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Determination of Heavy Metal Concentrations in Normal and Pathological Human Endometrial Biopsies and In Vitro Regulation of Gene Expression by Metals in the Ishikawa and Hec-1b Endometrial Cell Line

机译:正常和病理性人类子宫内膜活检中重金属含量的测定以及石川和Hec-1b子宫内膜细胞系中金属的基因表达的体外调控

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摘要

It is well known that several metals, such as lead, mercury, cadmium, and vanadium, can mimic the effects of estrogens (metallo-estrogens). Nevertheless, there are only a few studies that have assessed the effects of toxic metals on the female genital tract and, in particular, endometrial tissue. In this context, we measured the concentrations of several trace elements in human endometrial tissue samples from individuals with hyperplasia or adenocarcinoma and in normal tissues. Hyperplasic endometrial tissue has a 4-fold higher concentration of mercury than normal tissue. Mercury can affect both the AhR and ROS signaling pathways. Thus, we investigated the possible toxic effects of mercury by in vitro studies. We found that mercury increases oxidative stress (increased HO1 and NQO1 mRNA levels) and alters the cytoskeleton in the human endometrial Ishikawa cell line and to a lesser extent, in the “less-differentiated” human endometrial Hec-1b cells. The results might help to explain a potential link between this metal and the occurrence of endometrial hyperplasia.
机译:众所周知,几种金属,例如铅,汞,镉和钒,可以模仿雌激素(metallo-estrogens)的作用。然而,只有少数研究评估了有毒金属对女性生殖道尤其是子宫内膜组织的影响。在这种情况下,我们测量了患有增生或腺癌的人的子宫内膜组织样品以及正常组织中几种微量元素的浓度。增生性子宫内膜组织的汞浓度比正常组织高4倍。汞可以影响AhR和ROS信号通路。因此,我们通过体外研究调查了汞可能的毒性作用。我们发现汞增加了氧化应激(增加了HO1和NQO1 mRNA的水平)并改变了人类子宫内膜Ishikawa细胞系的细胞骨架,并在较小分化的人类子宫内膜Hec-1b细胞中改变了细胞骨架。结果可能有助于解释这种金属与子宫内膜增生发生之间的潜在联系。

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