| Literature DB >> 29749265 |
Hoon Hyun1, Min Ho Park2, Wonbong Lim3, So Yeon Kim4, Danbi Jo1, Jin Seok Jung1, Gayoung Jo1, Sewook Um5, Deok-Won Lee6, Dae Hyeok Yang7.
Abstract
Currently available chemotherapy is associated with serious side effects, and therefore novel drug delivery systems (DDSs) are required to specifically deliver anticancer drugs to targeted sites. In this study, we evaluated the feasibility of visible light-cured glycol chitosan (GC) hydrogels with controlled release of doxorubicin⋅hydrochloride (DOX⋅HCl) as local DDSs for effective cancer therapy in vivo. The storage modulus of the hydrogel precursor solutions was increased as a function of visible light irradiation time. In addition, the swelling ratio of the hydrogel irradiated for 10 s (GC10/DOX) was greater than in 60 s (GC60/DOX). In vitro release test showed that DOX was rapidly released in GC10/DOX compared with GC60/DOX due to the density of cross-linking. In vitro and in vivo tests including cell viability and measurement of tumor volume showed that the local treatment of GC10/DOX yielded substantially greater antitumor effect compared with that of GC60/DOX. Therefore, the visible light-cured GC hydrogel system may exhibit clinical potential as a local DDS of anticancer drugs with controlled release, by modulating cross-linking density.Entities:
Keywords: Glycol chitosan; cross-linking density; doxorubicin⋅hydrochloride; local drug delivery system; visible light irradiation
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Year: 2018 PMID: 29749265 DOI: 10.1080/21691401.2018.1470529
Source DB: PubMed Journal: Artif Cells Nanomed Biotechnol ISSN: 2169-1401 Impact factor: 5.678