Rosario Gracy X, Konno Toshihiro, Soares Michael J
Institute of Maternal-Fetal Biology, Department of Pathology and Laboratory Medicine, University of Kansas Medical Center, Kansas City, KS 66160, USA.
Dev Biol. 2008 Feb 15;314(2):362-75. doi: 10.1016/j.ydbio.2007.12.007. Epub 2007 Dec 15.
Oxygen is a critical regulator of placentation. Early placental development occurs in a predominantly low oxygen environment and is, at least partially, under the control of hypoxia signaling pathways. In the present study, in vivo hypobaric hypoxia was used as an experimental tool to delineate hypoxia-sensitive events during placentation. Pregnant rats were exposed to the equivalent of 11% oxygen between days 6.5 and 13.5 of gestation. Pair-fed pregnant animals exposed to ambient conditions were included as a control group. Uterine mesometrial blood vessels in the hypoxia-exposed animals were greatly expanded and some contained large cuboidal cells that were positive for cytokeratin and other markers characteristic of invasive trophoblast cells. Unlike later in gestation, the route of trophoblast cell invasion in the hypoxia-exposed animals was restricted to endovascular, with no interstitial invasion observed. Hypoxia-activated endovascular trophoblast invasion required exposure to hypoxia from gestation day 8.5 to day 9.5. Activation of the invasive trophoblast lineage was also associated with an enlargement of the junctional zone of the chorioallantoic placenta, a source of invasive trophoblast cell progenitors. In summary, maternal hypoxia during early stages of placentation activates the invasive endovascular trophoblast cell lineage and promotes uterine vascular remodeling.
氧气是胎盘形成的关键调节因子。早期胎盘发育主要发生在低氧环境中,并且至少部分受缺氧信号通路的控制。在本研究中,使用体内低压缺氧作为实验工具来描绘胎盘形成过程中对缺氧敏感的事件。在妊娠第6.5天至13.5天期间,将怀孕大鼠暴露于相当于11%氧气的环境中。将暴露于环境条件下的配对喂养怀孕动物作为对照组。暴露于缺氧环境的动物子宫系膜血管大幅扩张,一些血管中含有大的立方形细胞,这些细胞细胞角蛋白呈阳性,且具有侵袭性滋养层细胞的其他特征性标志物。与妊娠后期不同,暴露于缺氧环境的动物中滋养层细胞的侵袭途径仅限于血管内,未观察到间质侵袭。缺氧激活的血管内滋养层侵袭需要从妊娠第8.5天至第9.5天暴露于缺氧环境。侵袭性滋养层谱系的激活还与绒毛尿囊胎盘连接区的扩大有关,连接区是侵袭性滋养层细胞祖细胞的来源。总之,胎盘形成早期的母体缺氧激活了侵袭性血管内滋养层细胞谱系并促进子宫血管重塑。