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Direct Effect of Chenodeoxycholic Acid on Differentiation of Mouse Embryonic Stem Cells Cultured under Feeder-Free Culture Conditions

机译:赤铁氧胆酸直接效应在无饲喂饲料培养条件下培养小鼠胚胎干细胞的分化

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Chenodeoxycholic acid (CDCA), a farnesoid X receptor (FXR) ligand, is a member of the nuclear receptor family and is probably involved in regulating the cellular activities of embryonic stem (ES) cells. Recently, although it was reported that the FXR ligand can mediate differentiation, apoptosis, and/or growth arrest in several cell types, it is still not well known how CDCA mediates effects in ES cells. Therefore, we investigated the direct effect of CDCA on mES cells. Feeder-free mES cells were treated in a dose-dependent manner with CDCA (50, 100, and 200 muM) for 72 h, and then a 100 muM CDCA treatment was performed for an additional 72 h. We analyzed the morphology, cell growth, cell characteristics, immunocytochemistry, and RT-PCR. In CDCA-treated cells, we observed the disappearance of pluripotent stem cell markers including alkaline phosphatase, Oct4, and Nanog and a time- and dose-dependent increase in expression of nestin, PAX6, and a-smooth muscle actin, but not a-fetoprotein. The 100 muM CDCA-treated cells in their second passage continued this differentiation pattern similar to those in the controls. In conclusion, these results suggest that CDCA can guide mES cells by an FXR-independent pathway to differentiate into ectoderm and/or mesoderm, but not endoderm.
机译:ChenodoOxycholic acid(CDCA),法德曲面X受体(FXR)配体,是核受体家族的成员,可能参与调节胚胎茎(ES)细胞的细胞活性。最近,虽然据报道,FXR配体可以在几种细胞类型中介导分化,细胞凋亡和/或生长停滞,但仍然没有公知的CDCA如何在ES细胞中介导影响。因此,我们研究了CDCA对MES细胞的直接影响。将饲养的MES细胞以剂量依赖性方式用CDCA(50,100和200毫米)处理72小时,然后进行100毫安CDCA处理另外72小时。我们分析了形态,细胞生长,细胞特征,免疫细胞化学和RT-PCR。在CDCA处理的细胞中,我们观察到包括碱性磷酸酶,OCT4和纳米的多能干细胞标记物的消失,以及巢蛋白,PAX6和嗜平肌肌动蛋白表达的时间和剂量依赖性增加,但不是 - 胎儿蛋白。其第二段中的100毫米CDCA处理细胞继续这种与对照中的分化模式类似。总之,这些结果表明CDCA可以通过FXR独立的途径引导MES细胞来分化成胚芽和/或中胚层,但不是内胚层。

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