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Human Glioblastoma Visualization: Triple Receptor-Targeting Fluorescent Complex of Dye, SIWV Tetra-Peptide, and Serum Albumin Protein

Authors
An, Jong MinMoon, HeejoVerwilst, PeterShin, JinwooKim, B. MoonPark, Chul-KeeKim, Jong SeungYeo, Seung GeunKim, Hyo YoungKim, Dokyoung
Issue Date
25-6월-2021
Publisher
AMER CHEMICAL SOC
Keywords
fluorescent probe; albumin complex; fluorescence-guided surgery; glioblastoma targeting; two-photon microscopy
Citation
ACS SENSORS, v.6, no.6, pp.2270 - 2280
Indexed
SCIE
SCOPUS
Journal Title
ACS SENSORS
Volume
6
Number
6
Start Page
2270
End Page
2280
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/127819
DOI
10.1021/acssensors.1c00320
ISSN
2379-3694
Abstract
Fluorescence guided surgery (FGS) has been highlighted in the clinical site for guiding surgical procedures and providing the surgeon with a real-time visualization of the operating field. FGS is a powerful technique for precise surgery, particularly tumor resection; however, clinically approved fluorescent dyes have often shown several limitations during FGS, such as non-tumor-targeting, low in vivo stability, insufficient emission intensity, and low blood-brain barrier penetration. In this study, we disclose a fluorescent dye complex, peptide, and protein for the targeted visualization of human glioblastoma (GBM) cells and tissues. Our noble triple receptor-targeting fluorescent complex (named BSA-OXN-SIWV) consists of (i) dipolar oxazepine dye (OXN), which has high stability, low cytotoxicity, bright fluorescence, and two-photon excitable, (ii) tetra-peptide (SIWV) for the targeting of the caveolin-1 receptor, and (iii) bovine serum-albumin (BSA) protein for the targeting of albondin (gp60) and secreted protein acidic and rich in cysteine receptor. The photophysical properties and binding mode of BSA-OXN-SIWV were analyzed, and the imaging of GBM cell lines and human clinical GBM tissues were successfully demonstrated in this study. Our findings hold great promise for the application of BSA-OXN-SIWV to GBM identification and the surgery at clinical sites, as a new FGS agent.
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