Hepatitis B virus preS1-derived lipopeptide functionalized liposomes for targeting of hepatic cells

内吞作用 脂质体 体内 全身给药 受体介导的内吞作用 体外 药理学 基因传递 遗传增强 医学 细胞 生物 生物化学 生物技术 基因
作者
Xuanmiao Zhang,Quan Zhang,Qiang Peng,Jing Zhou,Longfei Liao,Xun Sun,Ling Zhang,Tao Gong
出处
期刊:Biomaterials [Elsevier BV]
卷期号:35 (23): 6130-6141 被引量:51
标识
DOI:10.1016/j.biomaterials.2014.04.037
摘要

To enhance the liver-specific delivery, HBVpreS/2-48myr (HBVP), a synthetic HBVpreS-derived lipopeptide endowed with compelling liver tropism, was conjugated to PEGylated liposomes (HBVP-Lip) for hepatic cell-specific delivery. Compared with the non-targeted liposomes, a significantly higher amount of HBVP-Lip were taken up by the primary mice hepatocytes through a receptor-mediated endocytosis mechanism. The endocytosis inhibition assay demonstrated that the endocytosis of HBVP-Lip was mediated mainly by caveolin and clathrin. After systemic administration in mice, HBVP-Lip could be specifically internalized into hepatocytes efficaciously. Furthermore, the hepatoprotective effects of HBVP-Lip loaded with silybin (SLB) on carbon tetrachloride induced acute liver damage were remarkably stronger than the SLB solution and SLB loaded non-targeted liposomes. Preliminary safety results suggested that no acute systemic toxicity or immunotoxicity was observed after intravenous administration with HBVP-Lip. These results indicated that the HBVP-Lip could deliver the payloads to the hepatocytes with high specificity in vitro and in vivo, and raise new possibilities for liver-specific drug delivery systems, gene delivery systems, and bio-imaging systems.
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