Hypoxia-directed and activated theranostic agent: Imaging and treatment of solid tumor
Abstract
Hypoxia, a distinguished feature of various solid tumors, has been considered as a key marker for tumor progression. Inadequate vasculature and high interstitial pressures result in relatively poor drug delivery to these... [ view full abstract ]
Hypoxia, a distinguished feature of various solid tumors, has been considered as a key marker for tumor progression. Inadequate vasculature and high interstitial pressures result in relatively poor drug delivery to these tumors. Herein, we developed an antitumor theranostic agent, 4, which is activated in hypoxic conditions and can be used for the diagnosis and treatment of solid tumors. Compound 4, bearing biotin, a tumor-targeting unit, and SN38, an anticancer drug, proved to be an effective theranostic agent for solid tumors. SN38 plays a dual role: as an anticancer drug for therapy and as a fluorophore for diagnosis, thus avoids an extra fluorophore and limits cytotoxicity. Compound 4, activated in the hypoxic environment, showed high therapeutic activity in A549 and HeLa cells and spheroids. In vivo imaging of solid tumors confirmed the tumor-specific localization, deep tissue penetration and activation of 4, as well as the production of a strong anticancer effect through the inhibition of tumor growth in a xenograft mouse model validating it as a promising strategy for the treatment of solid tumors.
Authors
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Hyun Min Kim
(Bioimaging Research Team, Korea Basic Science Institute)
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Eun-joong Kim
(Department of Biomedical Engineering, School of medicine, Kyung Hee University)
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Hyunseung Lee
(Bioimaging Research Team, Korea Basic Science Institute)
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Jong Seung Kim
(Department of Chemistry, Korea University)
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Kwan Soo Hong
(Bioimaging Research Team, Korea Basic Science Institute)
Topic Areas
Targeted drug delivery and Nanocarriers , Nanomedecine for cancer diagnosis & therapy
Session
PS2 » Poster Session & Sponsors Exhibition (13:30 - Thursday, 29th September, Patio 25)
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