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Murine liver damage caused by exposure to nano-titanium dioxide

机译:暴露于纳米二氧化钛对小鼠肝脏的损害

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Due to its unique physiochemical properties, nano-titanium dioxide (nano-TiO2) is widely used in all aspects of people's daily lives, bringing it into increasing contact with humans. Thus, this material's security issues for humans have become a heavily researched subject. Nano-TiO2 can enter the body through the mouth, skin, respiratory tract or in other ways, after which it enters the blood circulation and is deposited in the liver, changing biochemical indicators and causing liver inflammation. Meanwhile, the light sensitivity of these nanoparticles allows them to become media-generating reactive oxygen species (ROS), causing an imbalance between oxidation and anti-oxidation that leads to oxidative stress and liver damage. Nano-TiO2 can be transported into cells via phagocytosis, where the nanoparticles bind to the mitochondrial membrane, resulting in the disintegration of the membrane and the electron transport chain within the mitochondria. Thus, more ROS are produced. Nano-TiO2 can also enter the nucleus, where it can directly embed into or indirectly affect DNA, thereby causing DNA breakage or affecting gene expression. These effects include increased mRNA and protein expression levels of inflammation-related factors and decreased mRNA and protein expression levels of I kappa B and IL-2, resulting in inflammation. Long-term inflammation of the liver causes HSC cell activation, and extracellular matrix (ECM) deposition is promoted by multiple signalling pathways, resulting in liver fibrosis. In this paper, the latest progress on murine liver injury induced by environmental TiO2 is systematically described. The toxicity of nano-TiO2 also depends on size, exposure time, surface properties, dosage, administration route, and its surface modification. Therefore, its toxic effects in humans should be studied in greater depth. This paper also provides useful reference information regarding the safe use of nano-TiO2 in the future.
机译:由于其独特的理化特性,纳米二氧化钛(nano-TiO2)被广泛用于人们日常生活的各个方面,从而使其与人类的接触日益增加。因此,这种材料对人类的安全性问题已成为研究的热点。纳米二氧化钛可以通过口腔,皮肤,呼吸道或其他方式进入人体,然后进入血液循环并沉积在肝脏中,从而改变生化指标并引起肝脏炎症。同时,这些纳米颗粒的光敏性使它们成为产生介质的活性氧(ROS),导致氧化和抗氧化之间的不平衡,从而导致氧化应激和肝损害。纳米二氧化钛可以通过吞噬作用转运到细胞中,在那里纳米颗粒与线粒体膜结合,导致膜和线粒体内的电子传输链解体。因此,产生了更多的ROS。纳米二氧化钛也可以进入细胞核,直接嵌入或间接影响DNA,从而导致DNA断裂或基因表达。这些影响包括炎症相关因子的mRNA和蛋白表达水平升高以及IκB和IL-2的mRNA和蛋白表达水平降低,从而导致炎症。肝脏的长期炎症导致HSC细胞活化,并且多种信号通路促进细胞外基质(ECM)沉积,从而导致肝纤维化。本文系统地描述了环境TiO2引起的鼠肝损伤的最新进展。纳米二氧化钛的毒性还取决于尺寸,暴露时间,表面性质,剂量,给药途径及其表面改性。因此,应更深入地研究其对人体的毒性作用。本文还提供了有关将来安全使用纳米TiO2的有用参考信息。

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