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Visualization of Macrophage Recruitment to Inflammation Lesions using Highly Sensitive and Stable Radionuclide-Embedded Gold Nanoparticles as a Nuclear Bio-Imaging Platform

Authors
Lee, Sang BongLee, Ho WonSingh, Thoudam DebrajLi, YinghuaKim, Sang KyoonCho, Sung JinLee, Sang-WooJeong, Shin YoungAhn, Byeong-CheolChoi, SangilLee, In-KyuLim, Dong-KwonLee, JaetaeJeon, Yong Hyun
Issue Date
2017
Publisher
IVYSPRING INT PUBL
Keywords
gold nanoparticles; nuclear bio-imaging platform; macrophage migration; acute inflammation
Citation
THERANOSTICS, v.7, no.4, pp.926 - 934
Indexed
SCIE
SCOPUS
Journal Title
THERANOSTICS
Volume
7
Number
4
Start Page
926
End Page
934
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/86428
DOI
10.7150/thno.17131
ISSN
1838-7640
Abstract
Reliable and sensitive imaging tools are required to track macrophage migration and provide a better understating of their biological roles in various diseases. Here, we demonstrate the possibility of radioactive iodide-embedded gold nanoparticles (RIe-AuNPs) as a cell tracker for nuclear medicine imaging. To demonstrate this utility, we monitored macrophage migration to carrageenan-induced sites of acute inflammation in living subjects and visualized the effects of anti-inflammatory agents on this process. Macrophage labeling with RIe-AuNPs did not alter their biological functions such as cell proliferation, phenotype marker expression, or phagocytic activity. In vivo imaging with positron-emission tomography revealed the migration of labeled macrophages to carrageenan-induced inflammation lesions 3 h after transfer, with highest recruitment at 6 h and a slight decline of radioactive signal at 24 h; these findings were highly consistent with the data of a bio-distribution study. Treatment with dexamethasone (an anti-inflammation drug) or GSK5182 (an ERR. inverse agonist) hindered macrophage recruitment to the inflamed sites. Our findings suggest that a cell tracking strategy utilizing RIe-AuNPs will likely be highly useful in research related to macrophage-related disease and cell-based therapies.
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