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Destroying Deep Lung Tumor Tissue through Lung-Selective Accumulation and by Activation of Caveolin Uptake Channels Using a Specific Width of Carbon Nanodrug

Authors
Kim, Sang-WooPark, Jun-YoungLee, SoyoungKim, Sang-HyunKhang, Dongwoo
Issue Date
7-Feb-2018
Publisher
AMER CHEMICAL SOC
Keywords
lung tumor; carbon nanotubes; caveolin uptake; lung accumulation; anticancer efficacy
Citation
ACS APPLIED MATERIALS & INTERFACES, v.10, no.5, pp.4419 - 4428
Journal Title
ACS APPLIED MATERIALS & INTERFACES
Volume
10
Number
5
Start Page
4419
End Page
4428
URI
https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/4039
DOI
10.1021/acsami.7b16153
ISSN
1944-8244
Abstract
The main difficulty With current anticancer nanotherapeutics comes from the low efficiency of tumor targeting. Althoughniany strategies have been investigated, including cancer-specific antibody conjugation, lung tumors remain one of the invulnerable types of cancer that must be overcome in the near future. Meanwhile, despite their advantageous physiochemical properties, carbon nanotube structures are not considered safe medical drug delivery agents, but are considered a hazardous source that may cause pulmonary toxicity. However, high-aspect-ratio (width vs. length) nanostructures can he used as very efficient drug delivery agents due to their lung tissue accumulation property. Furthermore, selection of a specific width if the carbon nanostructures can activate additional caveolin uptake channels in cancer cells, thereby maximizing internalization of the nanodrug. The present study aimed to evaluate the therapeutic potential of carbon nanotube-based nanodrugs having various widths (10-30 nm, 60-100 mn, and 125-150 nm) as a delivery agent to treat lung tumors. The results of-the present study provided evidence that both lung tissue accumulation (passive targeting) and caveolin-assisted uptake (active targeting) can simultaneously contribute to the destruction of lung tumor tissues of carbon nanotube.
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