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The Role of Megalin in the Transport of Gentamicin Across BeWo Cells an In Vitro Model of the Human Placenta

机译:巨蛋白在庆大霉素跨BeWo细胞运输中的作用BeWo细胞是人胎盘的体外模型

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摘要

Aminoglycosides (AG) are known to readily cross the placenta, although the mechanisms responsible for placental transport have not been characterized. Megalin is expressed in human placenta, and it is reasonable to speculate, given its role in renal AG uptake, that it is similarly involved in placental transport. However, the role of megalin in placental AG uptake has not been established. An in vitro model to study megalin-mediated placental transport has also not been previously described. The objectives of this study, therefore, were to evaluate the human choriocarcinoma (BeWo) cell line as a model to study megalin-mediated placental transport and to assess the uptake kinetics of gentamicin, an AG antibiotic, using this in vitro model. BeWo cells were grown on Transwell® plates, and megalin expression and functional activity were assessed. Uptake of 3H-gentamicin was also evaluated in the presence and absence of megalin inhibitors. Expression of megalin protein and mRNA in BeWo cells were confirmed via immunoblot and qPCR analysis. Uptake of fluorescein isothiocyanate (FITC)-labeled bovine serum albumin (BSA) (a megalin substrate) was time-, concentration-, and temperature-dependent consistent with a transporter-mediated process. FITC-BSA uptake was also significantly reduced in the presence of unlabeled gentamicin (a megalin substrate) and sodium maleate (to induce megalin shedding) suggesting that megalin is functionally active in BeWo cells. Gentamicin uptake exhibited time and temperature dependence, saturability and Michaelis-Menten kinetics, all of which suggest a transporter-mediated process. Gentamicin uptake was also significantly reduced in the presence of the megalin inhibitors RAP and EDTA suggesting that megalin is likely involved in gentamicin uptake.
机译:氨基糖苷类(AG)易于穿过胎盘,尽管尚未阐明负责胎盘运输的机制。巨蛋白在人胎盘中表达,鉴于其在肾脏AG摄取中的作用,可以合理地推测它与胎盘运输有关。但是,尚未确定巨蛋白在胎盘AG摄取中的作用。以前也没有描述研究巨蛋白介导的胎盘运输的体外模型。因此,本研究的目的是评估人绒癌组织(BeWo)细胞系,以研究巨蛋白介导的胎盘运输,并使用该体外模型评估庆大霉素(一种AG抗生素)的吸收动力学。 BeWo细胞在Transwell®平板上生长,并评估megalin的表达和功能活性。在存在和不存在巨蛋白抑制剂的情况下,还评估了 3 H-庆大霉素的摄取。通过免疫印迹和qPCR分析证实了巨噬蛋白在BeWo细胞中的表达。荧光素异硫氰酸酯(FITC)标记的牛血清白蛋白(BSA)(megalin底物)的摄取是时间,浓度和温度依赖性的,与转运蛋白介导的过程一致。在未标记的庆大霉素(巨蛋白底物)和马来酸钠(诱导巨蛋白脱落)的存在下,FITC-BSA的摄取也显着降低,表明巨蛋白在BeWo细胞中具有功能活性。庆大霉素的吸收表现出时间和温度依赖性,饱和度和Michaelis-Menten动力学,所有这些都表明转运蛋白介导的过程。在存在巨蛋白抑制剂RAP和EDTA的情况下,庆大霉素的摄取也显着降低,这表明巨蛋白可能与庆大霉素的摄取有关。

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