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八精氨酸肽修饰的纳米颗粒介导的肝细胞生长因子基因转染预处理可改善 LPS/D-半乳糖胺诱导的肝炎。

Pretreatment of hepatocyte growth factor gene transfer mediated by octaarginine peptide-modified nanoparticles ameliorates LPS/D-galactosamine-induced hepatitis.

机构信息

Laboratory of Innovative Nanomedicine, Faculty of Pharmaceutical Sciences, Hokkaido University, Sapporo, Hokkaido, Japan.

出版信息

Nucleic Acid Ther. 2012 Oct;22(5):360-3. doi: 10.1089/nat.2012.0352. Epub 2012 Sep 10.

Abstract

We previously reported that an octaarginine- and pH-sensitive fusogenic peptide-modified multifunctional envelope-type nano device (R8-GALA-MEND) produces a high level of gene expression in the liver. In this study, we report on an examination of whether this gene delivery system exerts potent hepatoprotective effects against lipopolysaccharide/D-galactosamine (LPS/D-GalN)-induced acute liver injury. In vivo-jetPEI(™)-Gal, a commercially available in vivo transfection reagent, was used as a reference. The systemic administration of the R8-GALA-MEND or in vivo-jetPEI(™)-Gal showed that the latter was more toxic than the R8-GALA-MEND, indicating that R8-GALA-MEND is a safer system than in vivo-jetPEI(™)-Gal. Pretreatment with R8-GALA-MEND or in vivo-jetPEI(™)-Gal loaded with hepatocyte growth factor (HGF) pDNA inhibited serum GPT and GOT levels from becoming elevated. However, the survival rate of the mice was significantly enhanced in the case of R8-GALA-MEND, but not for the in vivo-jetPEI(™)-Gal treatment. These results demonstrate that R8-GALA-MEND has the potential for use in the pretreatment of an acute liver injury.

摘要

我们之前报道过,一种八精氨酸和 pH 敏感的融合肽修饰的多功能包膜型纳米装置(R8-GALA-MEND)在肝脏中产生高水平的基因表达。在本研究中,我们研究了这种基因传递系统是否对脂多糖/半乳糖胺(LPS/D-GalN)诱导的急性肝损伤具有强大的肝保护作用。体内喷射 PEI(™)-Gal,一种市售的体内转染试剂,被用作参考。R8-GALA-MEND 或体内喷射 PEI(™)-Gal 的系统给药表明,后者比 R8-GALA-MEND 更具毒性,这表明 R8-GALA-MEND 比体内喷射 PEI(™)-Gal 更安全。用 R8-GALA-MEND 或体内喷射 PEI(™)-Gal 预处理负载肝细胞生长因子(HGF)pDNA 可抑制血清 GPT 和 GOT 水平升高。然而,在 R8-GALA-MEND 的情况下,小鼠的存活率显著提高,而体内喷射 PEI(™)-Gal 处理则没有。这些结果表明,R8-GALA-MEND 有可能用于急性肝损伤的预处理。

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