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Transcriptome Analysis Reveals New Insights into the Modulation of Endometrial Stromal Cell Receptive Phenotype by Embryo-Derived Signals Interleukin-1 and Human Chorionic Gonadotropin: Possible Involvement in Early Embryo Implantation

机译:转录组分析揭示了由胚胎衍生信号白介素-1和人类绒毛膜促性腺激素调节子宫内膜基质细胞受体表型的新见解:可能参与早期胚胎植入

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摘要

The presence of the conceptus in uterine cavity necessitates an elaborate network of interactions between the implanting embryo and a receptive endometrial tissue. We believe that embryo-derived signals play an important role in the remodeling and the extension of endometrial receptivity period. Our previous studies provided original evidence that human Chorionic Gonadotropin (hCG) modulates and potentiates endometrial epithelial as well as stromal cell responsiveness to interleukin 1 (IL1), one of the earliest embryonic signals, which may represent a novel pathway by which the embryo favors its own implantation and growth within the maternal endometrial host. The present study was designed to gain a broader understanding of hCG impact on the modulation of endometrial cell receptivity, and in particular, cell responsiveness to IL1 and the acquisition of growth-promoting phenotype capable of receiving, sustaining, and promoting early and crucial steps of embryonic development. Our results showed significant changes in the expression of genes involved in cell proliferation, immune modulation, tissue remodeling, apoptotic and angiogenic processes. This points to a relevant impact of these embryonic signals on the receptivity of the maternal endometrium, its adaptation to the implanting embryo and the creation of an environment that is favorable for the implantation and the growth of this latter within a new and likely hostile host tissue. Interestingly our data further identified a complex interaction between IL1 and hCG, which, despite a synergistic action on several significant endometrial target genes, may encompass a tight control of endogenous IL1 and extends to other IL1 family members.
机译:子宫腔中概念的存在需要植入胚胎和子宫内膜组织之间相互作用的精细网络。我们认为,胚胎来源的信号在子宫内膜接受期的重塑和延长中起着重要作用。我们以前的研究提供了原始证据,表明人类绒毛膜促性腺激素(hCG)调节并增强了子宫内膜上皮以及基质细胞对白细胞介素1(IL1)的响应,白细胞介素1(IL1)是最早的胚胎信号之一,可能代表了一种新的途径,胚胎可以通过这种途径来促进其自身在子宫内膜宿主体内的植入和生长。本研究旨在更广泛地了解hCG对子宫内膜细胞接受性的调节的影响,尤其是细胞对IL1的响应性以及能够接受,维持和促进肝癌早期和关键步骤的生长促进表型的获得。胚胎发育。我们的结果表明,涉及细胞增殖,免疫调节,组织重塑,凋亡和血管生成过程的基因表达发生了显着变化。这表明这些胚胎信号对母体子宫内膜的接受能力,其对植入胚胎的适应以及创造有利于后者在新的且可能是敌对的宿主组织中的植入和生长的环境的相关影响。 。有趣的是,我们的数据进一步确定了IL1和hCG之间的复杂相互作用,尽管对几个重要的子宫内膜靶基因有协同作用,但它可能包含对内源性IL1的严格控制并扩展到其他IL1家族成员。

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