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Toxicity and genotoxicity of Nano-SiO 2 on human epithelial intestinal HT-29 cell line

机译:纳米SiO 2对人上皮肠道HT-29细胞系的毒性和遗传毒性

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Silica mesoporous nanoparticles have been recently selected for a wide range of applications from electronics to medicine due to their intrinsic properties. Among medical applications, drug delivery using SiO 2 nanoparticles by oral route is under study. Major benefits are expected including higher specificity and sensitivity together with side effect reduction. Since literature shows that very complex and unexpected interactions could occur between nanomaterials and biological systems, one critical issue is to control the nanoparticle cytotoxicity/genotoxicity for normal tissues and specially stomach and intestine when oral route is considered. The aim of the work is to study the cytotoxicity and genotoxicity of SiO 2 nanoparticles on HT29 human intestine cell line, using conventional and innovative methodologies, for measuring cell viability and proliferation, global metabolism, genotoxicity, and nanoparticles uptake. Core-dye doped SiO 2 nanoparticles of 25 and 100 nm were specifically synthesized to track nanoparticles incorporation by confocal and video microscopy. Besides conventional approaches (sulforhodamine B, flow cytometry, and γ-H2Ax foci), we have performed a real-time monitoring of cell proliferation using an impedance- based system which ensure no interference between measures and nanoparticles physicochemical characteristics. Overall, our results showed that SiO 2-25nm and SiO 2-100nm induced a rather limited cytotoxic and genotoxic effects on HT-29 cells after a 24 h exposure. However, regarding cell viability and genotoxicity, inverse dose-dependant relationships were observed for SiO 2-100nm nanoparticles. In conclusion, it seems that the higher the dose of SiO 2-100nm, the lower the cytotoxic/genotoxic effects, data that well illustrate the complexity in identifying and understanding the hazards of nanoparticles for human health.
机译:二氧化硅介孔纳米粒子由于其固有特性,最近已被选择用于从电子到医学的广泛应用。在医学应用中,正在研究通过SiO 2纳米颗粒通过口服途径进行药物递送。预期主要益处包括更高的特异性和敏感性以及副作用的减少。由于文献表明纳米材料与生物系统之间可能发生非常复杂且出乎意料的相互作用,因此一个关键问题是在考虑口服途径时,控制纳米颗粒对正常组织尤其是胃和肠的细胞毒性/遗传毒性。该工作的目的是使用常规和创新方法研究SiO 2纳米颗粒对HT29人肠细胞系的细胞毒性和遗传毒性,以测量细胞活力和增殖,整体代谢,遗传毒性和纳米颗粒摄取。通过共聚焦和视频显微镜,专门合成了25和100 nm的掺有芯染料的SiO 2纳米颗粒。除了常规方法(磺胺丁丹B,流式细胞仪和γ-H2Ax病灶)以外,我们还使用基于阻抗的系统对细胞增殖进行了实时监控,以确保测量值与纳米颗粒理化特性之间不会发生干扰。总体而言,我们的研究结果表明,暴露24 h后,SiO 2-25nm和SiO 2-100nm对HT-29细胞诱导了相当有限的细胞毒性和遗传毒性作用。然而,关于细胞活力和遗传毒性,对于SiO 2-100nm纳米粒子观察到剂量依赖性的反比关系。总之,似乎SiO 2-100nm的剂量越高,细胞毒性/遗传毒性作用越低,这些数据充分说明了识别和理解纳米颗粒对人体健康的危害的复杂性。

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