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Targeted theranostic photoactivation on atherosclerosis

Authors
Song, Joon WooAhn, Jae WonLee, Min WooKim, Hyun JungKang, Dong OhKim, Ryeong HyunKang, Un GyoKim, Yeon HoonHan, JeongmooPark, Ye HeeNam, Hyeong SooYoo, HongkiPark, KyeongsoonKim, Jin Won
Issue Date
24-10월-2021
Publisher
BMC
Keywords
Atherosclerosis; Autophagy; Efferocytosis; Foam cells; Macrophage targetable phototheranostic agent; Photodynamic therapy
Citation
JOURNAL OF NANOBIOTECHNOLOGY, v.19, no.1
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF NANOBIOTECHNOLOGY
Volume
19
Number
1
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/136014
DOI
10.1186/s12951-021-01084-z
ISSN
1477-3155
Abstract
Background: Photoactivation targeting macrophages has emerged as a therapeutic strategy for atherosclerosis, but limited targetable ability of photosensitizers to the lesions hinders its applications. Moreover, the molecular mechanistic insight to its phototherapeutic effects on atheroma is still lacking. Herein, we developed a macrophage targetable near-infrared fluorescence (NIRF) emitting phototheranostic agent by conjugating dextran sulfate (DS) to chlorin e6 (Ce6) and estimated its phototherapeutic feasibility in murine atheroma. Also, the phototherapeutic mechanisms of DS-Ce6 on atherosclerosis were investigated. Results: The phototheranostic agent DS-Ce6 efficiently internalized into the activated macrophages and foam cells via scavenger receptor-A (SR-A) mediated endocytosis. Customized serial optical imaging-guided photoactivation of DS-Ce6 by light illumination reduced both atheroma burden and inflammation in murine models. Immuno-fluorescence and -histochemical analyses revealed that the photoactivation of DS-Ce6 produced a prominent increase in macrophage-associated apoptotic bodies 1 week after laser irradiation and induced autophagy with Mer tyrosine-protein kinase expression as early as day 1, indicative of an enhanced efferocytosis in atheroma. Conclusion: Imaging-guided DS-Ce6 photoactivation was able to in vivo detect inflammatory activity in atheroma as well as to simultaneously reduce both plaque burden and inflammation by harmonic contribution of apoptosis, autophagy, and lesional efferocytosis. These results suggest that macrophage targetable phototheranostic nanoagents will be a promising theranostic strategy for high-risk atheroma.
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