小鼠胎盘滋养细胞和巨噬细胞的特异性CSF-1结合与胎盘生长有关。

I Athanassakis-Vassiliadis, J Papamatheakis, S Vassiliadis
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引用次数: 16

摘要

先前的研究表明,集落刺激因子-1 (CSF-1)可以刺激胎源性贴壁、吞噬和非特异性酯酶阳性胎盘细胞群的体外增殖,这些细胞群对细胞角蛋白和Mac-1染色呈阳性。结合实验旨在测试这是否是该因子对这些细胞的直接影响。结合/洗脱和放射自显影实验表明,贴壁胎盘细胞特异性结合CSF-1。根据内皮标志物细胞角蛋白和波形蛋白的表达,从小鼠胎盘中分离出3个亚群:迷路源性滋养细胞(细胞角蛋白阳性,波形蛋白阴性)、海绵滋养细胞源性滋养细胞(细胞角蛋白阳性,波形蛋白阴性)和胎盘巨噬细胞(细胞角蛋白阴性,波形蛋白阳性)。3h -胸苷结合实验和结合实验表明,这些细胞同时响应并结合巨噬细胞特异性因子CSF-1。此外,结果表明,分离的滋养细胞生长速度低,对有丝分裂刺激非常敏感,而胎盘巨噬细胞单独生长速度高,因此对有丝分裂刺激不太敏感。这些发现支持在小鼠胎盘中存在一个重要的细胞因子调节网络,其中两个主要细胞群可能通过可溶性因子合作来刺激胎盘生长,从而促进胎儿发育。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Specific CSF-1 binding on murine placental trophoblasts and macrophages serves as a link to placental growth.

Previous studies have shown that the colony-stimulating factor-1 (CSF-1), stimulates the in vitro proliferation of a fetally-derived adherent, phagocytic and non-specific esterase positive placental cell population which stains positively for cytokeratin and Mac-1. Binding experiments were designed to test whether this is a direct effect of the factor on these cells. Binding/elution as well as autoradiography experiments, show that adherent placental cells specifically bind CSF-1. Based on the expression of the endothelial markers cytokeratin and vimentin three subpopulations of cells were isolated from the murine placenta: labyrinthine-derived trophoblasts (cytokeratin positive, vimentin negative), spongiotrophoblast-derived trophoblasts (cytokeratin positive, vimentin negative) and placental macrophages (cytokeratin negative, vimentin positive). 3H-Thymidine incorporation assays as well as binding experiments, showed that these cells simultaneously respond to and bind the macrophage-specific factor CSF-1. Furthermore, the results indicate that isolated trophoblasts have a low rate of growth and they are very sensitive to mitogenic stimulation, whereas placental macrophages alone have a high rate of growth and therefore are less sensitive to the mitogenic stimulus. These findings are in favour of the existence of an important cytokine regulatory network in the murine placenta, where two major cell populations may collaborate possibly via soluble factors to stimulate placental growth and thus fetal development.

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