| Literature DB >> 30285414 |
Wei Tang1, Zhibin Zhao2,3, Yuanyuan Chong1, Chengfan Wu1, Qingzhi Liu2,3, Jingbo Yang3, Rongbin Zhou3, Zhe-Xiong Lian2,3, Gaolin Liang1.
Abstract
Many chronic liver diseases will advance to hepatic fibrosis and, if without timely intervention, liver cirrhosis or even hepatocellular carcinoma. Anti-inflammation could be a standard therapeutic strategy for hepatic fibrosis treatment, but a "smart" strategy of hepatic fibrosis-targeted, either self-assembly or slow release of an anti-inflammation drug ( e.g., dexamethasone, Dex), has not been reported. Herein, we rationally designed a hydrogelator precursor Nap-Phe-Phe-Lys(Dex)-Tyr(H2PO3)-OH (1-Dex-P) and proposed a tandem enzymatic strategy of self-assembly and slow release of Dex, with which the precursor exhibited much stronger antihepatic fibrosis effect than Dex both in vitro and in vivo. Enzymatic and cell experiments validated that 1-Dex-P was first dephosphorylated by alkaline phosphatase to yield Nap-Phe-Phe-Lys(Dex)-Tyr-OH (1-Dex), which self-assembled into nanofiber 1-Dex. The nanofiber was then hydrolyzed by esterase to transform into nanofiber 1, accompanied by slow release of Dex. We anticipate that our "smart" tandem enzymatic strategy could be widely employed to design more sophisticated drug delivery systems to achieve enhanced therapeutic efficacy than free drugs in the future.Entities:
Keywords: dexamethasone; hepatic fibrosis; self-assembly; slow release; tandem
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Year: 2018 PMID: 30285414 DOI: 10.1021/acsnano.8b04143
Source DB: PubMed Journal: ACS Nano ISSN: 1936-0851 Impact factor: 15.881