚层细胞黏附网络(细胞黏附分子结合、细胞-细胞黏附介质活性和细胞黏着连接)以及代谢和基因表达网络的关键改变,以及来自人类滋养外胚层球体的可溶性分泌组。重要的是,证明了子宫内膜 EV 货物蛋白转移到滋养外胚层以介导滋养外胚层功能的变化。这一点通过子宫内膜 EVs、EV 摄取后滋养外胚层的蛋白质组以及 EV 介导的滋养外胚层细胞蛋白质组之间的相关性得到强调,这对于着床至关重要。这项工作深入了解了子宫内膜 EV 介导的人类滋养外胚层功能调节的分子机制,这对于理解着床过程中人类子宫内膜-胚胎信号转导至关重要。

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