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Tumor-binding prodrug micelles of polymer-drug conjugates for anticancer therapy in HeLa cells

Authors
Jung, BokyungJeong, Yong-CheolMin, Jun-HongKim, Jung-EunSon g, Yoon-JaePark, Jung-KiPark, Jung-HwanKim, Jong-Duk
Issue Date
14-May-2012
Publisher
Royal Society of Chemistry
Citation
Journal of Materials Chemistry, v.22, no.18, pp 9385 - 9394
Pages
10
Journal Title
Journal of Materials Chemistry
Volume
22
Number
18
Start Page
9385
End Page
9394
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/20884
DOI
10.1039/c2jm30534h
ISSN
0959-9428
1364-5501
Abstract
An interesting phytosphingosine (PHS), a natural sphingolipid metabolite comprising ceramides, is believed to play a vital role in strong anticancer therapeutic efficacy for various types of cancer cells, which is based on a programmed cellular death mechanism, so called apoptosis. However, extremely low water-solubility has been an obstacle to its usage as an anticancer drug via the systemic administration route. To utilize the benefits of PHS, we developed tumor-targeting polymer-drug conjugates wherein hydrophobic PHS was connected to the folate-grafted hydrophilic and biocompatible polymer through pH-sensitive linkages. The polymer-drug conjugates formed nano-sized (10-20 nm) spherical micelles spontaneously in aqueous media and they were found to have high drug contents (10.3 wt%). We present a systematic study of in vitro anticancer therapy in HeLa cells treated by tumor-targeting micelles in terms of anti-proliferation. The anticancer effect was analyzed by apoptotic cell death as well as the preferential distribution of loaded drug in the cancer cells. The synergistic effect by loading the commercial drug of doxorubicin was also studied. © 2012 The Royal Society of Chemistry.
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