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早期小鼠蜕膜中血管发育的影像学及其与白细胞和滋养层的关联。

Imaging of vascular development in early mouse decidua and its association with leukocytes and trophoblasts.

机构信息

Department of Biomedical and Molecular Sciences, Queen's University, Kingston, Ontario, Canada.

出版信息

Biol Reprod. 2012 Nov 29;87(5):125. doi: 10.1095/biolreprod.112.102830. Print 2012 Nov.

DOI:10.1095/biolreprod.112.102830
PMID:22954796
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3509781/
Abstract

In species with endometrial decidualization and hemochorial placentation (humans, mice, and others), leukocytes localize to early implant sites and contribute to decidual angiogenesis, spiral arterial remodeling, and trophoblast invasion. Relationships between leukocytes, trophoblasts, and the decidual vasculature are not fully defined. Early C57BL/6J implant sites were analyzed by flow cytometry to define leukocyte subsets and by whole-mount immunohistochemistry to visualize relationships between leukocytes, decidual vessels, and trophoblasts. Ptprc(+) (CD45(+)) cells increased in decidua between Gestational Day (GD) 5.5 and GD 9.5. Uterine natural killer (uNK) cells that showed dynamic expression of Cd (CD) 69, an activating receptor, and Klrg1 (KLRG1), an inhibitory receptor, localized mesometrially and were the dominant CD45(+) cells between GD 5.5 and GD 7.5. At GD 8.5, immature monocytes that occurred throughout decidua exceeded uNK cells numerically and many leukocytes acquired irregular shapes, and leukocyte-leukocyte conjugates became frequent. Vessels were morphologically heterogeneous and regionally unique. Migrating trophoblasts were first observed at GD 6.5 and, at GD 9.5, breached endothelium, entered vascular lumens, and appeared to occlude some vessels, as described for human spiral arteries. No leukocyte-trophoblast conjugates were detected. Whole-mount staining gave unparalleled decidual vascular detail and cell-specific positional information. Its application across murine models of pregnancy disturbances should significantly advance our understanding of the maternal-fetal interface.

摘要

在具有子宫内膜蜕膜化和血绒毛膜胎盘(人类、小鼠等)的物种中,白细胞定位于早期着床部位,并有助于蜕膜血管生成、螺旋动脉重塑和滋养层浸润。白细胞、滋养层和蜕膜血管之间的关系尚未完全确定。通过流式细胞术分析早期 C57BL/6J 着床部位,以定义白细胞亚群,并通过全组织免疫组织化学观察白细胞、蜕膜血管和滋养层之间的关系。Ptprc(+)(CD45(+))细胞在Gestational Day (GD) 5.5 和 GD 9.5 之间在蜕膜中增加。表现出激活受体 Cd(CD)69 和抑制受体 Klrg1(KLRG1)动态表达的子宫自然杀伤 (uNK) 细胞定位于系膜侧,并且是 GD 5.5 和 GD 7.5 之间的主要 CD45(+)细胞。在 GD 8.5,广泛存在于蜕膜中的未成熟单核细胞在数量上超过 uNK 细胞,许多白细胞获得不规则形状,白细胞-白细胞共轭变得频繁。血管形态多样且具有区域特异性。迁移的滋养层在 GD 6.5 首次被观察到,并且在 GD 9.5,穿透内皮细胞,进入血管腔,并似乎阻塞了一些血管,如人类螺旋动脉所述。未检测到白细胞-滋养层共轭物。全组织染色提供了无与伦比的蜕膜血管细节和细胞特异性位置信息。它在妊娠障碍的小鼠模型中的应用应该会显著提高我们对母体-胎儿界面的理解。

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