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首页> 外文期刊>Drug Design, Development and Therapy >Plasmid pORF-hTRAIL targeting to glioma using transferrin-modified polyamidoamine dendrimer
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Plasmid pORF-hTRAIL targeting to glioma using transferrin-modified polyamidoamine dendrimer

机译:使用转铁蛋白修饰的聚酰胺酰胺树状聚合物靶向胶质瘤的质粒pORF-hTRAIL

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A gene drug delivery system for glioma therapy based on transferrin (Tf)-modified polyamidoamine dendrimer (PAMAM) was prepared. Gene drug, tumor necrosis factor-related apoptosis-inducing ligand (hTRAIL)-encoding plasmid open reading frame (pORF-hTRAIL, Trail), was condensed by Tf-modified PAMAM to form nanoparticles (NPs). PAMAM-PEG-Tf/DNA NPs showed higher cellular uptake, in vitro gene expression, and cytotoxicity than PAMAM-PEG/DNA NPs in C6 cells. The in vivo targeting efficacy of NPs was visualized by ex vivo fluorescence imaging. Tf-modified NPs showed obvious glioma-targeting trend. Plasmid encoding green fluorescence protein (GFP) was also condensed by modified or unmodified PAMAM to evaluate the in vivo gene expression level. The PAMAM-PEG-Tf/plasmid encoding enhanced green fluorescence protein (pEGFP) NPs exhibited higher GFP expression level than PAMAM-PEG/pEGFP NPs. TUNEL assay revealed that Tf-modified NPs could induce much more tumor apoptosis. The median survival time of PAMAM-PEG-Tf/Trail-treated rats (28.5 days) was longer than that of rats treated with PAMAM-PEG/Trail (25.5 days), temozolomide (24.5 days), PAMAM-PEG-Tf/pEGFP (19 days), or saline (17 days). The therapeutic effect was further confirmed by magnetic resonance imaging. This study demonstrated that targeting gene delivery system had potential application for the treatment of glioma.
机译:制备了基于转铁蛋白(Tf)修饰的聚酰胺酰胺树状大分子(PAMAM)的神经胶质瘤基因药物递送系统。通过Tf修饰的PAMAM将基因药物,肿瘤坏死因子相关的凋亡诱导配体(hTRAIL)编码质粒开放阅读框(pORF-hTRAIL,Trail)缩合形成纳米颗粒(NPs)。与C6细胞中的PAMAM-PEG / DNA NPs相比,PAMAM-PEG-Tf / DNA NPs显示出更高的细胞摄取,体外基因表达和细胞毒性。通过离体荧光成像观察NP的体内靶向功效。 Tf修饰的NPs表现出明显的胶质瘤靶向趋势。编码绿色荧光蛋白(GFP)的质粒也可以通过修饰或未修饰的PAMAM进行缩合,以评估体内基因表达水平。编码增强的绿色荧光蛋白(pEGFP)NP的PAMAM-PEG-Tf /质粒比PAMAM-PEG / pEGFP NP表现出更高的GFP表达水平。 TUNEL分析显示Tf修饰的NPs可以诱导更多的肿瘤细胞凋亡。 PAMAM-PEG-Tf / Trail治疗的大鼠的中位生存时间(28.5天)比使用PAMAM-PEG / Trail /替莫唑胺(24.5天),PAMAM-PEG-Tf / pEGFP治疗的大鼠更长(28.5天) (19天)或生理盐水(17天)。通过磁共振成像进一步证实了治疗效果。这项研究表明靶向基因传递系统在神经胶质瘤的治疗中具有潜在的应用前景。

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