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A tetraethylene glycol coat gives gold nanoparticles long in vivo half-lives with minimal increase in size

机译:四甘醇涂层可为金纳米颗粒提供较长的体内半衰期且尺寸增加最小

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摘要

In this study, we describe the experiments determining whether coating gold nanoparticles with tetraethylene glycol (TEG) provides pharmacologically relevant advantages, such as increased serum half-life and resistance to protein adsorption. Monodisperse TEG-coated, NaBH4-reduced gold nanoparticles with a hydrodynamic size comparable to albumin were synthesized by reducing gold chloride with NaBH4 under alkaline conditions in the presence of TEG-SH. The particles were characterized by gel electrophoresis, column chromatography, and transmission electron microscopy. The nanoparticles were subsequently injected intravenously into mice, and their half-lives and final destinations were determined via photometric analysis, light microscopy (LM), and transmission electron microscopy. The TEG particles had a long half-life (~400 minutes) that was not influenced by splenectomy. After 500 minutes of injection, TEG particles were found in kidney proximal tubule cell vesicles and in spleen red and white pulp. The particles induced apoptosis in the spleen red pulp but not in white pulp or the kidney. Some of the TEG particles appeared to have undergone ligand exchange reactions that increased their charge. The TEG particles were shown to be resistant to nonspecific protein adsorption, as judged by gel electrophoresis and column chromatography. These results demonstrate that naturally monodisperse, small-sized gold nanoparticles coated with TEG have long in vivo plasma half-lives, are minimally toxic, and are resistant to protein adsorption. This suggests that a TEG coating should be considered as an alternative to a polyethylene glycol coating, which is polydisperse and of much larger size.
机译:在这项研究中,我们描述了确定用四甘醇(TEG)涂覆金纳米颗粒是否提供药理学相关优势(例如增加的血清半衰期和对蛋白质吸附的抵抗力)的实验。通过在碱性条件下在TEG-SH的存在下用NaBH4还原氯化金,合成了具有与白蛋白相当的流体力学尺寸的单分散TEG涂层,NaBH4还原的金纳米颗粒。通过凝胶电泳,柱色谱和透射电子显微镜对颗粒进行表征。随后将纳米颗粒静脉内注射到小鼠中,并通过光度分析,光学显微镜(LM)和透射电子显微镜确定其半衰期和最终终点。 TEG颗粒具有较长的半衰期(〜400分钟),不受脾切除术的影响。注射500分钟后,在肾近端小管细胞囊泡和脾脏的红色和白色浆液中发现了TEG颗粒。该颗粒诱导脾脏红髓中的细胞凋亡,但不引起白髓或肾脏中的细胞凋亡。一些TEG颗粒似乎发生了配体交换反应,从而增加了电荷。如通过凝胶电泳和柱色谱法所判断,TEG颗粒显示出对非特异性蛋白质吸附的抗性。这些结果表明,涂​​有TEG的天然单分散,小尺寸金纳米粒子具有较长的体内血浆半衰期,毒性极小,并且对蛋白质吸附具有抵抗力。这表明,应考虑将TEG涂层视为多分散且尺寸更大的聚乙二醇涂层的替代品。

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