Insights into embryo-endometrium immune interactions.

IF 2.5 2区 医学 Q2 DEVELOPMENTAL BIOLOGY
Rosanna Ramhorst, Lourdes Materazzi, Ana Schafir, Lara Castagnola, Laura Fernández, Elizabeth Soczewski, Esteban Grasso, Gustavo Martinez, Diego Gnocchi, Antonio Cattaneo, Lautaro Tessari, Marcela Irigoyen, Claudia Perez Leirós, Soledad Gori
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Abstract

Embryo implantation requires a tight immune homeostatic control that activates regulatory circuits. One interlocutor is the embryo, which produces soluble ligands and expresses receptors for different autocrine and paracrine factors. The other interlocutor is the receptive endometrium, which produces mediators to regulate proliferation, differentiation, adhesion and invasiveness of the embryo, among other processes. Here, we are going to discuss experimental evidence regarding human embryo-endometrial dialogue and give a new insight of the relevance of the immune cells to coordinate embryo implantation. In this sense, decidualization of endometrial stromal cells is a multistep process that gives rise to mature decidual cells and senescent decidual cells. The first subpopulation secretes pro-implantation factors and begins migration by encapsulating the embryo. In turn, the second does not complete differentiation but rather suffers a process of premature senescence that is characterized by the production of pro-inflammatory factors (SASP, senescence-associated secretory phenotype), which contribute to embryo implantation. However, alterations in these processes or in their regulation through microRNAs lead to the perpetuation of an inflammatory response and alterations in endometrial receptivity. Considering that decidual cells acquire the ability to differentially respond to embryo quality, here we also explored how the soluble factors produced by embryos (classified according to their quality) impact on the inflammatory response and shape dendritic and other immune cell recruitment during the peri implantation period. To address these aspects, we present experimental evidence that links endoplasmic reticulum stress, senescence and inflammation and we discuss whether embryos reprogram the immune response.

洞察胚胎-子宫内膜免疫相互作用。
胚胎植入需要严密的免疫稳态控制,激活调节回路。一个对话者是胚胎,它产生可溶性配体并表达不同自分泌和旁分泌因子的受体。另一个对话者是受体子宫内膜,它产生调节胚胎增殖、分化、粘附和侵袭等过程的介质。在此,我们将讨论有关人类胚胎-子宫内膜对话的实验证据,并对免疫细胞协调胚胎着床的相关性给出新的见解。从这个意义上说,子宫内膜间质细胞的脱体细胞化是一个多步骤的过程,产生成熟的蜕细胞和衰老的蜕细胞。第一个亚群分泌促着床因子,并通过包裹胚胎开始迁移。反过来,第二个细胞不能完成分化,而是经历了一个以促炎因子(SASP,衰老相关分泌表型)的产生为特征的过早衰老过程,这有助于胚胎着床。然而,这些过程的改变或其通过microrna调控的改变会导致炎症反应的持续和子宫内膜容受性的改变。考虑到蜕细胞获得对胚胎质量的差异反应能力,本研究还探讨了胚胎产生的可溶性因子(根据其质量分类)如何影响着床期的炎症反应和形状树突状和其他免疫细胞募集。为了解决这些问题,我们提出了内质网应激、衰老和炎症之间联系的实验证据,并讨论了胚胎是否对免疫反应进行了重编程。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Placenta
Placenta 医学-发育生物学
CiteScore
6.30
自引率
10.50%
发文量
391
审稿时长
78 days
期刊介绍: Placenta publishes high-quality original articles and invited topical reviews on all aspects of human and animal placentation, and the interactions between the mother, the placenta and fetal development. Topics covered include evolution, development, genetics and epigenetics, stem cells, metabolism, transport, immunology, pathology, pharmacology, cell and molecular biology, and developmental programming. The Editors welcome studies on implantation and the endometrium, comparative placentation, the uterine and umbilical circulations, the relationship between fetal and placental development, clinical aspects of altered placental development or function, the placental membranes, the influence of paternal factors on placental development or function, and the assessment of biomarkers of placental disorders.
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