In Vivo Neuroimaging of Exosomes Using Gold Nanoparticles

微泡 内吞循环 体内 外体 体内分布 神经影像学 鼻腔给药 药物输送 临床前影像学 细胞生物学 神经科学 化学 药理学 内吞作用 医学 生物 小RNA 生物化学 受体 基因 生物技术 有机化学
作者
Oshra Betzer,Nisim Perets,Ariel Angel,Menachem Motiei,Tamar Sadan,Gal Yadid,Daniel Offen,Rachela Popovtzer
出处
期刊:ACS Nano [American Chemical Society]
卷期号:11 (11): 10883-10893 被引量:381
标识
DOI:10.1021/acsnano.7b04495
摘要

Exosomes are emerging as effective therapeutic tools for various pathologies. These extracellular vesicles can bypass biological barriers, including the blood-brain barrier, and can serve as powerful drug and gene therapy transporters. However, the progress of therapy development is impeded by several challenges, including insufficient data on exosome trafficking and biodistribution and the difficulty to image deep brain structures in vivo. Herein, we established a method for noninvasive in vivo neuroimaging and tracking of exosomes, based on glucose-coated gold nanoparticle (GNP) labeling and computed tomography imaging. Labeling of exosomes with the GNPs was achieved directly, as opposed to the typical and less efficient indirect labeling mode through parent cells. On the mechanistic level, we found that the glucose-coated GNPs were uptaken into MSC-derived exosomes via an active, energy-dependent mechanism that is mediated by the glucose transporter GLUT-1 and involves endocytic proteins. Next, we determined optimal parameters of size and administration route; we demonstrated that 5 nm GNPs enabled improved exosome labeling and that intranasal, compared to intravenous, administration led to superior brain accumulation and thus enhanced in vivo neuroimaging. Furthermore, using a mouse model of focal brain ischemia, we noninvasively tracked intranasally administered GNP-labeled exosomes, which showed increased accumulation at the lesion site over 24 h, as compared to nonspecific migration and clearance from control brains over the same period. Thus, this exosome labeling technique can serve as a powerful diagnostic tool for various brain disorders and could potentially enhance exosome-based treatments for neuronal recovery.
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