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首页> 外文期刊>Archives of Toxicology >Long-term exposure of immortalized keratinocytes to arsenic induces EMT, impairs differentiation in organotypic skin models and mimics aspects of human skin derangements
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Long-term exposure of immortalized keratinocytes to arsenic induces EMT, impairs differentiation in organotypic skin models and mimics aspects of human skin derangements

机译:长期暴露于永生的角质形成细胞到砷诱导EMT,损害有机型皮肤模型中的分化和人类皮肤紊乱的模拟方面

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摘要

Arsenic is one of the most important human carcinogens and environmental pollutants. However, the evaluation of the underlying carcinogenic mechanisms is challenging due to the lack of suitable in vivo and in vitro models, as distinct interspecies differences in arsenic metabolism exist. Thus, it is of high interest to develop new experimental models of arsenic-induced skin tumorigenesis in humans. Consequently, aim of this study was to establish an advanced 3D model for the investigation of arsenic-induced skin derangements, namely skin equivalents, built from immortalized human keratinocytes (NHEK/SVTERT3-5). In contrast to spontaneously immortalized HACAT cells, NHEK/SVTERT3-5 cells more closely resembled the differentiation pattern of primary keratinocytes. With regard to arsenic, our results showed that while our new cell model was widely unaffected by short-time treatment (72 h) with low, non-toxic doses of ATO (0.05-0.25 mu M), chronic exposure (6 months) resulted in distinct changes of several cell characteristics. Thus, we observed an increase in the G2 fraction of the cell cycle accompanied by increased nucleus size and uneven tubulin distribution. Moreover, cells showed strong signs of de-differentiation and upregulation of several epithelial-to-mesenchymal transition markers. In line with these effects, chronic contact to arsenic resulted in impaired skin-forming capacities as well as localization of ki67-positive (proliferating) cells at the upper layers of the epidermis; a condition termed Bowen's disease. Finally, chronically arsenic-exposed cells were characterized by an increased tumorigenicity in SCID mice. Taken together, our study presents a new model system for the investigation of mechanisms underlying the tumor-promoting effects of chronic arsenic exposure.
机译:砷是最重要的人类致癌物质之一和环境污染物之一。然而,由于体内和体外模型缺乏适合缺乏适合的缺乏砷代谢存在,对潜在的致癌机制的评估是挑战性的。因此,在人类中开发砷诱导的皮肤肿瘤瘤的新实验模型具有很高的兴趣。因此,本研究的目的是为砷诱导的皮肤紊乱进行调查,建立一种先进的3D模型,即由永生的人角蛋白细胞(NHEK / SVTERT3-5)构建的皮肤等同物。与自发的永生化的HaCAT细胞相反,NHEK / SVTERT3-5细胞更接近初级角质形成细胞的分化模式。关于砷,我们的研究结果表明,虽然我们的新细胞模型广泛不受短时间治疗(72小时)的影响(72小时),但无毒剂量的ato(0.05-0.25 mu m),慢性暴露(6个月)导致在不同细胞特征的不同变化中。因此,我们观察到细胞周期的G2分数的增加伴随着增加的核尺寸和不均匀的小管蛋白分布。此外,细胞显示出强烈的去分化迹象和几种上皮 - 间充质过渡标记的上调。符合这些效果,对砷的慢性接触导致皮肤形成容量受损,以及在表皮的上层处的Ki67阳性(增殖)细胞的定位;鲍文疾病的病情。最后,慢性砷暴露的细胞的特征在于SCID小鼠中的致瘤性增加。我们的研究占据了一项新的模型系统,用于调查慢性砷暴露肿瘤促进作用的机制。

著录项

  • 来源
    《Archives of Toxicology》 |2018年第1期|共14页
  • 作者单位

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Christian Doppler Lab Biotechnol Skin;

    Med Univ Vienna Inst Canc Res Dept Med 1 Borschkegasse 8a A-1090 Vienna Austria;

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Christian Doppler Lab Biotechnol Skin;

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Christian Doppler Lab Biotechnol Skin;

    Med Univ Vienna Inst Canc Res Dept Med 1 Borschkegasse 8a A-1090 Vienna Austria;

    Med Univ Vienna Inst Canc Res Dept Med 1 Borschkegasse 8a A-1090 Vienna Austria;

    Med Univ Vienna Inst Canc Res Dept Med 1 Borschkegasse 8a A-1090 Vienna Austria;

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Muthgasse 18 Haus B A-1190 Vienna;

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Muthgasse 18 Haus B A-1190 Vienna;

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Christian Doppler Lab Biotechnol Skin;

    Med Univ Vienna Dept Dermatol Vienna Austria;

    Med Univ Vienna Dept Dermatol Vienna Austria;

    Med Univ Vienna Inst Canc Res Dept Med 1 Borschkegasse 8a A-1090 Vienna Austria;

    BOKU Univ Nat Resources &

    Life Sci Vienna Dept Biotechnol Christian Doppler Lab Biotechnol Skin;

    Med Univ Vienna Inst Canc Res Dept Med 1 Borschkegasse 8a A-1090 Vienna Austria;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 毒物学(毒理学);
  • 关键词

    Organotypic culture; Skin equivalents; Arsenic; Immortalized keratinocytes; EMT;

    机译:有机型文化;皮肤等同物;砷;永生的角质形成细胞;EMT;

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