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Three-dimensional porous HPMA-co-DMAEM hydrogels for biomedical application

Authors
Choi, Soon MoSingh, DeeptiCho, Yong WooOh, Tae HwanHan, Sung Soo
Issue Date
May-2013
Publisher
SPRINGER
Keywords
Cancer therapy; Dual responsive; Drug delivery system; In vivo bio-compatibility; Tissue engineering
Citation
COLLOID AND POLYMER SCIENCE, v.291, no.5, pp.1121 - 1133
Indexed
SCIE
SCOPUS
Journal Title
COLLOID AND POLYMER SCIENCE
Volume
291
Number
5
Start Page
1121
End Page
1133
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/28389
DOI
10.1007/s00396-012-2837-1
ISSN
0303-402X
Abstract
The aim of this work is to develop a novel biocompatible drug delivery carrier and tissue engineering scaffold with the ability of controlled drug release and also tissue regeneration. We have synthesized N-(2-hydroxypropyl)methacrylamide and 2-(dimethylamino)ethyl methacrylate copolymer-based hydrogels loaded with doxorubicin and tested in vitro. The manifestation of temperature sensitivity is noted with a sharp decrease or increase in hydrogel optical transparency that happens with the temperature exceeding a critical transition value. The drug release profile exhibited pH-sensitive behavior of the hydrogel. The hydrolytic degradation of gel and in vitro studies of polymer-doxorubicin conjugate and doxorubicin release from hydrogel matrix indicated that hydrogels were stable under acidic conditions (in buffers at pH 4.64 and 6.65). In both drug forms, polymer-doxorubicin conjugate and free doxorubicin could be released from the hydrogel scaffold at a rate depending directly on either the rate of drug diffusion from the hydrogel or rate of hydrogel degradation or at rate controlled by a combination of the both processes. In vitro analysis showed homogenous cell attachment and proliferation on synthesized hydrogel matrix. In vivo implantation demonstrated integration of the gel with the surrounding tissue of mice within 2 weeks and prominent neo-angiogenesis observed in the following weeks. This multifunctional hydrogels can easily overcome biological hurdles in the in vivo conditions where the pH range changes drastically and could attain higher site-specific drug delivery improving the efficacy of the treatment in various therapeutical applications, especially in cancer therapy, and could also be used as tissue engineering scaffold due to its porous interconnected and biocompatible behavior.
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Cho, Yong Woo
ERICA 공학대학 (DEPARTMENT OF MATERIALS SCIENCE AND CHEMICAL ENGINEERING)
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