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蜕膜细胞产生一种具有假定子宫内调节作用的肝素结合催乳素家族细胞因子。

Decidual cells produce a heparin-binding prolactin family cytokine with putative intrauterine regulatory actions.

作者信息

Alam S M Khorshed, Konno Toshihiro, Sahgal Namita, Lu Lu, Soares Michael J

机构信息

Institute of Maternal-Fetal Biology, Department of Pathology, University of Kansas Medical Center, Kansas City, Kansas 66160, USA.

出版信息

J Biol Chem. 2008 Jul 4;283(27):18957-68. doi: 10.1074/jbc.M801826200. Epub 2008 May 8.

Abstract

Pregnancy in mice and rats is associated with the production of a large family of hormones/cytokines related to prolactin (PRL). The hormones/cytokines are hypothesized to coordinate maternal and fetal adaptations to pregnancy. In this study, PRL-like protein-J (PLP-J, also known as PRL family 3, subfamily c, member 1 (Prl3c1)) is shown to be a product of the uterine decidua and a regulator of postimplantation intrauterine events. PLP-J-specific antibodies and a series of recombinant PLP-J proteins were generated and used to investigate PLP-J expression and as ligands for investigating biological targets. Decidual PLP-J migrates as a 29-kDa protein and localizes to a band of decidual cells surrounding the trophoblast cell layer on gestation day 8.5. PLP-J ligands specifically bound in situ to the surrounding uterine stromal cells and vasculature within the decidua of gestation day 8.5 implantation sites. We then investigated the in vitro actions of PLP-J on uterine stromal cells and endothelial cells. PLP-J specifically interacted with both cell populations. PLP-J promoted uterine stromal cell proliferation and inhibited endothelial cell proliferation. We determined that PLP-J does not interact with PRL receptors. Instead, PLP-J interacts with heparin-containing molecules, including syndecan-1, which is expressed in gestation day 8.5 pregnant uteri, as well as in uterine stromal cells and endothelial cells. The restricted expression of PLP-J and its specific interactions with uterine stromal cells and endothelial cells suggests that it acts locally and regulates decidual cell development and the endometrial vasculature.

摘要

小鼠和大鼠的妊娠与一大类与催乳素(PRL)相关的激素/细胞因子的产生有关。据推测,这些激素/细胞因子可协调母体和胎儿对妊娠的适应性变化。在本研究中,催乳素样蛋白-J(PLP-J,也称为催乳素家族3,c亚家族,成员1(Prl3c1))被证明是子宫蜕膜的产物,也是植入后子宫内事件的调节因子。我们制备了PLP-J特异性抗体和一系列重组PLP-J蛋白,用于研究PLP-J的表达,并作为研究生物靶点的配体。蜕膜中的PLP-J以29 kDa蛋白的形式迁移,并在妊娠第8.5天时定位于滋养层细胞层周围的蜕膜细胞带。PLP-J配体在妊娠第8.5天植入部位的蜕膜内与周围的子宫基质细胞和脉管系统发生特异性原位结合。然后,我们研究了PLP-J对子宫基质细胞和内皮细胞的体外作用。PLP-J与这两种细胞群体都有特异性相互作用。PLP-J促进子宫基质细胞增殖,抑制内皮细胞增殖。我们确定PLP-J不与催乳素受体相互作用。相反,PLP-J与含肝素的分子相互作用,包括在妊娠第8.5天的妊娠子宫以及子宫基质细胞和内皮细胞中表达的syndecan-1。PLP-J的限制性表达及其与子宫基质细胞和内皮细胞的特异性相互作用表明,它在局部发挥作用,调节蜕膜细胞发育和子宫内膜脉管系统。

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