首页> 外文期刊>Journal of biomedical materials research. Part B, Applied biomaterials. >Synthesis and efficient hepatocyte targeting of galactosylated chitosan as a gene carrier in vitro and in vivo.
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Synthesis and efficient hepatocyte targeting of galactosylated chitosan as a gene carrier in vitro and in vivo.

机译:半乳糖基化壳聚糖作为基因载体的合成和有效靶向肝细胞的体内和体外。

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While chitosan (CS) has been researched widely as a non-viral vector, its usefulness has been limited by its low cell specificity and transfection efficiency. Therefore, we successfully synthesized galactosylated chitosan (GC) and complexed it with an enhanced green fluorescent protein plasmid (pIRES-EGFP) for transfection into cultured H22 cells (murine hepatic cancer cell line) using various GC/EGFP (N/P) charge ratios. Maximal gene transfection rates detected by flow cytometry occurred at an N/P ratio 5:1. Compared with those of lipofectin/EGFP and naked pIRES-EGFP, GC/EGFP complexes show a very efficient cell-selective transfection to hepatocytes. The MTT assay detected relatively low cytotoxicity in cells transfected with GC. A recombinant plasmid granulocyte-macrophage colony-stimulating factor (GM-SCF) and interleukin (IL) 21 (pIRES/GM-CSF-IL21) was successfully constructed and GC/GM-CSF-IL21 nanoparticles (average diameter, 82.1 nm) were administered via the tail vein of mice with liver metastasis of colon cancer model, for 5 consecutive days. The GC/GM-CSF-IL21 nanoparticles exhibited hepatocyte and passive tumor specificity, increased therapeutic efficacy compared to control groups, promoted leukocytes to aggregate in tumor tissues, and activated the cytotoxicity of natural killer (NK) cells and cytolytic T lymphocyte (CTL). Our results indicate that GC can be used in gene therapy to improve transfection efficiency and can be used as an immunological stimulant in vivo.
机译:壳聚糖(CS)作为一种非病毒载体已得到广泛研究,但其实用性受到其细胞特异性和转染效率低的限制。因此,我们成功地合成了半乳糖基化壳聚糖(GC),并将其与增强的绿色荧光蛋白质粒(pIRES-EGFP)进行了复合,以使用各种GC / EGFP(N / P)电荷比转染到培养的H22细胞(鼠肝癌细胞系)中。通过流式细胞仪检测到的最大基因转染率发生在N / P比为5:1的情况下。与lipofectin / EGFP和裸pIRES-EGFP相比,GC / EGFP复合物对肝细胞显示出非常有效的细胞选择性转染。 MTT测定法在用GC转染的细胞中检测到相对较低的细胞毒性。成功构建了重组质粒粒细胞-巨噬细胞集落刺激因子(GM-SCF)和白介素(IL)21(pIRES / GM-CSF-IL21),并制备了GC / GM-CSF-IL21纳米粒子(平均直径为82.1 nm)。通过具有结肠癌模型的肝转移的小鼠的尾静脉连续给药5天。与对照组相比,GC / GM-CSF-IL21纳米颗粒具有肝细胞和被动性肿瘤特异性,增强了治疗功效,促进白细胞在肿瘤组织中聚集,并激活了自然杀伤(NK)细胞和溶细胞性T淋巴细胞(CTL)的细胞毒性。 。我们的结果表明,GC可以用于基因治疗以提高转染效率,并且可以用作体内的免疫刺激剂。

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