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Size dependent biodistribution and toxicokinetics of iron oxide magnetic nanoparticles in mice

机译:大小依赖biodistribution和毒性动力学氧化铁磁性纳米粒子的老鼠

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In spite of the immense benefits from iron oxide magnetic nanoparticles (IOMNs), there is scanty information regarding their metabolic activities and toxicity in vivo. In this study, we investigated the size dependent in vivo biodistribution, toxicokinetics, and toxicity and gene expression changes of various sizes of carboxyl coated IOMNs (diameters of 10, 20, 30, and 40 nm). Our findings demonstrated that the various sizes of IOMNs accumulated primarily in the liver and spleen on the first day post-injection. Interestingly, size dependent biodistribution and transport were observed: the smallest IOMNs (10 nm) showed the highest uptake by the liver, whereas the largest IOMNs (40 nm) showed the highest uptake by the spleen. Moreover, the IOMNs with the smallest size (10 nm) were cleared faster from the liver and kidneys, but more readily entered the brain and the uterus. IOMNs with the largest size (40 nm) accumulated more readily but were easily eliminated in the spleen. However, the level of iron in the heart decreased in all IOMN exposed groups. In addition, blood biochemistry, hematological analyses and histological examination demonstrated that there was no apparent acute toxicity caused by IOMNs in mice. However, smaller IOMNs (10 nm and 20 nm) more effectively changed the expression level of sensitive genes related to oxidant stress, iron transport, metabolic process, apoptosis, and others.
机译:尽管从氧化铁的巨大好处磁性纳米颗粒(IOMNs),有稀疏的有关他们的代谢活动的信息并在体内的毒性。调查规模相关的体内biodistribution、毒性动力学和毒性不同大小的基因表达变化羧基涂布IOMNs(直径为10年,20年,30,40海里)。不同大小的积累主要在IOMNs肝脏和脾脏的第一天post-injection。biodistribution和运输观察:最小IOMNs (10 nm)显示最高的吸收由肝脏,而最大IOMNs(40海里)显示最高的脾吸收。此外,IOMNs最小的大小(10海里)清除了从肝脏和更快肾脏,但更容易进入大脑子宫。积累更容易,但很容易消除在脾。在所有IOMN暴露铁在下降组。血液分析和组织学检查表明没有在老鼠身上明显IOMNs引起的急性毒性。然而,小IOMNs(10和20 nm)有效的表达水平发生了变化敏感的基因与氧化剂应激有关,铁运输、代谢过程、细胞凋亡和别人。

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