| Literature DB >> 24768405 |
Jing Yu1, Xu Xu1, FuLin Yao2, Zichao Luo2, Ling Jin1, BinBin Xie1, Shuai Shi1, Huixiang Ma1, XingYi Li3, Hao Chen1.
Abstract
Avastin(®) has been clinically proved to be effective in the treatment of intraocular neovascularization diseases. However, the short half-life of Avastin(®) need frequent administration to maintain its therapeutic efficiency. In this paper, we attempted to develop an in situ PEG hydrogels with great biocompatibility for sustained release of Avastin(®) to inhibit the corneal neovascularization. PEG hydrogels was formed via thiol-maleimide reaction using 4-arm PEG-Mal and 4-arm PEG-SH. The transparent hydrogel was rapidly formed under physiological conditions. By varying the concentration of 4-arm PEG-SH, PEG hydrogel with different gelling time, pore size, swelling ratio and mechanical property could be obtained. In vitro cytotoxicity indicated that the developed PEG hydrogel had no apparent cytotoxicity on L-929 cells after 7 days of incubation. In vitro release study showed the encapsulated Avastin(®) was sustained release from PEG hydrogels within a period of 14 days study. Sodium dodecyl sulfate-polyacrylamide gel electrophoresis (SDS-PAGE) analysis further confirmed that the released Avastin(®) did not undergo apparent hydrolysis within 14 days. As a conclusion, we could conclude that the developed PEG hydrogels as an injectable hydrogels might be suitable for extended Avastin(®) release to treat the corneal neovascularization.Entities:
Keywords: Avastin; Corneal neovascularization; PEG hydrogel; Sustained release
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Year: 2014 PMID: 24768405 DOI: 10.1016/j.ijpharm.2014.04.053
Source DB: PubMed Journal: Int J Pharm ISSN: 0378-5173 Impact factor: 5.875