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A Synthetic Thiourea-Based Tripodal Receptor that Impairs the Function of Human First Trimester Cytotrophoblast Cells

机译:合成的硫脲基三脚架受体损害人的头三个月滋养层细胞的功能

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摘要

A synthetic tripodal-based thiourea receptor (PNTTU) was used to explore the receptor/ligand binding affinity using CTB cells. The human extravillous CTB cells (Sw.71) used in this study were derived from first trimester chorionic villus tissue. The cell proliferation, migration and angiogenic factors were evaluated in PNTTU-treated CTB cells. The PNTTU inhibited the CTBs proliferation and migration. The soluble fms-like tyrosine kinase-1 (sFlt-1) secretion was increased while vascular endothelial growth factor (VEGF) was decreased in the culture media of CTB cells treated with ≥1 nM PNTTU. The angiotensin II receptor type 2 (AT2) expression was significantly upregulated in ≥1 nM PNTTU-treated CTB cells in compared to basal; however, the angiotensin II receptor, type 1 (AT1) and vascular endothelial growth factor receptor 1 (VEGFR-1) expression was downregulated. The anti-proliferative and anti-angiogenic effect of this compound on CTB cells are similar to the effect of CTSs. The receptor/ligand affinity of PNTTU on CTBs provides us the clue to design a potent inhibitor to prevent the CTS-induced impairment of CTB cells.
机译:基于合成的三脚架的硫脲受体(PNTTU)用于探索使用CTB细胞的受体/配体结合亲和力。本研究中使用的人类绒毛外CTB细胞(Sw.71)来源于早孕绒毛膜绒毛组织。在PNTTU处理的CTB细胞中评估了细胞增殖,迁移和血管生成因子。 PNTTU抑制CTBs增殖和迁移。在≥1 nM PNTTU处理的CTB细胞培养基中,可溶性fms样酪氨酸激酶1(sFlt-1)分泌增加,而血管内皮生长因子(VEGF)减少。与基础相比,≥1nM PNTTU处理的CTB细胞中2型血管紧张素II受体(AT2)的表达显着上调;但是,血管紧张素II受体1型(AT1)和血管内皮生长因子受体1(VEGFR-1)的表达下调。该化合物对CTB细胞的抗增殖和抗血管生成作用与CTS相似。 PNTTU对CTB的受体/配体亲和力为我们提供了设计有效抑制剂以防止CTS诱导的CTB细胞损伤的线索。

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