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Cited 45 time in webofscience Cited 56 time in scopus
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Intracoronary dual-modal optical coherence tomography-near-infrared fluorescence structural-molecular imaging with a clinical dose of indocyanine green for the assessment of high-risk plaques and stent-associated inflammation in a beating coronary arteryopen access

Authors
Kim, SunwonLee, Min WooKim, Tae ShikSong, Joon WooNam, Hyeong SooCho, Han SaemJang, Sun-JooRyu, JiheunOh, Dong JooGweon, Dae-GabPark, Seong HwanPark, KyeongsoonOh, Wang-YuhlYoo, HongkiKim, Jin Won
Issue Date
1-Oct-2016
Publisher
OXFORD UNIV PRESS
Keywords
Atherosclerosis; Inflammation; Imaging; Plaque; Stents
Citation
EUROPEAN HEART JOURNAL, v.37, no.37, pp 2833 - 2844
Pages
12
Indexed
SCI
SCIE
SCOPUS
Journal Title
EUROPEAN HEART JOURNAL
Volume
37
Number
37
Start Page
2833
End Page
2844
URI
https://scholarworks.korea.ac.kr/kumedicine/handle/2020.sw.kumedicine/5988
DOI
10.1093/eurheartj/ehv726
ISSN
0195-668X
1522-9645
Abstract
Aims Inflammation plays essential role in development of plaque disruption and coronary stent-associated complications. This study aimed to examine whether intracoronary dual-modal optical coherence tomography (OCT)-near-infrared fluorescence (NIRF) structural-molecular imaging with indocyanine green (ICG) can estimate inflammation in swine coronary artery. Methods and results After administration of clinically approved NIRF-enhancing ICG (2.0 mg/kg) or saline, rapid coronary imaging (20 mm/s pullback speed) using a fully integrated OCT-NIRF catheter was safely performed in 12 atheromatous Yucatan minipigs and in 7 drug-eluting stent (DES)-implanted Yorkshire pigs. Stronger NIRF activity was identified in OCT-proven high-risk plaque compared to normal or saline-injected controls (P = 0.0016), which was validated on ex vivo fluorescence reflectance imaging. In vivo plaque target-to-background ratio (pTBR) was much higher in inflamed lipid-rich plaque compared to fibrous plaque (P < 0.0001). In vivo and ex vivo peak pTBRs correlated significantly (P < 0.0022). In vitro cellular ICG uptake and histological validations corroborated the OCT-NIRF findings in vivo. Indocyanine green colocalization with macrophages and lipids of human plaques was confirmed with autopsy atheroma specimens. Two weeks after DES deployment, OCT-NIRF imaging detected strong NIRF signals along stent struts, which was significantly higher than baseline (P = 0.0156). Histologically, NIRF signals in peri-strut tissue co-localized well with macrophages. Conclusion The OCT-NIRF imaging with a clinical dose of ICG was feasible to accurately assess plaque inflammation and DES-related inflammation in a beating coronary artery. This highly translatable dual-modal molecular-structural imaging strategy could be relevant for clinical intracoronary estimation of high-risk plaques and DES biology.
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