首页> 外文期刊>The Journal of toxicological sciences >Acute hepatotoxicity of multimodal targeted imaging contrast agent NaLuF4:Gd,Yb,Er-PEG/PEI-FA in mice
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Acute hepatotoxicity of multimodal targeted imaging contrast agent NaLuF4:Gd,Yb,Er-PEG/PEI-FA in mice

机译:急性肝毒性的多峰靶向成像造影剂NALUF4:GD,YB,ER-PEG / PEI-FA在小鼠中

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In the past few decades, upconversion nanoparticles (abbreviated as UCNPs) have been more widely applied in the biomedical fields, such as in vitro and in vivo upconversion fluorescent bioimaging, photodynamic therapy, biological macromolecular detection, imaging mediated drug delivery and so on. But meanwhile, there is still not much research on the acute toxicity of upconversion nanoparticles in vivo, such as acute hepatotoxicity. In this work, we studied the in vivo biodistribution and acute hepatotoxicity of multimodal targeted contrast agent NaLuF4:Gd,Yb,Er-PEG/PEI-FA nanoprobe, which were synthesized by the solvothermal method and modified with Polyethylene glycol (PEG), Polyetherimide (PEI), folic acid (FA) on the surface. The acute hepatotoxicity in mice was systematically assessed after tail vein injection of different concentration of UCNPs. The results showed that NaLuF4:Gd,Yb,Er-PEG/PEI-FA nanoparticles with an average diameter of 44.5 +/- 10.4 nm, and three typical upconversion fluorescence emission bands at 520 nm, 540 nm and 660 nm under the excitation of 980 nm laser. In vivo distribution experiments results demonstrated that approximately 87% of UCNPs injected through the tail vein accumulate in the liver. In the acute hepatotoxicity test, the intravenously injection dose of UCNPs was 10, 40, 70 and 100 mg/kg, respectively. The body weight, blood routine, serum biochemistry, histomorphology and liver oxidative stress were detected and observed no significant acute hepatotoxicity damage under the injection dose of 100 mg/kg. In conclusion, NaLuF4:Gd,Yb,Er-PEG/PEI-FA nanoprobes are safe and reliable, and have potential applications in the field of tumor targeted multimodal imaging.
机译:在过去的几十年中,上转化纳米颗粒(缩写为UCNP)已经更广泛地应用于生物医学领域,例如体外和体内上变化荧光生物成像,光动力治疗,生物大分子检测,成像介导的药物递送等。但同时,仍然没有多大的研究体内上转化纳米颗粒的急性毒性,例如急性肝毒性。在这项工作中,我们研究了多峰靶向造影剂NALUF4:Gd,Yb,ER-PEG / PEI-FA纳米孔的体内生物分布和急性肝毒性,通过溶剂热法合成并用聚乙二醇(PEG),聚醚酰亚胺改性(PEI),表面上的叶酸(FA)。在尾静脉注射不同浓度的UCNP后系统评估小鼠中的急性肝毒性。结果表明,NALUF4:Gd,Yb,ER-PEG / PEI-FA纳米颗粒,平均直径为44.5 +/- 10.4nm,以及在激励下为520nm,540nm和660nm的三种典型上变化荧光发射带980 nm激光器。体内分布实验结果表明,大约87%的UCNP通过尾静脉注射在肝脏中。在急性肝毒性试验中,静脉内注射剂量分别为10,40,70和100mg / kg。检测体重,血液常规,血清生物化学,组织术和肝脏氧化应激,观察到在100mg / kg的注射剂量下没有显着的急性肝毒性损伤。总之,NALUF4:GD,YB,ER-PEG / PEI-FA纳米植物是安全可靠的,并且在肿瘤靶向多峰成像领域具有潜在的应用。

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